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Cancer Research at DKFZ 2014 1964 sSpi 24-96h AED! 2014 50 50 50 GERMAN CANCER RESEARCH CENTER IN THE HELMHOLTZ ASSOCIATION Cancer Research at DKFZ 2014 2 Welcome to the German Cancer Research Center Josef Puchta (left), Chancellor Angela Merkel and Otmar D. Wiestler. With “Cancer Research at DKFZ”, we would like to introduce the DKFZ (Deutsches Krebsforschungszentrum), Germany´s largest biomedical research center whose mission is to fight cancer through research. More than 3000 staff members, including 1000 scientists, contribute to unraveling the basic mechanisms that lead to cancer, identifying cancer risk factors, developing cancer prevention strategies, as well as translating our results from bench to bedside in order to improve cancer diagnosis, therapy and prevention. Cancer is a worldwide burden, with approximately 14.1 million new cases each year and around 8.2 million deaths from cancer. The disease constitutes a particularly challenging task for both research and clinical practice. There are more than 200 different cancer entities in almost every organ in the human body. The changes in affected cells are highly diverse and complex. In 2014, DKFZ is celebrating its 50th anniversary. We are very happy and proud that Chancellor Angela Merkel visited our center on April 23 in honor of this celebration. She was impressed by the major contributions researchers at DKFZ have made in recent years: We understand much better today how cancer develops; we diagnose the disease earlier, treat it better, and prevent it more effectively. In 2008, Harald zur Hausen, the long-standing director of the management board at DKFZ, was awarded the Nobel Prize for Medicine. He had discovered that human papillomaviruses cause cervical cancer, which led to the development of a vaccine that is now available worldwide. Perhaps you too would like to be part of this unique institution at the cutting edge of cancer research. “Cancer Research at DKFZ" gives you a taste of what research is like in our center. Come and join us as a PhD student, Post Doc, group leader or as a full Professor. We look forward to welcoming you to our institution. Best wishes Prof. Dr. Dr. h. c. Otmar D. Wiestler Chairman and Scientific Director Prof. Dr. Josef Puchta Administrative-Commercial Director 3 Contents DKFZ – The German Cancer Research Center______________6 NCT – National Center for Tumor Diseases Heidelberg______9 The German Consortium for Translational Cancer Research____________________________________ 10 Nobel Prize in Medicine 2008 - Harald zur Hausen________ 12 DKFZ Life-Science Lab________________________________ 14 Graduate Studies at the DKFZ_________________________ 15 Cancer Information Service___________________________ 16 Unit Cancer Prevention_______________________________ 17 Heidelberg – A Capital of Biomedical Sciences in Europe___ 20 CORE FACILITIES_________________________________________ 23 Genomics and Proteomics____________________________ 24 Imaging and Cytometry______________________________ 25 Information Technology______________________________ 26 Animal Laboratory Services___________________________ 27 Library_____________________________________________ 28 Joint Chemical Biology Core Facility of EMBL & DKFZ______ 29 Index_____________________________________________ 142 Imprint___________________________________________ 143 4 RESEARCH PROGRAMS_________________________ 31 Cell Biology and Tumor Biology_______________________ 32 Stem Cells and Cancer_______________________________ 34 Molecular Embryology_______________________________ 35 Signal Transduction and Growth Control _______________ 36 Epigenetics_________________________________________ 38 Systems Biology of Cellular Signal Transduction__________ 39 Redox Regulation___________________________________ 40 Molecular Metabolic Control _________________________ 41 Vascular Oncology and Metastasis _____________________ 42 Cell Growth and Proliferation _________________________ 43 Clinical Neurobiology ________________________________ 44 Chaperones and Proteases ___________________________ 45 Molecular Neurobiology _____________________________ 46 Molecular Biology of the Cell II________________________ 47 Cell Biology ________________________________________ 48 Molecular Biology of the Cell I ________________________ 49 Molecular Biology of Centrosomes and Cilia_____________ 50 Posttranscriptional Control of Gene Expression __________ 51 Cellular Senescence_________________________________ 52 Normal and Neoplastic CNS Stem Cells _________________ 53 Vascular Signaling and Cancer_________________________ 54 Stress-induced Activation of Hematopoietic Stem Cells____ 55 Experimental Hematology____________________________ 56 Biomarker identification______________________________ 57 Metastatic Niches___________________________________ 58 Synaptic Signalling and Neurodegeneration_____________ 59 Structural and Functional Genomics ________________ 60 Tumor Genetics_____________________________________ 62 Biophysics of Macromolecules_________________________ 63 Molecular Genome Analysis__________________________ 64 Molecular Genetics _________________________________ 65 Pediatric Neurooncology _____________________________ 66 Functional Genome Analysis __________________________ 67 Theoretical Bioinformatics ___________________________ 68 Theoretical Systems Biology __________________________ 69 Signaling and Functional Genomics ____________________ 70 Signal Transduction in Cancer and Metabolism __________ 72 Molecular RNA Biology and Cancer_____________________ 73 Membrane Biophysics _______________________________ 74 Systems Biology of Cell Death Mechanisms______________ 75 Proteostasis in Neurodegenerative Disease______________ 76 Lysosomal Systems Biology ___________________________ 77 Cancer Risk Factors and Prevention__________________ 78 Epigenomics and Cancer Risk Factors___________________ 80 Cancer Epidemiology ________________________________ 81 Molecular Genetic Epidemiology______________________ 82 Biostatistics________________________________________ 83 Clinical Epidemiology and Aging Research_______________ 84 Molecular Epidemiology______________________________ 85 Tumor Immunology____________________________________ 86 Translational Immunology ___________________________ 88 Immunogenetics____________________________________ 89 Molecular Immunology______________________________ 90 Developmental Immunology _________________________ 91 Cellular Immunology ________________________________ 92 Innate Immunity____________________________________ 93 Immune Tolerance___________________________________ 94 Imaging and Radiooncology__________________________ 96 Radiology__________________________________________ 98 Medical Physics in Radiology__________________________ 99 Radiopharmaceutical Chemistry _____________________ 100 Medical Physics in Radiation Oncology ________________ 101 Radiation Oncology_________________________________ 102 Molecular Radiooncology____________________________ 103 Nuclear Medicine __________________________________ 104 Medical and Biological Informatics ___________________ 105 Optical Nanoscopy _________________________________ 106 Translational Radiation Oncology_____________________ 108 Computer-assisted Interventions_____________________ 109 Infection and Cancer__________________________________ 110 Tumorvirology_____________________________________ 112 Genome Modifications and Carcinogenesis_____________ 113 Viral Transformation Mechanisms ____________________ 114 Characterization of Tumorviruses_____________________ 115 Pathogenesis of Virus Associated Tumors______________ 116 Oncolytic Adenoviruses_____________________________ 117 Noroviruses_______________________________________ 118 Infection and Innate Immune Sensing Dynamics________ 119 Translational Cancer Research_______________________ 120 Translational Oncology _____________________________ 122 Applied Tumor Biology ______________________________ 123 Preventive Oncology _______________________________ 124 Cellular and Molecular Pathology _____________________ 125 Molecular Tumor Pathology _________________________ 126 Dermato-Oncology _________________________________ 127 Molecular Hematology/Oncology ____________________ 128 Pediatric Oncology _________________________________ 130 Molecular Oncology of Solid Tumors___________________ 131 Molecular Oncology of Gastrointestinal Tumors_________ 132 Neurooncology____________________________________ 134 Neuropathology___________________________________ 135 Experimental Neuroimmunology_____________________ 136 Experimental Therapies for Hematologic Malignancies___ 137 Molecular Mechanisms of Tumor Cell Invasion__________ 138 Neuropeptides_____________________________________ 139 5 DKFZ The German Cancer Research Center The German Cancer Research Center (DKFZ) is one of the world’s leading biomedical research institutions. It serves the mission to identify and study cancer risk factors and to unravel mechanisms of cancer development. The findings from our basic research are systematically employed to develop new approaches for prevention, diagnosis and treatment. Employees: 2763 Staff Scientists: 878 Doctoral students: 384 Scientists from 63 nations (as of December 2013) The German Federal Government provides 90 percent of the funding of the German Cancer Research Center, and the State of Baden-Württemberg the remaining 10 percent. Additional income stems from external project funding, license revenues, donations and bequests. The 47 scientific divisions, 28 junior research groups and 13 clinical cooperation units are assigned to seven Research Programs: • • • • • • • Cell Biology and Tumor Biology Functional and Structural Genomics Cancer Risk Factors and Prevention Tumor Immunology Imaging and Radiooncology Infection and Cancer Translational Cancer Research Jointly with Heidelberg University Hospital, DKFZ has established the National Center for Tumor Diseases (NCT) Heidelberg where promising approaches from cancer research are translated into the clinic. The Cancer Information Service (KID) provides cancer patients, their families, and other interested parties with information that is readily understandable, scientifically founded, impartial, and up to date. In 2011, the German Consortium for Translational Cancer Research was introduced to the public by the BMBF, the German Federal Government, as one of six German Centers for Health Research. This initiative intends to foster the nationwide strategic collaboration of the most excellent scientists and clinicians in exploring common cancer diseases. 6 DKFZ Main Building 7 DKFZ The German Cancer Research Center “ATV” Building In the applied tumor virology building scientists work with viruses that cause cancer, such as HPV oder EBV, but also with viruses that infect and kill cancer cells, such as the oncolytic parvoviruses. “TP3” Building This building, completed in 2002, is where genome research takes places. This so-called “Genome-Building” harbors the DKFZ´s sequencing facility with 15 high-throughput next generation DNA sequencing instruments. It also houses servers with a data storage capacity of 10 terabytes, 1.2 terabytes of which is reserved for the three German projects in the International Cancer Genome Consortium. “TP4” Building This building in the technology park of the Neuenheim Campus was acquired in 2007 and provides additional space for 320 people. 7T MRI Building As part of the strategic alliance with Siemens, a 7T MRI system was installed in a new facility. Thirty tons of steel included in the surrounding walls shield the ultra high magnetic field from the environment. 8 NCT National Center for Tumor Diseases Heidelberg Initiated in 2004, and actively treating patients since 2005, the National Center for Tumor Diseases (NCT) Heidelberg was founded as an exceptional alliance between the German Cancer Research Center (DKFZ), Heidelberg University Medical School (HUMS) together with Heidelberg Medical Faculty and German Cancer Aid (Deutsche Krebshilfe). NCT is a comprehensive cancer center uniquely positioned to benefit from the wealth of DKFZ cancer research and the Heidelberg biomedical campus. NCT’s mission is two-fold: to provide optimal interdisciplinary oncology with current clinical therapies and to rapidly transfer scientific knowledge into clinical applications through comprehensive translational and preventive oncology. The new 5500 m2 NCT Core Building has been completed in 2010. NCT is the principal portal of entry for all oncology patients into the medical center, and the primary location of all oncology outpatient care. It integrates and supports all clinical and translational research activities of DKFZ and HUMS. DKFZ’s many scientific disciplines and interactions, including strategic partnerships with university medical centers and industry, provide a strong framework for NCT projects. Research at DKFZ 2014 In 2012, approx. 11,000 newly diagnosed cancer patients were seen at NCT and more than 18,000 anti-tumor therapies were administered. With more than 50,000 out-patient visits p.a., patient numbers are steadily growing. More than 300 diagnostic, therapeutic and preventive clinical trials, including investigator initiated trials, were developed and conducted. NCT pursues personalized oncology as a center-wide master strategy that coordinates all activities towards individualized cancer medicine, including patient-oriented genetics, proteomics, radiooncology, immunology and prevention. The recently established Heidelberg Center for Personalized Oncology (DKFZHIPO) forms a dedicated genomics, proteomics and bioinformatics platform of DKFZ, enabling excellent basic and translational research. Its clinical counterpart, the NCT Precision Oncology Program (NCT POP) combines molecular diagnostics, innovative therapeutics development, interdisciplinary patient care and prevention to define molecularly stratified patient cohorts and hypothesis-driven treatments. Towards this goal, the center aims to provide comprehensive high-throughput genetic and molecular analysis as a stratification tool for every NCT patient by 2015. 9 DKTK The German Consortium for Translational Cancer Research The DKTK Steering Committee (from left to right): Josef Puchta (Heidelberg), Christoph Peters (Freiburg), Otmar D. Wiestler (Heidelberg), Christian Peschel (Munich), Reinhold Schäfer (Berlin), Wolfgang Hiddemann (Munich), Christof von Kalle (Heidelberg), Martin Schuler (Essen/Düsseldorf), Michael Baumann (Dresden), Hubert Serve (Frankfurt), Klaus Schulze-Osthoff (Tübingen) Successful cancer research necessitates intensive exchange between very differing specialties. For this reason, cancer research often takes place at very large centers; in the USA in some incidences they have over 10,000 staff members. The German Cancer Consortium reaches a critical mass in another way, by establishing long term links between the German Cancer Research Center in Heidelberg and some of the largest university hospitals in Germany. Currently, some twenty institutions are cooperating at eight different sites. Seven programs in the fight against cancer A core function of cancer research is the continuous review of fundamental research results to identify new targets for prevention, diagnosis and treatment of cancer diseases. More than 420 physicians, scientists and their groups in the DKTK are committed to this “translational” concept. There are seven defined research programs, in each of which an increasing number of sites are participating: Joint platforms harness strengths The joint research work within DKTK is vitally supported by five platforms providing the necessary infrastructure for the Consortium. A core element is the “Clinical Communication Platform“. It allows the recruitment of patients at all sites and also serves as a shared pivot in innovative clinical trials. In addition, there will be technically oriented platforms. The aim is to harmonize the technical requirements over all sites to ensure comparable data and to provide a common structure allowing scientists from all locations access to methods that would otherwise be unavailable. Attractive offers for junior researchers In cancer research it is essential that different disciplines pull together. Accordingly, a broad program to develop junior researchers is extremely important. Young medical doctors, especially those with some clinical experience are offered the opportunity of training in cancer research at the “School of Oncology”. Likewise, researchers with a background in natural sciences will be introduced to translational research. | Oncogenic Pathways | Molecular Diagnostics | Cancer Immunology and Immunotherapy | Stem Cells in Oncology | Radiation Oncology and Imaging | Treatment Resistance | Cancer Prevention, Early Detection, and Outcomes 10 The individual research platforms are: | Clinical Communication Platform | GMP and Core Services | Preclinical Models | Drug Development | School of Oncology The DKTK Partner Sites DKTK Berlin Charité Comprehensive Cancer Center, Berlin PROFESSOR DR. REINHOLD SCHÄFER DKTK Dresden Medical Faculty and University Hopsital Carl Gustav Carus, Max-Planck-Institute for Molecular Cell Biology and Genetics, Helmholtz Research Center Dresden-Rossendorf PROFESSOR DR. MICHAEL BAUMANN DKTK Essen/Düsseldorf Westdeutsches Tumorzentrum of the University Hospital Essen, Heinrich Heine-University Düsseldorf PROFESSOR DR. MARTIN SCHULER DKTK Frankfurt/Mainz University Cancer Center Frankfurt, GoetheUniversity Frankfurt, Georg-Speyer-Haus, Frankfurt, Krankenhaus Nordwest, Frankfurt, University Medical Center, Mainz PROFESSOR DR. HUBERT SERVE DKTK Freiburg University Medical Center of the Albert-LudwigsUniversity Freiburg, Max-Planck-Institute of Immunobiology, Freiburg PROFESSOR DR. CHRISTOPH PETERS DKTK Heidelberg (Core Center) German Cancer Research Center Heidelberg (DKFZ), Heidelberg University Medical School, National Center for Tumor Diseases (NCT), Heidelberg; Associated Partner: Paul-Ehrlich-Institute, Langen, University of Cologne PROFESSOR DR. DR. H.C. OTMAR WIESTLER, PROFESSOR DR. JOSEF PUCHTA DKTK Munich Ludwig-Maximilians University Munich, Technische Universität Munich PROFESSOR DR. WOLFGANG HIDDEMANN DKTK Tübingen Faculty of Medicine and University Hospital, Eberhard Karls University of Tübingen, Fakulty of Life Science, Eberhard Karls Universität Tübingen PROFESSOR DR. KLAUS SCHULZE-OSTHOFF The second DKTK-Retreat on May 12th and 13th 2014 was a full success. More than 300 persons participated. Research at DKFZ 2014 11 Nobel Prize in Medicine 2008 Harald zur Hausen The idea was revolutionary back in 1972. Flying in the face of prevailing expert opinion, Harald zur Hausen hypothesized that the viruses that cause warts might also play a role in the development of cervical cancer. Supplying the evidence turned out to be more difficult than he had anticipated. In 1983, however, after years of relentless searching, zur Hausen and his team at last succeeded in isolating the DNA of this pathogen, also known as human papillomavirus (HPV), in a biopsy. What they had found was HPV16, a hitherto unknown representative of the large and complex family of papillomaviruses. In the following years, it transpired that the two high-risk virus types HPV16 and HPV18 are responsible for around 70 percent of all cases of cervical cancer worldwide. A total of 15 of the 170 HPVs so far identified have been shown to be carcinogenic. The DNA of papillomaviruses is found inmore than 99 percent of all tissue samples taken from women with cervical cancer. This type of cancer affects around half a million women every year. The disease often ends in death, especially in Third World countries which cannot afford cancer screening programs. Following their discovery of carcinogenic papillomaviruses, zur Hausen and his team studied how the pathogens survive in the cell and how the cells eventually mutate into cancer. It was their understanding of the biology of infection that enabled them to develop a vaccine to protect women against cervical cancer. Harald zur Hausen served as Chairman of the German Cancer Research Center from 1983 to 2003. In 2008, he was awarded the Nobel Prize in Medicine in honor of his outstanding contribution to science. 12 Press conference on October 6, 2008 in the DKFZ Communication Center. Research at DKFZ 2014 13 DKFZ Life-Science Lab: A place where students can think and experiment The Life-Science Lab which has been established at DKFZ offers extracurricular opportunities to talented middle and senior high school students with a particular interest in math and science. Here, the focus is on those areas in the life sciences in which research is being conducted at DKFZ and partner institutions. In addition to helping the students to develop interdisciplinary competence and to achieve personal goals that are educationally significant, they are also encouraged to work independently and to take responsibility for research activities so as to experience the pleasure of discovery and to learn how to collaborate constructively. The multi-year program is organized into six areas of activities: 1. Public Friday lectures on scientific, theoretical, and philosophical topics aim to awaken curiosity in the students. 2. Core research work takes place in scientist-mentored work groups in the fields of archeology, astrophysics, chemistry, experimental physics, informatics, climatology, art, mathematics, molecular cell biology, neuropsychology, medicine, pharmacy, philosophy, political science, quantum physics, robotics, synthetic biology, systems biology, theoretical physics, commerce, and zoology. 3. Weekend seminars present opportunities to broaden the scope of work group research. 4. (Inter)National summer academies, for example, internships lasting for several weeks as research fellows at the universities of Stanford and Berkeley, afford Participants in the robotics seminar construct a robot together with doctoral candidates from Kaiserslautern University (picture above). High school students work to obtain their „Lab License“ at the Bio-Science Lab (picture in the middle). Good attendance at one of the weekly Friday lectures (picture below). 14 5. 6. opportunities to put the acquired competence into an international context. The Bio-Science Lab and Phys-Tech Lab give depth to the broad theoretical instruction in the areas of biochemistry, molecular and cell biology, as well as in physics and technology, through both mentor-initiated and independent practical laboratory work. Research projects performed under scientific guidance promote the successful development of ideas or separate subprojects and facilitate self-organized and exploratory learning. Successful applicants may participate from eighth grade through to high school graduation. Students in their final year of school share their experience by acting as student mentors. Since 2005, the Alumni Association has been bringing former participants together, which furthers networking. Of particular significance is the integration into genuine research through the participation of scientific mentors from DKFZ, EMBL, the universities of Heidelberg, Mannheim, Kaiserslautern, and Landau as well as from Max Planck Institute, Heidelberg. The Life-Science Lab is further supported by cooperation partners from business and public sectors. In 2009, the Life-Science Lab won First Prize in the competition ”School meets Science” sponsored by the Robert-Bosch Foundation for its model character, while in 2010 the Initiative “Germany – Land of Ideas” awarded the Lab the status “Designated Site of Ideas”. Dr. Katrin Platzer Life-Science Lab DKFZ Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221/4214-01 Fax: +49 6221/4214-10 [email protected] www.life-science-lab.org Graduate Studies at the DKFZ Helmholtz International Graduate School for Cancer Research The Helmholtz International Graduate School for Cancer Research is the PhD Program of the German Cancer Research Center. The Graduate School has approximately 500 members, from all divisions and research groups of the center. Through the Graduate School, PhD students receive world-class training in interdisciplinary cancer research in preparation for a successful career in science. Members are recruited bi-annually from around the world through a highly competitive and stringent selection procedure. A core feature of the Graduate School is committed to scientific supervision of graduate students through annual Thesis Advisory Committees (TACs), consisting of the student’s PhD supervisor and at least two other senior scientists, one of whom is external to the German Cancer Research Center. The TAC meetings monitor the student’s progress, offer feedback on research already conducted and discuss any other issues, which might be relevant to the student’s work. Graduate students are further supported through a comprehensive training program, starting with a one-week “initial course” during the first months of their PhD and further professional training throughout their PhD through scientific and soft-skills courses, lecture series and careers seminars. Each student also takes part in the graduate studentorganized PhD retreat in their second year, including, in addition to a scientific program, career talks external speakers and talks from student guests of international collaborating institutes. The program of the Graduate School therefore ensures that throughout the PhD, scientific supervision, networking and coopera- Research at DKFZ 2014 tion between graduate students and leading scientists is facilitated at an international level. A further branch of graduate education, the German-Israeli Helmholtz Research School in Cancer Biology was established in 2012 in collaboration with the Weizmann Institute of Science in Rehovot, Israel. Research School graduate students work on joint scientific projects and are jointly supervised by a senior scientist from both the German Cancer Research Center and the Weizmann Institute. All projects include an extended research stay at the partner institute, during which time the graduate students have full access to the resources and services of the partner through integration into the respective graduate schools. Annual meetings, joint workshops and on-going seminar series and courses of the Research School ensure a continuous exchange between the partners. If you are interested in finding out more about the opportunities for graduate studies at the German Cancer Research Center, then please visit our website: www.dkfz.de/phd Manager of the Graduate and Research Schools: Dr. Lindsay Murrells Contact: [email protected] 15 Cancer Information Service National Reference Center for Cancer Information The Staff Physicians who have received special training in health communication answer telephone and email inquiries. Science journalists and scientific staff from the areas of medicine, pharmacy, biosciences and psychology are responsible for literature and information searches and editing. The Cancer Information Service has been established at the German Cancer Research Center since 1986. Its aim is to offer up-to-date cancer information to cancer patients, their families and friends, and to other interested members of the public in Germany. Additionally, the service reaches out to health professionals involved in the care and support of cancer patients. The Cancer Information Service answers individual questions on all cancer-related topics: causes and risk factors, prevention and early detection, diagnosis, treatment and followup care. In addition, the Cancer Information Service supplies contact details of institutions and organizations involved in medical and psychosocial care and support of cancer patients. All information is evidence-based, comprehensive, readily understandable and tailored to individual needs. Publicly funded by the Federal Ministry of Education and Research, the service’s information is neutral and independent. 16 The Cancer Information Service can be reached through different channels – via telephone, e-mail and its very informative up-to-date homepage. The service also issues various brochures and fact sheets on relevant topics. At the National Center for Tumor Diseases (NCT) Heidelberg and at the University Cancer Center (UCC) Dresden, the Cancer Information Service offers face-to-face counseling. • The telephone service is available daily from 8 a.m. to 8 p.m. at +49 6221 999 8000. Calls within Germany (Phone: 0800 420 30 40) are toll-free. • All email inquiries to [email protected] or via the secured e-mail form on the website are answered within two working days. • On its website www.krebsinformationsdienst.de, the Cancer Information Service provides information on a multitude of topics: new research findings, up-to-date scientific knowledge in oncology, useful tips for cancer patients, contact information, and links to further quality assured information resources. Prospects The high demand for quality assured cancer information will continue to grow due to demographic trends, rising cancer incidence and the introduction of novel clinical therapeutic options.. Particular emphasis is placed on the development of special information offerings for health professionals. Both strong integration into the German Cancer Research Center and utmost commitment to evidence-based, quality-tested cancer information are prerequisites for the development of the Cancer Information Service into a National Reference Center for Cancer Information. Performance Figures 2012 Inquiries answered total 29,371 By telephone 23,682 By email 3,737 By telephone and email 485 Letters 1,379 Face-to-face counseling 88 Website visitors per month 230,000 in average Cancer Information Service Head of Division: Dr. Susanne Weg-Remers Phone: +49 6221 999 8000 Phone: 0800 420 30 40 Daily from 8 a.m. to 8 p.m. Toll-free within Germany [email protected] www.krebsinformationsdienst.de Unit Cancer Prevention WHO Collaborating Centre for Tobacco Control In 2002, the Cancer Prevention unit was designated a World Health Organization Collaborating Centre (WHO-CC) for Tobacco Control, with the objective of making a noticeable contribution to national and international efforts to curb tobacco consumption. Its three main aims are to prevent the onset of smoking, to help smokers to quit, and to protect the population against secondhand smoke. Since the establishment of the WHO-CC, several measurable results have been achieved. Legislation for the protection of non-smokers from secondhand smoke was introduced; one Federal Law and 16 State Laws in 2007/2008 are based on the Centre’s scientific groundwork. Several other national tobacco control policies have been implemented, for which the WHOCC for Tobacco Control developed recommendations. Furthermore, the WHO-CC for Tobacco Control elaborated guidelines for implementation of Article 12 (education, communication, training and public awareness) of the WHO Framework Convention on Tobacco Control (WHO-FCTC). In order to increase the evidence base for tobacco control policies, the WHO-CC collaborates with the International Tobacco Control Policy Evaluation Project (ITC). As an ongoing cohort study, the ITC project follows smokers and non-smokers for several years and can thus monitor the effects of tobacco control measures on individual attitudes and behaviour. Significant accomplishments of the past years: The WHO-CC: • demonstrated that in 2007, 106,623 deaths were attributable to cigarette smoking in Germany and that there was a north-south gradient regarding the tobacco-attributable mortality rate (Gesundheitswesen 2010, doi:10.1055/s-0030-1252039). • showed that numerous tobacco additives are increasing the attractiveness and palatability of cigarettes as well as the health risks of smoking (SCENIHR. Addictiveness and attractiveness of Tobacco Additives.12 November 2010, http:// ec.europa.eu/health/scientific_committees/emerging/docs/scenihr_o_031. Research at DKFZ 2014 • • • pdf; Public Information Tobacco Control (PITOC), http://www.dkfz.de/de/tabakkontrolle/PITOC_Additives_in_Tobacco_ Products.html). published data on menthol capsules in cigarette filters showing that they are attractive to young people, thus promoting smoking initiation. Based on this scientific evidence a German court prohibited the introduction of cigarettes with menthol capsules on the German market (German Cancer Research Center (Ed.), Menthol Capsules in Cigarette Filters – Increasing the Attractiveness of a Harmful Product, Heidelberg, Germany, 2012; Verwaltungsgericht Braunschweig (2012) Urteil Az. 5 A 206/11). showed that public smoking bans promote smoking reduction at home (Mons U, Nagelhout GE, Allwright S, Guignard R, van den Putte B, Willemsen MC, Fong GT, Brenner H, Pötschke-Langer M & Breitling LP (2013) Impact of national smoke-free legislation on home smoking bans: findings from the International Tobacco Control Policy Evaluation Project Europe Surveys. Tob Control 22(e1): e2-9). disclosed the German Cigarette Industry Organization’s role in obstructing the development and implementation of effective tobacco control policies in Germany • • • (Gesundheitswesen 2008, 70:315-24). published the first National Tobacco Atlas Germany 2009, an illustrative education handbook on the social, health and economic aspects related to tobacco and its use (Tabakatlas Deutschland 2009, 2009, Steinkopff Verlag). published German language text and comments, in collaboration with the German Ministry of Health, on the WHO Framework Convention of Tobacco Control and recommendations for Germany (Perspektiven für Deutschland: Das Rahmenübereinkommen der WHO zur Eindämmung des Tabakgebrauchs – FCTC, 2011, DKFZ). published the first report worldwide on e-cigarettes showing the ambivalent character of these products (German Cancer Research Center (Ed.), E-cigarettes – an overview. Heidelberg, Germany, 2013). German Cancer Research Center Unit Cancer Prevention WHO Collaborating Centre for Tobacco Control Head of Department: Dr. Martina Pötschke-Langer Im Neuenheimer Feld 280 D-69120 Heidelberg Phone: +49 6221-423008 Fax : +49 6221-423020 [email protected] 17 DKFZ Career Service Scientific Life beyond the Lab The DKFZ Career Service aims to support all Masters, PhD students and postdocs at DKFZ in the planning of their professional future. The Career Service provides career-related workshops and conferences, personal coaching and advice, and expansion of the career network by following up with scientists after their stay at DKFZ. Sharing experience with scientists in academia, industry and beyond is a great help to make informed decisions about one’s own career. At career days PhD students and postdocs, with the support of the Career Service, invite scientists with interesting career paths for a short presentation and panel discussion. Further career seminars are coordinated together with other Heidelberg institutions so that, at least once per year, it is possible to meet scientists with careers in academia, industry, R&D, consulting, publishing, research management, patenting, teaching, etc. The Career Service organizes workshops on e.g., application skills, CV writing, networking “Career Plan B (Life/Work Planning)”, soft skills, business for scientists etc. A detailed overview can be found in the chapter “Scientific Career Development/Service” in the DKFZ Advanced Training Program. PhD students and postdocs from DKFZ can make an appointment for a personal and confidential conversation of 45 minutes with our Career Advisor, Dr. Barbara Janssens. There they can discuss their specialty, competencies, possibilities and career planning. Furthermore, they can get information on how and where to look for professional possibilities, application advice, or preparation for their application or interview. 18 You are very welcome to join the DKFZ Alumni Network both while working at DKFZ and after leaving. You can apply for a free email address which will forward messages to your private email, so you can be contacted under first. [email protected]. Additionally, we warmly invite you to join our DKFZ group on the professional social media network LinkedIn. This is a group of current and past members of the DKFZ where you can search and connect with scientists working in an area that interests you. Search for the group “DKFZ Career Network” on LinkedIn and join this open group and, relevant to your status, request membership of the subgroup “Currently@DKFZ” or “DKFZ Alumni”. Finally, the career service supports extensive yearly surveys from and for PhD students and postdocs to ascertain the status quo, questions and needs concerning young researchers´scientific careers. Career Manager: Dr. Barbara Janssens is Belgian (PhD in molecular/cell biology Ghent University), did a postdoc in Paris and worked five years as an editor at Wiley-Blackwell. Project Coordinator: Marion Gürth studied biology at the TU Darmstadt, worked as a Research Assistant at Heidelberg University and as a freelance website translator. Office H1.06.015b (15b 6th floor main building west) at the Graduate Program Office M070 www.dkfz.de/careers Technology Transfer at DKFZ – From Patents to Products to Patients The Office of Technology Transfer at DKFZ works at the interface between research and industry, building relationships between academic and industrial partners, e.g. collaboration agreements, license agreements and spinoffs. Founded in 1997 and headed by molecular biologist Dr. Ruth Herzog, the office is tasked with accelerating innovations that will create value from DKFZ’s research for the benefit of society and patients. The team supports DKFZ scientists in patenting and finding a suitable industrial partner for their new inventions and projects. The options chosen, in consultation with the scientist, may involve licensing, collaborating with established companies or starting a new company. As a rule, revenues from licenses are shared with the inventors and plowed back into cancer research. Ruth Herzog explains: “Only with patented inventions can we get partners to invest in developing DKFZ’s technologies into drugs, medical products or instruments. Pharma partners in particular must be able to count on the exclusivity they get from patent protection to recoup the huge sums they spend on research and clinical development of a new cancer drug.” Although the failure rate in this business is high (due to high costs and tough competition), the Office has helped to produce a number of success stories: 1. DKFZ was instrumental in developing a vaccine to prevent cancer Two vaccines provide protection against human papilloma viruses associated with the development of cervical cancer and are the DKFZ’s best known invention to date. Professor Harald zur Hausen was awarded the 2008 Nobel Prize for Medicine for research that led to this development. 2. DKFZ’s research has produced spin-off companies Spin-offs are important partners paving the road to commercialization. Take MTM laboratories AG, for instance. This publicly traded company for in vitro diagnostics Research Research at DKFZ at DKFZ 2013/2014 2014 3. was acquired by Roche in 2011 and is now part of the Roche Tissue Diagnostics unit (Ventana Medical Systems, Inc.). Apogenix, another DKFZ spin-off and a biopharmaceutical company developing novel protein therapeutics for the treatment of cancer and inflammatory diseases, has successfully completed the phase II study for its lead compound Apocept™ for the second line treatment of glioblastoma. DKFZ has built strategic alliances with industry The strategic and translational alliance with Bayer Healthcare draws on the strengths of both partners and thus accelerates the process from “bench to bedside”. Recently, DKFZ and Bayer agreed to work more closely together in the field of immunotherapy in a joint laboratory in Heidelberg. Equally important is the alliance with Roche and the Heidelberg University Hospital in the field of personalized medicine, in a venture that spans research collaboration and clinical studies. Dr. Ruth Herzog, M.A., CLP Creating value from research. Head of the Office of Technology Transfer Phone: +49 6221/42-2955 Fax: +49 6221/42-2956 [email protected] 19 Heidelberg A Capital of Biomedical Sciences in Europe In the charming city of Heidelberg with its biomedical Campus Neuenheim DKFZ is surrounded by strong partner institutions. 20 Heidelberg University Heidelberg University, founded in 1386, is Germany’s oldest university and one of the strongest research universities in Europe. The successes in both rounds of the Excellence Initiative and in international rankings prove its leading role in the scientific community. In terms of educating students and promoting promising young academics, Heidelberg relies on its two strongest points: research-based teaching and outstanding, well-structured training for doctoral candidates. Heidelberg University is a comprehensive university with the full spectrum of subjects including medicine. It aims to strengthen the individual disciplines, to further interdisciplinary cooperation and to carry research results over into society and industry. Heidelberg also draws its strength from its cooperation with local non-university research institutions such as the DKFZ and the Max Planck Institutes. In addition, the university is tied into a worldwide network of research and teaching collaborations which give evidence of its marked global interconnectedness. Heidelberg University Hospital and Medical Faculty Heidelberg University Hospital is one of the largest and most prestigious medical centers in Germany. The Medical Faculty of Heidelberg University belongs to the internationally most renowned biomedical research institutions in Europe. Both institutions have the common goal of developing new therapies and implementing them rapidly for patients. With about 11,000 employees, training and qualification is an important issue. Every year, around 118,000 patients are treated on an inpatient basis and around 1.000.000 cases on an outpatient basis in more than 50 clinics and departments with 2,200 beds. Currently, about 3,500 future physicians are studying in Heidelberg; the reform Heidelberg Curriculum Medicinale (HeiCuMed) is one of the top medical training programs in Germany. European Molecular Biology Laboratory Heidelberg The European Molecular Biology Laboratory is a basic research institute funded by public research monies from 20 member states and associate member state Australia. Research at EMBL is conducted by approximately 85 independent groups covering the spectrum of molecular biology. The Laboratory has five units: the main Laboratory in Heidelberg, and Outstations in Hinxton (the European Bioinformatics Institute), Grenoble, Hamburg, and Monterotondo near Rome. The cornerstones of EMBL’s mission are: to perform basic research in molecular biology; to train scientists, students and visitors at all levels; to offer vital services to scientists in the member states; to develop new instruments and methods in the life sciences and to actively engage in technology transfer activities. Around 190 students are enrolled in EMBL’s International PhD programme. Additionally, the laboratory offers a platform for dialogue with the general public through various science communication activities such as lecture series, visitor programmes and the dissemination of scientific achievements. Max Planck Institute for Medical Research Heidelberg The institute was founded in 1930 as the Kaiser Wilhelm Institute for Medical Research, and was re-founded as a Max Planck Institute in 1948. Its original goal was to apply the methods of physics and chemistry to basic medical research, and it still works on fundamental biological questions that are of long-term medical significance. One main area of research is neurophysiology: What are the changes in the brain that underlie processes like learning and remembering? What does the threedimensional circuit diagram of the billions of nerve cells in the brain look like? How can the processes in nerve cells in the living brain be made visible through new microscopic methods? A second main area of research at the institute concerns the complex chemical reactions in living cells. These are performed by enzymes, and the research aims to determine the atomic structure of important enzyme molecules, particularly through the use of the newly available free-electron lasers (FELs) in difficult cases. 21 Core Facilities 22 CORE FACILITIES The DKFZ Core Facilities provide the infrastructure for excellence. Cutting-edge techniques and equipment are the foundation of high quality research. At each core unit, experienced scientific and technical staff members assist researchers in the planning, conduct and analysis of experiments. These services are available to all DKFZ members and visiting scientists. Research at DKFZ 2014 23 Core Facilities Genomics and Proteomics • Next Generation Sequencing Biomedical research increasingly depends on global molecular analyses of normal and diseased phenotypes. These include qualitative as well as quantitative investigations at the genome and proteome levels and are required to eventually achieve a mechanistic understanding of disease or to identify novel markers for diagnosis, prognosis or prediction. Central infrastructures are key components in such research processes, as these provide access to state-of-the-art technology platforms that are operated by dedicated personnel, thus overcoming redundant implementation of often demanding technologies within an institute. Accordingly, the Genomics and Proteomics Core Facility (GPCF) at DKFZ covers four major areas and provides professional services. • The genomics part of the facility operates one of Europe’s largest next-generation sequencing units and operates • within several national (e.g., DKTK) and international (e.g., ICGC) cancer genome projects, in addition to a variety of individual in-house projects. Gene expression profiling, genotyping and methylation analysis is carried out using array-based technologies, providing high throughput at reasonable cost. All these applications generate molecular profiles at the level of nucleic acids, providing information about genetic as well as epigenetic alterations in the disease context. Technologies in mass spectrometry and NMR are provided for qualitative and quantitative analysis of proteins, protein modifications and small molecules. These applications allow views of the activation states of signaling proteins in cancer pathways and help to generate mechanistic knowledge of tumor diseases. We further provide small and large-scale • technologies to analyze protein-protein interactions and interactions proteins have with other molecules. In the field of functional genomics, we generate monoclonal antibodies targeting proteins as well as cancer-relevant mutant variants. Some antibodies have been licensed and are now used in diagnosis. Cell lines stably expressing recombinant proteins from isogenic loci in the respective genomes are generated to assess phenotypes of proteins and mutants in in vitro as well as in vivo systems, e.g., via generation of xenograft mouse models for the molecular characterization of metastasis processes. The central infrastructure of the GPCF offers assisted access to a number of costly instruments being utilized by a number of scientific groups, and it further distributes the human ORF clone resource of the international ORFeome Collaboration for recombinant expression of encoded proteins, also in isogenic cell lines. Our mission is to enable the application of state-of-the-art technologies. We carry out joint projects with scientific groups within DKFZ to implement the latest technologies that serve science needs. In addition to providing full or assisted access to services, we are involved in the DKFZ teaching program. Furthermore, the GPCF organizes tech-talks, seminars and practical courses where we inform interested scientists, predocs and technicians on the technological background of novel applications. Head PROF. DR. STEFAN WIEMANN Units Next Generation Sequencing Microarray technologies Bioinformatics (HUSAR) Monoclonal Antibodies Protein Analysis Protein Interaction Screening Molecular Structural Analysis Isogenic Cell Line Technology 24 Core Facilities Imaging and Cytometry Biomedical research benefits greatly from imaging and cell enrichment processes, but scientific results in these fields are reliant upon the efficient and correct use of complex and expensive instrumentation. Dynamic progress in the development of such technology results in a constant requirement for new or updated equipment, as well as experienced staff members able to guarantee the correct, appropriate use of the instruments; execution of the experiments; and data management – all of which is time consuming. In order to minimize such investment of capital and personnel for individual groups, the DKFZ has established the Imaging and Cytometry Core Facility; made up of individual units, it provides a wide range of high quality services in four different fields for all DKFZ members and visiting researchers. Each unit is directed by a highly experienced scientist. The units are responsible not only for the allocation and maintenance of instruments, lab space and to some extent, consumables, but their scientific and technical staff also offers training and assistance in sample preparation, instrument application, experimental set-up design, interpretation of the results, and detailed, unit-specific seminars. Small Animal Imaging 1. 2. 3. Flow Cytometry The Small Animal Imaging unit supports clients with a variety of radiological methods, among them ultrasound, µPET, µCT, µSPECT and MRT, to collect and quantify morphological and functional data in vivo. The Flow Cytometry unit performs cell cloning or enrichment of up to 4 subpopulations simultaneously by using several flow cytometric cell sorters (up to 5 laser, cuvette and jet-in-air sorter), enabling analysis of up to 19 parameters per cell. The Light Microscopy unit provides a number of manual and fully automated wide-field and confocal laser-scanning microscopes. The range of services is sup- Light Microscopy 4. Electron Microscopy plemented by support in sample preparation (e.g. paraffin and cryo-sectioning, laser microdissection) and spatial visualization of whole-mount specimens, as well as data analysis and digital image processing. The Electron Microscopy (EM) unit offers full service and guided access in EM preparation and imaging, including conventional Epon-EM, low-temperature EM (high-pressure freezing, freeze substitution and cryo-sectioning), immuno-EM and single particle EM (negative staining, rotary shadowing). Head PROF. JÜRGEN KARTENBECK (IN CH.) Units Light Microscopy Facility Core Facility Electron Microscopy Small Animal Imaging Flow Cytometry Research at DKFZ 2014 25 Core Facilities Information Technology Information technology needs and requirements continue to increase at DKFZ. This is due, in particular, to modern laboratory technologies in areas such as genome analysis and radiological image processing, which generate huge amounts of data on a petabyte scale. Communication technology and office applications have penetrated our everyday work and the introduction of the electronic laboratory notebook has reinforced this trend. Furthermore, as more and more personal data are being processed, aspects of IT safety play an ever more important role in many departments of DKFZ and as a requirement in many national and international scientific projects and collaborations such as the German Consortium for Translational Cancer Research (DKTK). However, not only confidentiality and integrity of data are important, the availability of IT is also essential for scientific work. Therefore, redundant IT systems are needed in many places. IT has gained a pivotal role as an enabling technology in the life sciences and particularly in cancer research. The task of the Information Technology Core Facility (ITCF) is to optimize the use of information technology at DKFZ, to advise staff from all in-house departments in selecting IT tools for their specific needs in a general context, to implement and operate centralized IT services as well as to support the planning and operation of individual solutions. This is done on a service-oriented basis. All essential strategic and operative functions and tasks at DKFZ are substantially supported by IT. The Software Systems group provides central IT software systems for both client and server sides. These include, for example, central services such as user administration, software distribution and license monitoring, rights and resources management in file services, data base servers, web servers, document management and the electronic laboratory notebook. The Databases group is responsible for database development and support for all in-house departments. In addition, it provides technical support for DKFZ’s Internet and Intranet presentations as well as survey tools and cooperation platforms. The Desktop Services group runs the service center for user inquiries, deals with all matters related to the desktop environment such as notebooks, MacOS, Windows and mobile devices, and runs the high-quality printing center. Central servers, mail and file services, printing services, data storage as well as scientific computing are the tasks of the Central Servers group. The Networks group takes care of the physical data network, Internet connections, dedicated connections to partners, and security services. Head HOLGER HAAS Working Groups Software Systems Databases Desktop Services Central Servers Networks 26 Core Facilities Animal Laboratory Services Cancer represents a devastating disease. The mission of the DKFZ is research on the molecular mechanisms of carcinogenesis and the improvement and development of cancer therapies. Scientists at the DKFZ work, whenever possible, with cell cultures or try to answer scientific questions by computer simulation (replacement). In many cases, due to the complexity of tumorigenesis the significance of alternative in vitro or in silico systems is limited, so that animal experiments are indispensable. These are restricted to the minimum extent possible (reduction); animals are treated with respect and with the most advanced techniques (refinement). For their experiments, DKFZ scientists preferentially use rodents, in rare cases, amphibians also. To mimic the development of a distinct cancer in humans, cancer researchers employ various tumor models; genetically manipulated mice with a tissuespecific gain or loss of one or several genes serve to evaluate the functional role of such genetic factors in cancer development. To some extent, the mechanisms of tumor development are analysed in mice that have been treated with carcinogenic agents. To study the characteristics of human tumor cells, mice with a compromised immune system are often used, since they tolerate the transplantation of cells from other species and allow their growth. The staff of the DKFZ Animal Laboratory Services Core Facility supports scientists requiring animal organs or animals, bred in-house or selectively purchased, for experimentation. A team of clinical veterinarians and biologists advises and assists researchers in the design and realization of their experiments. Managers of the core facility train technicians and caretakers and provide technical courses for scientific personnel. By these means, it is assured that all animals are kept according to national and international animal welfare laws. In addition, the welfare of the animals is ensured by maintaining them under the most hygienic conditions. In the Laboratory of Microbiological Diagnostics and Animal Medicine, the health status of the animals is regularly checked (www.dkfz. de/en/abteilungen/v/v231.html). The Transgenic Service supports scientists at DKFZ in the generation of genetically modified mouse lines that serve for investigation of distinct human tumor diseases (www.dkfz.de/en/transgenservice/index.html). In the Cryopreservation Unit, the most important mouse strains are preserved for further studies by collecting spermatozoa or early-stage embryos from mutant mice and subsequent freezing in liquid nitrogen. In addition, a database of all mouse mutants available in-house is provided (www. dkfz.de/en/kryokonservierung/index.html). The Tumor Models Unit carries out cancer studies in experimental animals by application of carcinogenic agents and by transplantation of tumor cells into immune-deficient mice. Additionally, diet and therapy studies are carried out (www. dkfz.de/en/tumormodelle/index/html). Head PROF. DR. KURT REIFENBERG Units Tumor Models Cryopreservation Animal Laboratory Facility Microbiological Diagnostic and Laboratory Animal Medicine Transgenic Service Research at DKFZ 2014 27 Core Facilities Library amongst others, provided through the library’s website. Currently, the library offers access to more than 1000 e-journals. Monographs, reference books, laboratory handbooks etc. are available online, as well as in print. Publications that are not available from the library’s collection may be ordered through document delivery and thus made available. Several databases are offered by the library for literature searches. Here, the library offers individually customized trainings in databases like PubMed, Web of Science and SciFinder. The same is true for the bibliographic management software EndNote and Reference Manager. The library’s reading room The library’s reading room offers a quiet working space with wireless internet and the possibility of immediate help from the staff if needed. Due to technical development, research and scientific communication processes are currently facing large changes. Today, the flood of information is rising rapidly. If this information is used wisely in conjunction with ever-increasing projects, tools and programs, it will become a valuable addition to researchers. Here, the library is supporting the scientists in all aspects of “scientific information and communication”. The library’s team obtains the required scientific literature and information which is, We also offer assistance when questions involving bibliometric issues, citation analysis, open access or copyright arise. The library is also responsible for the DKFZ publications database. Currently, the library is working with scientists in order to expand the database to an institutional repository. Furthermore, the library is parenting the DKFZ archive. This archive collects and registers all documents regarding the history of the DKFZ. Head DAGMAR SITEK 28 Core Facilities Joint Chemical Biology Core Facility of EMBL & DKFZ Small inhibitory molecules are widely used as therapeutic agents, but they are also excellent “bio-tool” compounds for basic research. They are often used as experimental tools to address important biological questions via loss-of-function experiments. The aim of this core facility is to provide research groups with inhibitory molecules against their target of interest and enable them to answer essential questions in their research. The facility assists groups in the development of primary and secondary assays for screening against our in-house compound library and guides them through the process of identifying bio-tool compounds for their specific target. It also offers computational chemistry services. The Chemical Biology Core Facility is a collaboration between DKFZ, the European Molecular Biology Laboratory (EMBL) in Heidelberg and Heidelberg University, and is located at EMBL. For further information on this service, please visit the site: www.embl.de/services/core_facilities/chemcore/index.html Medicinal chemistry support is usually required following a small molecule screen. Here, the research group “Cancer Drug Development” headed by Dr. Aubry Miller offers assistance on a collaborative basis. Ligand docked into target protein Head DR. JOE LEWIS In cooperation with EMBL University of Heidelberg Research at DKFZ 2014 29 30 Research Programs RESEARCH PROGRAMS The DKFZ covers the entire breadth of modern cancer research. Fields of research range from knowledge of the molecular basis of the development of cancer, distribution and risk factors within the population to diagnosis and treatment. More than 100 division heads, group leaders and senior scientists, 200 postdocs and about 400 PhD students work together at the DKFZ. As an interdisciplinary environment, DKFZ employs scientists with qualifications in medicine, biology, biochemistry, physics, chemistry, mathematics, informatics or related issues. At DKFZ, researchers benefit from intensive scientific exchange between research programs and individual groups which serves as a basis for the internationally renowned research at the center. Research groups are organized in seven research programs: Cell Biology and Tumor Biology, Functional and Structural Genomics, Cancer Risk Factors and Prevention, Tumor Immunology, Imaging and Radiooncology, Infection and Cancer, and Translational Cancer Research. Research at DKFZ 2014 31 Coordinator PROF. DR. HELLMUT AUGUSTIN Cell Biology and Tumor Biology Research Program (FSP-A) concentrates the basic cell and tumor biology-focused research groups at the center. As such, the mission of the FSP-A groups is either the molecular, cellular and functional analysis of the mechanisms leading to tumor initiation, tumor promotion and tumor progression including metastasis or the pursuit of fundamental discipline-independent basic science. Scientists of the research program “Cell and Tumor Biology” aim at tackling these fundamental questions: • They investigate how genome stability is ensured, as inherited or acquired alterations in the genome are causative for tumor initiation and progression. The experimental program also focuses on epigenetic mechanisms and RNA biology. • They study cell surveillance and damage control mechanisms, which allow cells to monitor molecular processes and respond to pathologic damage. This includes the control of protein stability and turnover. • They unravel critical signaling pathways and networks which enable cells to perceive and correctly respond to information and to govern cellular processes. Scientists in this research program investigate how dysregulation of these mechanisms is linked to malignancies. • They analyze cell differentiation pathways and the biology of stem and progenitor cells taking into consideration that perturbed cell differentiation and dysregulated stem cell programs are at the heart of many oncological and non-oncological diseases. • They exploit the complexity of tumor cell interactions with their microenvironment to analyze a tumor not just as a clump of tumor cells leading to local disease but rather as a complex pathologic organ causing systemic disease. Metabolic changes are studied as risk factor and consequence of tumorigenesis and tumor progression. To tackle these questions, the scientists employ a broad array of highly specialized molecular, cellular and organismic tools and techniques. With scientific excellence being the primary recruitment criterion, outstanding groups are affiliated with the FSP-A. Thus, their cutting-edge basic cell and tumor biology research establishes the knowledge-based foundation for the rational translation and exploitation into medical application for some of the most devastating human diseases. For a conceptually broader basic science appreciation beyond its primary tumor biology focus, DKFZ’s cell and tumor biology research program is part of the DKFZ-ZMBH-Alliance, a strategic partnership between the FSP-A and the Center for Molecular Biology of Heidelberg University (ZMBH) which was established in 2007 in order to overcome the classical boundaries between the two strong university and non-university institutions on the Heidelberg campus. Details about research projects of the individual FSP-A research groups can be found on the respective pages. 32 Research Program Genetically stably multicolor labelled tumor cells for tumor cell heterogeneity and biological competition experiments Research at DKFZ 2014 33 Cell and Tumor Biology Stem Cells and Cancer Division Head: Prof. Dr. Andreas Trumpp Stem Cells and Cancer (A010) Managing Director of the Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3901 [email protected] The adult bone marrow harbors a reservoir of dormant HSCs. Although dormant HSCs do not contribute to the day-to day generation of new blood cells, they are efficiently and reversibly activated in response to bone marrow stress induced, for example, by chemotherapeutic agents (5-FU) or toxic substances (such as BrdU). Stem cells are essential to maintain regenerative tissues and are critical components of repair in response to tissue injury and infection. Moreover, genetic alterations of stem cells and their progeny can lead to the generation of “cancer stem cells” (CSCs) that drive tumorigenesis and metastasis in hierarchically organized cancer entities. Due to their remarkable resistance to chemotherapy and radiation, CSCs are thought to be responsible for tumor re-occurrence and the initiation and maintenance of metastases. One of the goals of our program is to elucidate the molecular and cellular basis of hematopoietic stem cell (HSC) self-renewal and differentiation. We have recently shown that the most potent HSCs during homeostasis are in a state of deep dormancy. In response to stress signals which can be mediated by bacterial (LPS) or viral infections (Interferons) or by chemotherapy mediated cell loss, these dormant HSCs become activated to produce new stem cells and progenitors (Figure). Using genome-wide transcriptomics, proteomics and methylome analysis (in collaboration with Prof. Christoph Plass), we have recently established the molecular landscape of HSCs and various progenitors in the bone marrow to understand the molecular basis of self-renewal and multipotency, as well as the complex dynamic interactions between stem cells and their niche. In addition, the group has established a program to functionally characterize malignant stem cells of leukemias and carcinomas at various levels. For example, we have developed methods to isolate blood circulating “metastasis initiating cells” (MICs) directly from the peripheral blood of breast cancer patients and characterized them function- ally by transplanting them into immunocompromised mice. These studies revealed the identification of MICs, which have an EPCAM+CD44+MET+CD47+ phenotype and are able to initiate new bone and lung metastasis. Moreover, the number of these MICs in the blood of patients correlated with overall survival and offers novel possibilities for the design of better diagnostic and therapeutic tools for metastatic breast cancer. We have also identified novel subclasses of pancreatic cancer and developed biomarkers to identify them. Stratification of patients according to the subtypes revealed striking differences in their overall survival and tumor cells isolated from these patients show differential sensitivity to conventional and targeted therapies. Next generation sequencing and molecular characterization of subtype specific cancer and metastasis stem cells will provide the basis for the generation of novel diagnostic and therapeutic tools to target advanced therapy resistant cancers including metastasis. Future Outlook: The “Stem Cells and Cancer” Division characterizes both normal and malignant stem cells functionally using in vivo approaches. We then use genomic, genetic, molecular and cellular methods to uncover the mechanisms which control and drive normal and uncontrolled self-renewal. Starting with model systems, we typically extend our work to the analysis of primary patient derived samples (blood, bone marrow, tumor samples, metastasis) with the goal of developing innovative strategies to detect and target cancer and metastasis stem cells in clinical settings. ESSENTIAL PUBLICATIONS: (1.) Baccelli I. et al. (2013). Identification of a population of blood circulating tumor cells from breast cancer patients that initiates metastasis in a xenograft assay. Nature Biotechnology, 31, 539–544. (2.) Essers MAG. (2009). IFNa activates dormant HSCs in vivo. Nature, 458, 904–908. (3.) Wilson A. et al. (2008). Hematopoietic stem cells reversibly switch from dormancy to self-renewal during homeostasis and repair. Cell, 135, 1118–1129. (4.) Trumpp A. (2010). Awakening dormant haematopoietic stem cells. Nature Rev Immunol, 10, 201–209. 34 Research Program Cell and Tumor Biology Molecular Embryology Division Head: Prof. Dr. Christof Niehrs Analyses of the molecular processes taking place during embryonic development have shown that the principles guiding embryonic development in humans and in animals are very similar on a molecular level. Today it is known that genes involved in the development also play a role in human diseases. The Division of Molecular Embryology is studying mechanisms regulating cell differentiation. The aim is to characterize molecular mechanisms relevant for the formation of the body axis in frogs and mice. To this end, we are identifying developmental control genes and investigating how these are regulated and what their functions are. Our special interest is investigating the mechanisms of the Wnt signaling pathway in this context. Future Outlook: Future research is aimed at identifying novel Wnt pathway components, to study their role and mechanism of action. ESSENTIAL PUBLICATIONS: (1.) Cruciat CM. et al. (2013). RNA helicase DDX3 is a regulatory subunit of casein kinase 1 in Wnt-βcatenin signaling. Science, 339: 1436–1441. (2.) Bilic J. et al. (2007). Wnt induces LRP6 signalosomes and promotes dishevelled-dependent LRP6 phosphorylation. Science, 316, 1619–1622. (3.) Davidson G. et al. (2005). Casein kinase 1 couples Wnt receptor signaling to the cytoplasmic transduction apparatus. Nature, 438, 867–872. (4.) Glinka A. et al. (1998). Dickkopf-1 is a member of a new family of secreted proteins and functions in head induction. Nature, 391, 357–362. Molecular Embryology (A050) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4693 [email protected] Two-headed Xenopus embryo following experimental overstimulation of the head inducer Dickkopf 1. Research at DKFZ 2014 35 Cell and Tumor Biology Signal Transduction and Growth Control Divison Head: Prof. Dr. Peter Angel Signal Transduction and Growth Control (A100) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4570 [email protected] The Division is working on the characterisation of the genetic response of organisms and their cells to external signals (growth factors, inflammation-related cytokines, carcinogens and tumor promoters) employing newly generated genetically modified mouse models (which replicate features of human diseases) and celland organ cultures derived thereof. We want to define and characterize altered gene functions, which result in imbalanced signaling pathways and downstream genetic programs forming the basis for acquired capabilities of uncontrolled cell growth, evasion of apoptosis, sustained angiogenesis and finally enhanced tissue invasion and metastasis. To date and currently, we have applied genetically modified animal models, in vitro organ systems, and genome-wide expression analyses in order to decipher the individual functions of AP-1 subunits. Our study of individual AP-1 subunits, of their regulation as well as the identification of distinct targets genes and genetic programs critically involved in cancer development and progression has yielded major contributions to our current understanding of genetic programs in physiological (e.g. embryogenesis, vascular biology/angiogenesis, wound healing) and pathological processes (chronic inflammation, tumorigenesis). In collaboration with clinical partners these studies, accompanied by analyses of human tumor samples, aim ultimately to define novel molecular markers for diagnosis and therapeutic intervention. state-of-the-art methods including modified transgenic mice, various tumor models, interspecies heterologous co-culture cell systems, genome-wide expression and epigenetic analyses combined with systems biological approaches, and molecular and cellular biology to study tumor-relevant genetic networks. We will focus on mechanisms of cell-cell communication in wound healing, and cross-talk between tumor cells and cells of the microenvironment (endothelial-, mesenchymal- and immune cells). The main attention will be focused on (soluble) mediators of cell communication as well as downstream signalling pathways and genetic programs initiated in the corresponding target cells. The main projects concern: 1. Physiology and pathology of wound healing: controlling genetic programs of cell proliferation, migration and differentiation. 2. Function of the cell surface protein podoplanin in brain and skin tumors. 3. Genetic and epigentic programs of tumor angiogenesis and vessel physiology; role of the tumor stroma. 4. Function of the cell surface receptor RAGE and its ligands (S100 proteins) in the regulation of genetic programs in inflammation and cancer. ESSENTIAL PUBLICATIONS: (1.) Szabowski A. et al. (2000). c-Jun and JunB antagonistically control cytokine-regulated mesenchymal- Future Outlook: With the goal to bridge basic science and translational research, in collaboration with partners at the DKFZ, University Heidelberg and external partners, our program will focus on intra- and intercellular signaling pathways and downstream genetic programs in cancer to develop and evaluate molecules as potential biomarkers or drug targets. We will utilize epidermal interaction in skin. Cell 103, 745–755. (2.) Hess J. et al. (2004). Functions of AP-1 subunits: Quarrel and Harmony among Siblings. J. Cell Sci 117, 5965–5973. (3.) Gebhardt C. et al. (2008) RAGE signaling sustains inflammation and promotes tumor development; J Exp Med 205, 275–285. (4.) Licht A.H. et al. (2010). Junb regulates arterial contractility and cellular migration via its direct target Myl9, J Clin Invest 120, 2307–2318. 36 Research Program Immunohistological analysis of a mouse liver tissue section showing induction of liver progenitor cells (red) in response to chronic liver damage in a murine model of inflammation driven liver carcinogenesis. Research at DKFZ 2014 37 Cell and Tumor Biology Epigenetics Division Head: Prof. Dr. Frank Lyko Epigenetics (A130) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3800 [email protected] Epigenetic mechanisms regulate the interpretation of genetic information and adapt gene expression patterns to changing developmental or environmental contexts. Several epigenetic mechanisms have been identified so far, with DNA cytosine methylation representing the best-studied and possibly most relevant epigenetic mark. Interestingly, cytosine methylation is also present in RNA, suggesting a conserved epigenetic function of DNA and RNA methylation. Our research focuses on understanding the biological function of cytosine methylation as a versatile epigenetic mark. Importantly, altered DNA methylation patterns represent one of the earliest and most consistent hallmarks of human cancers. However, the factors that shape the tumor methylome remain poorly understood. We are using next-generation sequencing technologies to analyze DNA methylation and hydroxymethylation patterns on the genome scale, with a particular focus on mouse tumor models. We have also established a novel research focus on RNA methylation, which suggests that this modification plays a key role in epigenetic regulation and inheritance. Finally, we are using several unique model systems, such as honeybees, locusts and crayfish, to better understand the role of epigenetics in ecological adaptation and phenotypic plasticity. Future Outlook: The division will continue its focus on three major topics: cancer epigenetics, RNA epigenetics and ecological epigenetics. To identify the driving forces behind cancer-associated epigenetic mutations, we will continue to develop our bioinformatics toolkit for the characterization of cancer epigenomes. To further establish RNA methylation as a fundamentally novel epigenetic mechanism, we will explore the role of this modification in protein translation and small RNA silencing pathways. Finally, we will further analyze the role of DNA methylation in ecological adaptation by establishing marbled crayfish as a novel model system for epigenetics research. ESSENTIAL PUBLICATIONS: (1.) Raddatz, G., et al. (2012). Dnmt3a protects active chromosome domains against cancer-associated hypomethylation. PLoS Genetics, 8, e1003146. (2.) Tuorto, F., et al. (2012). RNA cytosine methylation by Dnmt2 and NSun2 promotes tRNA stability and protein synthesis. Nature Structural and Molecular Biology, 19, 900–905. (3.) Lyko F. et al. (2010). The honey bee epigenomes: differential methylation of brain DNA in queens and Microscopic image of cancer stem cells expressing EGFP under the control of the OCT4-promoter. 38 Research Program workers. PLoS Biology, 8, e1000506. (4.) Schaefer M. et al. (2010). RNA methylation by Dnmt2 protects transfer RNAs against stress-induced cleavage. Genes & Development, 24, 1590–1595. Cell and Tumor Biology DNA Repair Mechanisms and Cancer Junior Research Group Head: Dr. Hans Hombauer The maintenance of the genome integrity represents an important challenge for every living organism. A variety of factors of environmental origin (chemicals, radiation, viruses, etc), but also others intrinsic to the cellular metabolism (i.e. oxidative species, DNA replication errors) are frequently damaging/altering the information of the DNA. Changes in the genetic information (mutations) are the cause of several human diseases, including cancer. Not surprisingly, living organisms have developed a variety of DNA repair mechanisms that in a concerted manner safeguard the stability of the genome. Our research group investigates the molecular mechanisms that allow DNA repair pathways to preserve genome stability, specifically the DNA mismatch repair (MMR) pathway. This pathway is a post-replicative repair mechanism that increases DNA replication fidelity (to about three orders of magnitude) by recognizing errors introduced during DNA replication, and promoting repair by an excision and re-synthesis mechanism. Mutations that inactivate MMR result in Lynch Syndrome, also referred to as Hereditary Non-Polyposis Colorectal Cancer (HNPCC). This syndrome is characterized by genome instability, especially at repetitive sequences or microsatellites (microsatellite instability or MSI) and early-onset of colorectal and other types of cancer. Furthermore, we are interested to identify and characterize alternative mechanisms that can result in MMR inactivation, and how specific missense mutations inactivate MMR function in a dominant manner. These studies might reveal why specific MMR missense mutations result in different degrees of cancer manifestation (i.e. early-onset, high penetrance, relapse). Moreover, our future work aims at the identification and characterization of previously unrecognized genes that affect DNA replication fidelity and repair. We expect that some of these thus identified genes will at a future date become essential diagnostic tools in cancer susceptibility syndromes. ESSENTIAL PUBLICATIONS: (1.) Hombauer H. et al. (2011). Visualization of Eukaryotic DNA Mismatch Repair Reveals Distinct Recog- DNA Repair Mechanisms and Cancer (A310) nition and Repair Associated Intermediates. Cell, 147, German Cancer Research Center 1040–1053. Im Neuenheimer Feld 581 (2.) Hombauer H., et al. (2011). Mismatch repair, but not heteroduplex rejection, is temporally coupled to 69120 Heidelberg replication in Saccharomyces cerevisiae. Science, 334, Phone:+49 6221 42-3239 1713–1716. [email protected] (3.) Jaehnig E., et al. (2013). Checkpoint kinases regulate a global network of transcription factors in response to DNA damage. Cell Reports, 4, 174–188. (4.) Smith C. et al. (2013). Dominant mutations in Saccharomyces cerevisiae PMS1 identify the Mlh1-Pms1 endonuclease active site and an Exonuclease 1-in- Future Outlook: We are interested in expanding the mechanistic understanding of the MMR reaction by identifying and characterizing mutations/ genes that prevent the accumulation of mutations. To learn more about these processes, we combine genetics, molecular and cell biology approaches in S. cerevisiae and mammalian tissue culture. Our studies aim to characterize the mechanistic aspects of the MMR reaction, in particular, the MMR repair intermediate Mlh1-Pms1 (Mlh1-Pms2 in humans), which we have recently identified as active sites of repair in budding yeast. Research at DKFZ 2014 dependent mismatch repair pathway. PLoS Genetics, in press. Visualization of Mismatch repair Mlh1Pms1 complexes in wild-type (A) and exo1Δ mutant (B) in living yeast cells. Deletion of EXO1 results in increased abundance of Mlh1-Pms1 foci (some foci examples are indicated with white arrows). 39 Cell and Tumor Biology Redox Regulation Division Head: PD Dr. Tobias P. Dick Redox Regulation (A160) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2320 [email protected] Elevated generation of oxidants (reactive oxygen species) is associated with inflammation and many age-related disorders, including malignancy. Correspondingly, oxidants have been generally regarded as unwanted and damaging products. However, more recently it has become clear that some oxidants, in particular hydrogen peroxide (H2O2), also play beneficial roles as signaling molecules in healthy cells. Oxidants regulate adaptive stress responses and cell fate decisions through post-translational modification of transcription factors and other target proteins. In particular, the signaling functions of oxidants are typically based on the reversible oxidation of protein thiol residues, leading to transient activation or inactivation of individual enzymes. In our laboratory we are investigating signaling pathways by which H2O2 contributes to the regulation of cellular physiology. We are interested in the nature of redox alterations that accompany chronic inflammation and malignant growth. Special attention is devoted to the molecular mechanisms by which oxidants achieve specificity as signaling molecules. Another area of focus is to uncover the spatio-temporal dynamics of oxidative processes in vivo. detailed understanding of these differences may lead to new ideas as to how to interfere with tumor growth. Molecular mechanisms of oxidative signaling: How are H2O2-sensitive signaling proteins oxidized in an efficient and specific manner? Growing evidence suggests that certain peroxidases act as primary oxidant receptors and pass on oxidizing equivalents to specific target proteins. Monitoring redox changes in cells, tissues and organisms: We recently developed geneticallyencoded biosensors for oxidized glutathione and H2O2. A major application is to monitor redox processes as they occur in the physiological context of the whole organism. Fundamental principles of redox homeostasis: The glutathione system is central to eukaryotic redox homeostasis and drug resistance but remains incompletely understood. We are combining redox imaging and reverse genetics in the model eukaryote S. cerevisiae to reveal the fundamental regulatory principles of the glutathione system. ESSENTIAL PUBLICATIONS: (1.) Morgan, B. et al. (2013). Multiple glutathione di- Future Outlook: The role of H2O2 sensing and signaling in inflammation: H2O2 is released during tissue injury and may act as one of the early signals for the recruitment and activation of immune cells. Recently, we identified H2O2-sensitive proteins involved in inflammatory signaling. Our aim is to elucidate the specific links between inflammatory activators, H2O2 and immune effector mechanisms. Redox homeostasis in tumor cells: Many, if not most, tumor cells differ in redox homeostasis compared to their normal counterparts. More Redox-sensitive cysteine residues (yellow) can act as molecular switches. 40 Research Program sulfide removal pathways mediate cytosolic redox homeostasis. Nature Chemical Biology, 9, 119-125. (2.) Albrecht S.C. et al. (2011). In vivo mapping of hydrogen peroxide and oxidized glutathione reveals chemical and regional specificity of redox homeostasis. Cell Metab, 14, 819–829. (3.) Gutscher M. et al. (2008). Real-time imaging of the intracellular glutathione redox potential. Nat Meth, 5, 553–559. (4.) Kienast A. et al. (2007). Redox regulation of peptide receptivity of major histocompatibility complex class I molecules by ERp57 and tapasin. Nat Immunol, 8, 864–872. Cell and Tumor Biology Molecular Metabolic Control Division Head: Prof. Dr. Stephan Herzig The department “Molecular Metabolic Control” is a common research unit between the German Cancer Research Center (DKFZ), the Center for Molecular Biology (ZMBH) at the University of Heidelberg and the University Hospital Heidelberg. The department is investigating the molecular basis of severe metabolic disorders, including the Metabolic Syndrome and type 2 diabetes, and their roles in tumor initiation and progression. The main causes of these metabolic disorders are believed to be malfunctions in the activity of genes regulating our metabolism. By analyzing the signaldependent activity of such genes in response to hormonal, nutritional and inflammatory cues, we aim to define disease-causing malfunctions in glucose, fat and protein metabolism, ultimately aiming at the identification of genes and gene products which increase the susceptibility to metabolic diseases. Subsequently, identified gene defects are tested for their potential to serve as molecular connections between metabolic and tumor diseases and as potential novel drug targets within these disease entities. Thus far, we have already characterized a number of molecular switches that are dysregulated under certain metabolic conditions and promote aberrant metabolism in diabetes and cancer. Future Outlook: In the future, we will address the question if and how the differential recruitment of specific transcriptional complexes to genomic target sites provides a molecular relay station for nutritional, hormonal and inflammatory signals in the control of energy homeostasis and the pathogenesis of aging-associated diseases, including diabetes and cancer. Specifically, we will investigate whether and how relevant transcription factor complexes bridge metabolism, inflammation and tumor development through the integrated control of metabolic pathways, inflammatory responses, and cell fate decisions. By using a translational research approach, we anticipate unravelling clinically significant Research at DKFZ 2014 molecular determinants in the pathogenesis of the Metabolic Syndrome and type 2 diabetes that are directly coupled to an increased cancer risk in these patients, thereby serving as potential new therapeutic targets in metabolic disorders. In particular, we will focus on three main areas 1. Transcriptional networks, systemic lipid distribution, and lipotoxicity 2.Molecular integration of inflammation and metabolism 3.Brown adipocyte stem cells and control of energy homeostasis ESSENTIAL PUBLICATIONS: (1.) Kulozik Ph. et al. (2011). Hepatic deficiency in transcriptional co-factor TBL1 promotes liver steatosis and hypertriglyceridemia. Cell Metabolism, 13, 389– 400. (2.) Vegiopoulos A. et al. (2010). COX-2 controls ener- Molecular Metabolic Control (A170) gy homeostasis in mice by de novo recruitment of German Cancer Research Center brown adipocytes. Science, 328, 1158–1161. Im Neuenheimer Feld 280 (3.) Lemke U. et al. (2008). The glucocorticoid receptor controls hepatic dyslipidemia through Hes1. Cell Me- 69120 Heidelberg tab., 8, 212–223. Phone: +49 6221 42 3581 (4.) Herzig S. et al. (2001). CREB regulates hepatic glu- [email protected] coneogenesis through the coactivator PGC-1. Nature, 413, 179–183. Lipid droplets (red) in adipocytes serve as main energy supply for the body. 41 Cell and Tumor Biology Vascular Oncology and Metastasis Division Head: Prof. Dr. Hellmut Augustin Vascular Oncology and Metastasis (A190) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 1500 [email protected] The Augustin laboratory studies the complexity of interactions occuring between tumor cells and blood and lymphatic vessels during tumor progression and metastasis, most notably as it relates to the growth of blood vessels in tumors. Angiogenesis, the sprouting of new blood vessels from existing vessels, is an oncofetal process that occurs physiologically during development and postnatal growth, but in adults is mostly restricted to pathological processes, which makes angiogenesis an attractive target. Angiogenesis is characterized by a distinct cascade of molecular and cellular events, which enable cells of the vessel wall (endothelial cells) to sprout from a pre-existing capillary and to form new lumenized capillaries which anastomose to form a vascular network that matures over time with the recruitment of perivascular mural cells (smooth muscle cells, pericytes). Molecules of the Angiopoietin/Tie ligand/receptor family play central roles in these processes. Our scientists study the molecular mechanisms of Angiopoietin/Tie signaling in blood and lymphatic vessels and analyze the molecular and functional properties of endothelial cells and pericytes during physiological and pathological angiogenesis and vessel remodeling. Given the critical roles of blood and lymphatic dysfunction for numerous oncological and non-oncological diseases, this work aimed at better understanding the complexity of vessel functions has immediate translational implications for subsequent therapeutic exploitation. Future Outlook: It is increasingly recognized that angiogenesisregulating molecules do not just control the growth of blood and lymphatic vessels, but also have critical maintenance functions in the adult. Molecules of the Angiopoietin/Tie ligand/receptor family exert gatekeeper functions within the vascular system to control tissue homeostasis and serve metabolic maintenance functions. Future work of the laboratory will be aimed at better understanding the molecular mechanisms of the vessel wall in the control of tissue homeostasis, most notably as it relates to maintenance and repair processes. Experimental approaches include (i) the vascular control of liver regeneration and liver tumorigenesis, (ii) the role of blood vessels in contributing to fibrotic tissue remodeling, (iii) the role of the vasculature in controlling tissue metabolism, including obesity, (iv) the role of blood vessels during ageing and the role of vessel wall resident and bone marrow-derived stem cells during this process, and (v) the role of blood vessels in mediating the metastatic dissemination of circulating tumor cells. The lab will further intensify its efforts to elucidate the molecular and functional properties of the least well understood cells of the vessel wall, the perivascular pericytes, a cell type lining the outer surface of capillaries. We will study pericyte-endothelial interactions in depth to unravel pericyte function during pathological conditions including fibrosis and tumor progression. ESSENTIAL PUBLICATIONS: (1.) Felcht M. et al. (2012). Angiopoietin-2 differentially regulates angiogenesis through Tie2 and integrin signaling. J. Clin. Invest., 122, 1991–2005. Mouse pups are born with an avascular retina. After birth, retinal blood vessels grow centrifugally from the optic disc over a period of 6 to 8 days to form a complex sheet-like capillary network that eventually prunes and matures over time. Due to its versatility and opportunities for high resolution analysis, the postnatal retinal angiogenesis model has developed as the most popular model to study angiogenesis in vivo. (2.) Kutschera S. et al. (2011). Differential endothelial transcriptomics identifies Semaphorin 3G as a vascular class 3 semaphorin. Arterioscler. Thromb. Vasc. Biol., 31, 151–159. (3.) Alajati A. et al. (2008). Spheroid-based engineering of a human vasculature in mice. Nature Methods, 5, 439–445. (4.) Fiedler U. et al. (2006). Angiopoietin-2 sensitizes endothelial cells to TNF-alpha and has a crucial role in the induction of inflammation. Nature Med., 12, 235–239. 42 Research Program Cell and Tumor Biology Cell Growth and Proliferation Division Head: Prof. Dr. Bruce Edgar The precise control of cell proliferation is essential for development in growing animals and plants, and for tissue homeostasis in adults. Loss of this control is a pre-requisite for carcinogenesis. Research in Dr. Edgar’s group focuses on the mechanisms that control cell growth and proliferation using the Drosophila model system. They use diverse molecular, genetic and cytological approaches to discover, and then characterize, genes and pathways that regulate the growth and proliferation of cells in vivo in several different organs and tissue types in this small fruitfly. Genes discovered in this way often prove to be oncogenes or tumor suppressors in humans, and thus these basic studies fuel more applied cancer research. Ongoing projects address the control of cell proliferation by the E2F, Retinoblastoma, and APC/C complexes, the mechanism of growth-dependent endoreplication cell cycles, nutrient-regulated cell growth via the insulinTOR signaling network, and the regulation of homeostatic and neoplastic growth in the fly’s gut by intestinal stem cells. Future Outlook: The laboratory continues to focus on the regulation of the cell growth and proliferation in several cell types in Drosophila. The main projects concern: • Regulation of cell cycle exit during differentiation • Cell cycle control by Hsp90 and the APC/C ubiquitin ligase • Control of Endocycles by E2F and the CRL4 ubiquitin ligase • Growth regulation of the Endocycle • Mechanism of endocycling in murine trophoblast giant cells Research at DKFZ 2014 • • • • Intestinal stem cell control by cell signaling pathways including Jak/Stat, EGFR/ Ras/MAPK, Hippo, and others Whole-genome screens for regulators of intestinal stem cell proliferation and differentiation Cell cycle controls in intestinal stem cells and their progeny Development of an in vitro intestinal stem cell culture model ESSENTIAL PUBLICATIONS: (1.) Jiang H. et al. (2009). Cytokine/Jak/Stat signaling mediates regeneration and homeostasis in the Drosophila midgut. Cell, 137, 1343–1355. (2.) Jiang H. et al. (2011). EGFR/Ras/MAPK signaling mediates adult midgut epithelial homeostasis and regeneration in Drosophila. Cell Stem Cell, 8, 84–95. (3.) Shibutani S.T. et al. (2008). Intrinsic negative cell Cell Growth and Proliferation (A220) cycle regulation provided by PIP box- and Cul4Cdt2- German Cancer Research Center mediated destruction of E2f1 during S phase. Dev Cell, ZMBH 15, 890–900. Im Neuenheimer Feld 282 (4.) Shaw R.L. et al. (2010). The Hippo pathway regulates intestinal stem cell proliferation during Dros- 69120 Heidelberg ophila adult midgut regeneration. Development, 137, Phone: +49 6221 54 6827 4147–4158. [email protected] sSpi 24-96h AED! Stem cell tumors (green cells) in a fruit fly intestine caused by forced activation of Spitz, a conserved EGFtype growth factor. The fly intestine has many similarities to its human counterpart, and is being used by Dr. Edgar’s research group to understand the genetic basis of gastrointestinal tumorigenesis. 43 Cell and Tumor Biology Clinical Neurobiology Division in Cooperation with Heidelberg University Medical Center Head: Prof. Dr. Hannah Monyer Clinical Neurobiology (A230) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3100 [email protected] The common theme of the lab projects regards mechanisms underlying brain plasticity. One effort is related to the differential contribution of distinct glutamate receptor subtypes to short- and long-term synaptic plasticity and the modulation of glutamate receptors by auxiliary proteins. Furthermore we investigate the functional role of GABAergic interneurons to learning and memory. GABAergic interneurons are the principal source of inhibition in the adult brain and synchronize the activity of neuronal networks with millisecond precision, a prerequisite for most higher brain functions. Projects focusing on GABAergic interneuron function are tightly interlinked and include studies at the molecular-cellular, network and behavioral level. We identified molecular targets that are ideal to manipulate GABAergic interneuron activity in order to probe cell and network function. Thus, we take recourse to genetically modified mice with reduced GABAergic interneuron recruitment or altered connectivity and study the effect for spatial coding and memory. We focus on the hippocampal-entorhinal formation, a brain structure that is required for spatial navigation in rodents and episodic memory in humans. Finally, we study plasticity resulting from the integration of newborn neurons into established postnatal networks. Neurogenesis projects focus on genes involved in cell generation, migration and differentiation. 2. Projects revolving around GABAergic interneuron function will entail more local genetic manipulation. So far, the genetic manipulation affected GABAergic interneurons in the whole forebrain but it would be ideal to manipulate interneurons selectively in the hippocampal-entorhinal cortex formation. Furthermore, virus-mediated gene expression of light-activated channels (e.g. Channelrhodopsin) allows the reliable on-line identification of GABAergic interneurons in freely moving mice and subsequent interference with the cellular activity during behavioral performance. This approach opens up possibilities to establish causal relationships between GABAergic interneuron activity, spatial coding and memory. Finally, we discovered novel bidirectional GABAergic pathways between hippocampus and medial entorhinal cortex whose function for neuronal synchronization between these two major brain areas remains to be established. 3) Projects regarding neurogenesis will focus on modification of neurogenesis by environmental factors and establish the functional significance of neurogenesis for hippocampal and olfactory learning. ESSENTIAL PUBLICATIONS: (1.) Melzer S. et al. (2012).Long-range-projecting GABAergic neurons modulate inhibition in hippocampus and entorhinal cortex. Science. 335, 1506– Future Outlook: We will extend our ongoing investigations in the following directions: 1. We will seek to unravel mechanisms by which newly identified auxiliary proteins modulate receptor signaling. We will determine interacting domains between auxiliary proteins and receptors. Furthermore, we will establish whether the expression of auxiliary proteins can be modulated by activity. 1510. (2.) Engelhardt J. et al. (2010). CKAMP44. A brain-specific protein attenuating short-term synaptic plasticity in the dentate gyrus. Science, 327, 1518–1522. (3.) Korotkova T. et al. (2010). NMDA receptor ablation on parvalbumin-positive interneurons impairs hippocampal synchrony, spatial representations, and working memory. Neuron, 68, 557–569. (4.) Allen K. et al. (2011). Gap junctions between interneurons are required for normal spatial coding in the hippocampus and short-term spatial memory. J. Neurosci., 31, 6542–6552. 44 Research Program Cell and Tumor Biology Chaperones and Proteases Division Head: Prof. Dr. Bernd Bukau Our research aims at understanding the molecular basis of the intricate functional network of chaperones and proteases responsible for maintaining protein homeostasis in the cytosol. Our main focus is on: (1) Biogenesis of proteins. Concurrently with their synthesis, nascent polypeptides are subjected to enzymatic processing, chaperoneassisted folding or membrane targeting, processes for which the ribosome serves as docking platform of enzymes, targeting factors and chaperones. We are dissecting these events and the relationship between translation and protein folding/assembly. (2) Functional network of Hsp70 chaperone machines. The Hsp70 chaperone network constitutes a versatile cellular system regulating protein conformation. We analyze the mechanism of Hsp70 and co-chaperones in protein quality control. (3) Cellular strategies coping with protein misfolding and aggregation. Protein aggregation is an organised process in vivo, leading to deposition of aggregates at specific cellular sites. We are determining parameters and factors controlling protein aggregation, and are dissecting the mechanism of clearance of misfolded and aggregated proteins by chaperones and proteases. 2. 3. Functional network of Hsp70 chaperone machines. How do J-proteins activate the Hsp70 cycle? How do nucleotide exchange factors of the Hsp110 family cooperate with Hsp70 in protein quality control? How do Hsp70-J-proteins distinguish the different categories of client proteins? Cellular strategies coping with protein misfolding and aggregation. What mechanisms mediate sorting of aggregationprone proteins into distinct deposits? Which factors are responsible for clearance of misfolded/aggregated proteins? How do AAA+ chaperones and Hsp70 systems mediate protein disaggregation and refolding? What is the basis for the triage decision between degradation and refolding of misfolded proteins? ESSENTIAL PUBLICATIONS: (1.) Oh E. et al. (2011). Selective ribosome profiling re- Chaperones and Proteases (A250) German Cancer Research Center ZMBH Im Neuenheimer Feld 282 69120 Heidelberg Phone: +49 6221 54 6795 [email protected] veals the cotranslational chaperone action of trigger factor in vivo. Cell 147, 1295–1308. (2.) Erbse A. et al. (2006). ClpS is an essential component of the N-end rule pathway in Escherichia coli. Nature. 439, 753–756. (3.) Weibezahn J. et al. (2004). Thermotolerance requires refolding of aggregated proteins by substrate translocation through the central pore of ClpB. Cell, 119, 653–665. Future Outlook: We will focus on three long-term topics: 1. Biogenesis of proteins. What are the mechanisms of chaperone-assisted cotranslational protein folding? What is the basis for functional orchestration of ribosome-associated chaperones, enzymes and targeting factors? Is protein assembly a co-translational process, in which nascent chains of components of a protein complex interact with other complex components to achieve assembly. Does the translation process itself control protein assembly? Research at DKFZ 2014 (4.) Tyedmers J. et al. (2010). Cellular strategies for controlling protein aggregation. Nat. Rev. Cell Biol. 11, 777–788. Mechanism of protein aggregate dissolution through Hsp70/Hsp100 cooperation. The ring-shaped Hsp100 has two structural states, one inactive and the other activated. A molecular toggle keeps the Hsp100 chaperone in the inactive state. Hsp70 causes the toggle to flip, thereby activating the Hsp100 chaperone. In this state it can pull protein strands out of the aggregate. The activation of Hsp100 is not permanent, with the chaperone reverting to the repressed state after the aggregate has dissolved. Hsp100 Hsp100 inactive activated Hsp70 protein aggregate 45 Cell and Tumor Biology Molecular Neurobiology Division Head: Prof. Dr. Ana Martin-Villalba Molecular Neurobiology (A290) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Unraveling the complex functions of CD95 in the central nervous system has been the main focus of our research in the past years. In particular, we discovered the multiple roles played by CD95 in different neural, immune and tumor cells. We have identified the CD95 as a major trigger of cell migration/invasion leading to recruitment of inflammatory cells and tumor progression. On the other hand, CD95 crucially contributes to stem cell survival and lineage differentiation. Our current research focus is on further characterization of stem cell biology in homeostasis and response to injury in the brain and pancreas; the role of inflammation in neurodegenerative diseases such as Parkinson disease and autoimmune diseases; and the role of stem cells and inflammation in glioblastoma- and pancreatic adenocarcinoma-initiation and progression. To tackle these questions, we combine biochemical and modern genomic technologies as well as cell biology and genetics in human cells and mouse model systems. Future Outlook: Stem cells in adulthood are involved in tissue homeostasis and response to injury. Alteration of the default program controlling stem cell‘s proliferation, survival and differentiation in these scenarios set the ground for tumor initiation. Our current and future research centers on understanding the molecular program involved in the control of stem cell quiescence/ activation in the brain and pancreas during homeostasis and disease and its modulation by the innate immune system. Findings from adult stem cells will be further examined in human cancer stem cells and animal models of glioblastoma and pancreatic adenocarcinoma. Our research intends to contribute to the identification of molecular mechanisms involved in stem cells’ biology, and tumor initiation and/or progression. ESSENTIAL PUBLICATIONS: (1.) Letellier E. et al. (2010). CD95-ligand on peripheral myeloid cells activates Syk kinase to trigger their recruitment to the inflammatory site. Immunity, 32, Phone: +49 6221 42 3766 240–252. This article was picked and evaluated by “Faculty of 1000” with a F1000 Factor of 6 http:// [email protected] f1000biology.com/article/id/2629957. (2.) Corsini N. et al. (2009). The death receptor CD95 activates adult neural stem cells for working memory formation and brain repair. Cell Stem Cell, 5, 178–190. (3.) Kleber S. et al. (2008). Yes and PI3K bind CD95 to signal invasion of glioblastoma. Cancer Cell, 13, 235– 248. This article was picked and evaluated by “Faculty of 1000” members with a F1000 Factor of 3.2.http:// f1000medicine.com/article/id/1119774/evaluation. (4.) Sancho-Martinez I. et al. (2009). Tyrosine phosphorylation and CD95: a FAScinating switch. Cell Cycle 8, 838–842. Neurosphere derived from neural stem cells from the subventricular zone of NestinCre-ERT2 iYFP reporter mice 24 hours after tamoxifen induction. 46 Research Program Cell and Tumor Biology Molecular Biology of the Cell II Division Head: Prof. Dr. Ingrid Grummt Our group identifies, characterizes and exploits the molecular mechanisms that control gene expression at the genetic and epigenetic level, aiming to understand the chain of events by which external signals are transferred into the cell nucleus to regulate transcription of specific genes. Focussing on the role of nuclear noncoding RNA (ncRNA) in chromatin structure and epigenetic regulation, we found that ncRNA has an impact on many chromatinmediated processes, linking both RNA and chromatin fields. We have discovered a novel RNAbased strategy for epigenetic programming, showing that ncRNAs are capable of forming DNA:RNA triplexes with regulatory gene sequences. These triplex structures are specifically recognized by the DNA methyltransferase DNMT3b, thereby inducing DNA methylation and transcriptional silencing. Other ncRNAs guide histone modifying enzymes to specific genomic sites, demonstrating that ncRNAs can act as selective ligands for chromatin modifying enzymes. Deciphering novel epigenetic and metabolic control mechanisms of gene expression will reveal how epigenetic defects cause human diseases and will be instrumental in facilitating therapeutic strategies in the future. regulation of chromatin and transcription and will investigate the mechanism by which these ncRNAs regulate the function of transcription factors and chromatin modifying enzymes. We will perform genome-wide analyses to explore with which proteins these regulatory RNAs are associated and will validate their role in key biological processes. We expect that in the long term, these studies will lead to an understanding of the mechanisms that propagate a specific chromatin structure through cell division and will provide mechanistic insights into the functions of ncRNAs in transcriptional regulation. ESSENTIAL PUBLICATIONS: (1.) Schmitz K.-M. et al. (2010). Triplex formation between noncoding RNA and DNA targets DNMT3b to regulatory gene regions. Genes&Dev. 24, 2265–2269. (2.) Feng W. et al. (2010). PHF8 activitates transcrip- Molecular Biology of the Cell II (A030) tion of rRNA genes through H3K4me3 binding and German Cancer Research Center H3K9me1/2 demethylation. Nature Struct. Mol. Biol. Im Neuenheimer Feld 581 17, 445–450. (3.) Zhou Y. et al. (2009). Acetylation by hMOF regu- 69120 Heidelberg lates NoRC-dependent heterochromatin formation, Phone: +49 6221 42 3423 nucleosome positioning and transcriptional silenc- [email protected] ing. Nature Cell Biol. 11, 1010–1016. (4.) Mayer C. et al. (2006). Intergenic transcripts regu- Future Outlook: Evidence from a variety of experimental systems demonstrates that non-coding RNAs (ncRNAs) play a significant role in the control of gene expression and epigenetic regulation. It seems that ncRNAs are numerous and highly adapted in roles that require specific nucleic acid recognition without complex catalysis, such as in guiding RNA modifications or in directing post-transcriptional regulation of gene expression and chromatin structure. We intend to identify ncRNAs involved in the Research at DKFZ 2014 late the epigenetic state of rRNA genes. Mol. Cell 22, 351–361. Non-coding RNAs act in concert with chromatin modifying enzymes to establish distinct epigenetic marks at transcriptionally active and silent genes, characterized by specific nucleosome positions, histone marks (Ac, Me), and DNA methylation (CH3). 47 Cell and Tumor Biology Cell Biology Helmholtz Professorship Head: Prof. Dr. Werner W. Franke Cell Biology (A991) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3212 [email protected] Cell morphology, character, function and interaction with other cells are established and predominantly determined by their architectonic organization, i.e. the cytoskeleton, in both normal and pathological states, in situ and in cell culture. In particular, our studies focus on the structural and molecular elements forming the cytoplasmic filament systems, notably the microfilament bundles as well as the intermediate-sized filaments and their anchorage structures, the dense plaques located on the cytoplasmic sides of the cell-cell connecting junctions, i.e. primarily the adhering junctions and the desmosomes. We are extending and completing our analyses of the major constituent molecules of these cell type-specific junctions using biochemical and immunological methods, including chemical cross-linking as well as high-resolution immunofluorescence and immunoelectron microscopy. To this end, we generate antibodies against cell typespecific cytoskeletal molecules and examine, in collaboration with pathologists, their diagnostic value for tumor cell typing, notably for the identification of the specific primary tumor of metastatic tumor cells. In addition, we have recently demonstrated spontaneous and cumulative syntheses of proteins that then can be assembled to certain novel and semistable structures, including cell-cell junctions, that are able to transform “out of histogenesis” a given tumor cell type directly to a novel different tumor cell type. Double-label immunofluorescence microscopy of a monolayer culture of epithelial cells (human keratinocytes of line HaCaT) connected by cell-cell bridges with central desmosomes (red and yellow show the major molecule, desmoplakin) anchoring bundles of keratin filaments (green). For details see W.W. Franke (2009) Cold Spring Harb. Perspect. Biol. 1, a003061. 48 Research Program Future Outlook: The ongoing and future work aims at the completion of the molecular composition of the cell-cell junctions and the identification of novel types of junctions; their specific functions and mode of formation; the elucidation of their value in tumor diagnosis; and of their roles in tumor spread and metastasis. ESSENTIAL PUBLICATIONS: (1.) Franke W.W. et al. (2013). Transmembrane protein PERP is a component of tessellate junctions and of other junctional and non-junctional plasma membrane regions in diverse epitheliail and epitheliumderived cells. Cell Tissue Res. 353, 99–115. (2.) Franke W.W. & Pape U.-F. (2012). Diverse types of junctions containing tight junction proteins in stratifi ed mammalian epithelia. Ann. N. Y. Acad. Sci., 1257, 152–157. (3.) Pieperhoff S. et al. (2012). The plaque protein myozap identified as a novel major component of adhering junctions in endothelia of the blood and lymph vascular systems. J. Cell. Mol. Med., 16, 1709–1719. (4.) Franke W.W. & Rickelt S. (2011). Mesenchymal-epithelial transitions: Spontaneous and cumulative syntheses of epithelial marker molecules and their assemblies to novel cell junctions connecting human hematopoietic tumor cells to carcinomatoid tissue structures. Int. J. Cancer, 129, 2588–2599. Cell and Tumor Biology Molecular Biology of the Cell I Helmholtz Professorship Head: Prof. Dr. Günther Schütz Our laboratory is studying the role of nuclear receptors during normal development and disease. Since germline-inactivation of the mineralocorticoid receptor (MR) or the glucocorticoid receptor (GR) gene results in early lethality, we generated mutant mice with neuron-specifc inactivation of either gene in the forebrain. To avoid effects on brain development, we established a transgenic mouse line that allows inducible gene inactivation in adult forebrain neurons. The subventricular zone (SVZ) of the lateral ventricle and the subgranular zone (SGZ) of the dentate gyrus (DG) are the largest germinal zones of sustained neurogenesis during adulthood. We found that the orphan nuclear receptor tailless (Tlx) is exclusively expressed in these slowly dividing neural stem cells (NSCs). We also found that overexpression of Tlx induced expansion of the neural stem cell population in mice. These cells initiate the development of glioma-like lesions and gliomas. Glioma development is accelerated upon loss of the tumor suppressor p53 in adult neural stem cells. Therefore, our goal is to generate transgenic mouse models that will allow for elucidation of the molecular mechanisms involved in disease development. In a novel project we study the function of microRNAs in adult neural stem cells and neurons, their impact on neural plasticity, and their involvement in the CNS control of energy balance and metabolism. Future Outlook: The major aims in our future work will be: genome-wide identification of binding sites of the mineralo- and glucocorticoid receptor in the hippocampus by ChIP-Seq methodology. With this method we will identify the regulatory sequences that cause spatial and temporal expression of the target genes of these nuclear receptors. We anticipate that with these approaches, chromatin immunoprecipitation coupled to massively parallel sequencing, the characterization of target genes for these nuclear receptors (GR, MR) will be possible. These efforts will thus lead to a molecular understanding of the action of these regulatory factors. Molecular Biology of the Cell I (A992) ESSENTIAL PUBLICATIONS: (1.)Kirilov, M. et al. (2013). Dependence of fertility on German Cancer Research Center kisspeptin-Gpr54-signaling at the GnRH neuron. Im Neuenheimer Feld 280 Nat. Commun., 4, 2492. doi: 10.1038/ncomms3492. 69120 Heidelberg (2.) Habermehl D. et al. (2011). Glucocorticoid activity Phone: +49 6221 42 3411 during lung maturation is essential in mesenchymal [email protected] and less in alveolar epithelial cells. Mol. Endocrinol., 25, 1280–1288. (3.) Liu H.-K. et al. (2010). The nuclear receptor tailless induces long term neural stem cell expansion and brain tumor initiation. Genes. Dev., 24, 683–695. (4.) Engblom D. et al. (2008). Glutamate receptors on dopamine neurons control the persistence of cocaine-seeking. Neuron, 59, 497–508. glucocorticoids GR + GRE - + AP1 or NFкB The glucocorticoid receptor modulates transcription by different modes of action. Research at DKFZ 2014 P STAT5 STAT5 P nGRE 49 Cell and Tumor Biology Molecular Biology of Centrosomes and Cilia Helmholtz University Junior Research Group Head: Dr. Gislene Pereira Molecular Biology of Centrosomes and Cilia (A180) German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 3447 [email protected] Centrosomes of mammalian and fungi cells play a decisive role in the temporal and spatial organisation of the microtubules of the bipolar spindle, which segregates the sister chromatids to opposite poles of the cell during mitosis. In addition, a large body of evidence suggests that centrosomes also function as a signalling platform that integrates a multitude of cellular signals to control cell fate determination and/or cell cycle progression. Our lab has a long-standing interest in understanding how centrosome-associated components control mitotic exit and cytokinesis on a molecular level. Our work has significantly contributed to the identification and molecular characterisation of a centrosome-associated mitotic checkpoint, named as the spindle position checkpoint (SPOC). This checkpoint stops cell cycle progression in response to mis-orientation of the mitotic spindle along the mother-daughter cell polarity axis. More recently, a similar centrosome-based SPOC mechanism was reported to exist in higher eukaryotic cells undergoing asymmetric cell divisions. This highlights an important functional conservation, which is currently being explored by our group. In addition, we are investigating the molecular mechanisms by which two conserved centrosome-associated cell cycle regulators, the NDR kinase Dbf2 and the phosphatase Cdc14, regulate cytokinesis (i.e. the physical separation of mother and daughter cells) after completion of mitosis. Future Outlook: In all eukaryotic cells, mitotic checkpoints and the temporal and spatial control of cytokinesis are of extreme importance for the maintenance and the accurate segregation of the genome. Therefore, the molecular characterisation of SPOC signalling and cell cycle control of cytokinesis will constitute an important part of our future research. In addition, over the last five years, we became interested in investigating how specialised sub-structures of centrosomes, named centrioles, serve as a template for the formation of the basal body, from which cilia and flagella are assembled. Cilia are highly conserved microtubule-based organelles that play an essential role in signalling and cell motility. Defects in the formation or function of cilia are related to a large number of severe genetic disorders, known as ciliopathies. Our aims are to understand the molecular mechanisms that control the transition from centriole to basal body and how ciliogenesis is coordinated with cell cycle progression in mammalian cells. For more information about our research activities, please visit our website: www.dkfz.de/en/celldivision/index.php ESSENTIAL PUBLICATIONS: (1.) Caydasi A.K. et al. (2009). Spindle alignment regulates the dynamic association of checkpoint proteins with yeast spindle pole bodies. Dev Cell., 16, 146–156. Cell division imaged in the budding yeast Saccharomyces cerevisiae. The chromosomes are shown in blue, the mitotic spindle in green and the centrosome. (2.) Meitinger F. et al. (2011). Phosphorylation-dependent regulation of the F-BAR protein Hof1 during cytokinesis. Genes & Dev., 25, 875–888. (3.) Schmidt K.N. et al. (2012). Cep164 mediates vesicular docking to the mother centriole during early steps of ciliogenesis, J. Cell Biol., 199, 1083–1101. (4.) Kuhns S. et al. (2013). The microtubule affinity regulating kinase MARK4 promotes axoneme extension during early ciliogenesis. J. Cell Biol., 200, 505–522. 50 Research Program Cell and Tumor Biology Posttranscriptional Control of Gene Expression Helmholtz University Junior Research Group Head: PD Dr. Georg Stöcklin In eukaryotes, the activity of all genes depends on the level of transcription in the nucleus. In addition, many genes are regulated at the post-transcriptional level by mechanisms that control the translation efficiency and degradation rate of individual mRNAs in the cytoplasm. This allows cells to respond rapidly to external stimuli and alter protein expression levels directly. Our lab examines control of translation and mRNA decay in human cell lines and mouse macrophages. We have extensively analyzed a group of unstable mRNAs that contain adenylate-urylate(AU)-rich elements and the cognate RNA-binding proteins that regulate the stability of these mRNAs. More recently, we identified a novel class of stem-loop motifs, which promote mRNA degradation by recruiting a protein termed Roquin. Importantly, this stem-loop motif is present in the mRNA encoding TNF, the most potent pro-inflammatory cytokine of the mammalian organism. Through a transcriptome-wide analysis, we identified a distinct group of mRNAs whose translation is specifically regulated during the course of macrophage activation. Interestingly, we found that many feedback inhibitors of the NF-kB pathway are regulated at the level of translation; current experiments address the molecular mechanisms underlying this mode of regulation. Cells exposed to environmental stress respond by reducing their global rate of translation. We discovered that translation suppression in response to cold shock is mediated via an unusual pathway and is essential for cells to survive hypothermia, underlying the importance of posttranscriptional control mechanisms. Currently, we are investigating the mechanisms by which hypoxia and oxidative stress suppress global protein synthesis. Finally, we discovered an RNA-binding protein that is required for cell cycle arrest after DNA damage. Loss of this protein causes mitotic errors and the accumulation of damaged DNA. Importantly, reduced expression of this protein in human squamous cell carcinoma also correlates with reduced patient survival. Our current Research at DKFZ 2014 efforts are to determine the molecular mechanism by which this RNA-binding protein exerts its function in the DNA damage response. Future Outlook: Future work in the lab will focus on identifying novel cis-acting elements and trans-acting factors that control both the degradation and translation of specifically regulated mRNAs. In addition, we examine the mechanisms responsible for suppressing global protein synthesis in response to environmental stress signals. ESSENTIAL PUBLICATIONS: (1.) Leppek K. et al. (2013). Roquin promotes constitutive mRNA decay via a conserved class of stem-loop recognition motifs. Cell, 153, 869–881. (2.) Hofmann S. et al. (2012). Translation suppression promotes stress granule formation and cell survival in response to cold shock. Mol Biol Cell., 23, 3786– Posttranscriptional Control of Gene Expression (A200) German Cancer Research Center 3800. Im Neuenheimer Feld 280 (3.) Spasic M. et al. (2012). Genome-wide assessment 69120 Heidelberg of AU-rich elements by the AREScore algorithm. PLoS Phone +49 6221 54 6887 Genet., 8(1):e1002433. doi: 10.1371/journal. (4.) Sandler H. et al. (2011). Not1 mediates recruitment of the deadenylase Caf1 to mRNAs targeted for degradation by tristetraprolin. Nucleic Acids Res., 39, [email protected] and Zentrum für Molekulare Biologie der Universität Heidelberg (ZMBH) 4373–4386. During cold shock, mammalian cells suppress protein synthesis. Translationally arrested mRNAs assemble into stress granules (cyan) in the cytoplasm and the mitochondrial network (green) shows severe alterations. Nuclei are visualized in purple. 51 Cell and Tumor Biology Cellular Senescence Junior Research Group Head: Dr. Thomas G. Hofmann Cellular Senescence (A210) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4631 [email protected] The DNA damage response (DDR) is at the heart of cancer etiology. Cancer cells show a dysfunctional DDR which is associated with increased genomic instability and resistance to DNA damage-inducing treatments. Cells respond to DNA damage by tipping the cell fate balance to achieve one of the following outcomes: DNA repair, cellular senescence, or cell death. Commitment to a particular cell fate is regulated by an evolutionary conserved signal transduction network which is coordinated by a set of DNA damage-responsive checkpoint kinases. Our research group is studying the regulatory processes controlling cell fate decisions in response to DNA damage. Our aim is to elucidate the molecular mechanisms underlying the selectivity of the cellular decision process in response to damage insults, which could vary between DNA repair, cell death, and senescence. To this end, we are identifying novel regulators and substrates of checkpoint kinases, and investigating their biological function and mechanism of action in the DDR network. We have a particular interest in understanding the function of proteins localizing to specific nuclear domains termed Promyelocytic leukemia (PML) bodies. Indeed, PML bodies have been proposed to act as nuclear cell fate regulatory centers. Future Outlook: Our goal is to yield sufficient insight into cell fate control mechanisms in order to define molecular targets which will allow us to modulate the DDR in cancer cells, and subsequently channel it towards cell elimination. ESSENTIAL PUBLICATIONS: (1.) Bitomsky N. et al. (2013). Autophosphorylation and Pin1 binding coordinate DNA damage-induced HIPK2 activation and cell death. Proc. Natl. Acad. Sci. USA, (epub ahead of print). (2.) Winter M. et al. (2008). Control of tumor suppressor HIPK2 stability by ubiquitin ligase Siah-1 and checkpoint kinases ATM and ATR. Nature Cell Biology, 10, 812–824. (3.) Milovic-Holm K. et al. (2007). FLASH links the CD95 signaling pathway to the cell nucleus and nuclear bodies. EMBO J., 26, 391–401. (4.) Hofmann T.G. et al. (2002). Regulation of p53 activity by its interaction with Homeodomain-interacting protein kinase-2. Nature Cell Biology, 4, 1–10. DNA damage checkpoint kinases (red & green) are recruited to DNA double-strand breaks at chromatin (blue) following ionizing radiation. 52 Research Program Cell and Tumor Biology Normal and Neoplastic CNS Stem Cells Junior Research Group Head: Dr. Hai-Kun Liu Active adult neurogenesis is one of the most exciting discoveries in neuroscience of the last decade. The subventricular zone (SVZ) of the lateral ventricle (LV) and the subgranular zone (SGZ) of the dentate gyrus (DG) in the hippocampus are the largest germinal zones of sustained neurogenesis during adulthood in the mammalian central nervous system. Astrocyte-like type B cells in the adult SVZ are thought to be multipotent neural stem cells (NSCs). These cells give rise to transient amplifying type C cells, which in turn differentiate into type A cells (neuroblasts) that migrate to the olfactory bulb (OB) through the rostral migratory stream (RMS). NSCs in the SGZ mainly give rise to new granular cells in the DG which are thought to be important for spatial learning and memory. Adult neurogenesis in the SVZ represents a unique system to study regulation of NSC proliferation, differentiation and directed neuronal migration in vivo. Strikingly, these cells can also initiate gliomagenesis after acquiring the same oncogenic mutations which were found in human brain tumor patients. Our lab aims to identify crucial molecular pathways that are important for the regulation of normal and neoplastic neural stem cells. To achieve this goal, we are mainly using mouse models in which we have altered the activity of some oncogenes, tumor suppressors and chromatin remodellers specifically in adult mouse neural stem cells. 2. 3. tity of stem cells and their progenies. One of the major focuses in our lab is to understand the interplay between crucial transcriptional factor and chromatin remodelers, in particular their functions during neural stem cell self-renewal and differentiation. Neoplastic neural stem cells: One important issue of targeting braintumor stem cells (BTSCs) is to avoid damaging normal stem cells. Thus our goal is to identify critical differences between normal and tumor stem cells which will provide important information for targeting exclusively BTSCs. Mouse models of brain tumors: We have developed several inducible mouse brain tumor models by introducing frequently found genetic mutations in human patients. We consider the inducible model a better model to recapitulate the human glioblastoma, and it will be extremely interesting to further investigate the cellular and molecular changes before detectable brain tumor formation in this particular model. Normal and Neoplastic CNS Stem Cells (A240) German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 3266 [email protected] ESSENTIAL PUBLICATIONS: (1.) Feng W. et al. (2013). The chromatin remodeler CHD7 regulates adult neurogenesis via activation of SoxC transcription factors. Cell Stem Cell, 13, 62–72. (2.) Liu H-K. et al. (2010). The nuclear receptor tailless induces long-term neural stem cell expansion and Future Outlook: We have generated several mouse models which can be used to introduce genetic mutations specifically in NSCs. We are currently using these models to study: 1. Genetic and epigenetic regulation of neural stem cells: Epigenetic mechanisms are crucial for the regulation of the most important characteristics of stem cells that are self-renewal and multipotency. Key transcriptional factors play decisive roles in the determination of the iden- Research at DKFZ 2014 brain tumor initiation. Genes Dev ,24, 683–695. (3.) Liu H-K. et al. (2008). The nuclear receptor Tailless is required for neurogenesis in the adult subventricular zone. Genes Dev, 22, 2473–2478. (4.) Belz T. et al. (2007). Inactivation of the gene for the nuclear receptor tailless in the brain preserving its function in the eye. Eur J Neurosci, 26, 2222–2227. A GFP labeled newborn neuron in the mouse adult hippocampus. 53 Cell and Tumor Biology Vascular Signaling and Cancer Helmholtz University Junior Research Group Head: PD Dr. Andreas Fischer Vascular Signaling and Cancer (A270) German Cancer Research Center Im Neuenheimer Feld 280 Blood vessels are a prerequisite for the maintenance of all organ functions. Embryogenesis is dependent on the development and outgrowth of blood vessels, which provide the organism with oxygen and nutrients. Sprouting angiogenesis occurs rarely in the adult organism but can be observed for example during wound healing and also in cancer. Thus, a detailed knowledge about factors regulating angiogenesis and genetic networks, which provide a functional quiescent vascular bed, is highly desirable. Besides the formation of new blood vessels, maintenance of existing blood vessels is also essential. Endothelial cells provide the inner lining of all blood vessels. Disturbed endothelial cell functions are implicated in the pathogenesis of several cardiovascular diseases. Importantly, tumor growth and metastasis are strictly dependent on vascular growth and remodeling. 69120 Heidelberg Phone: +49 6221 42 4150 [email protected] Future Outlook: Our research group investigates signaling pathways that keep blood vessels in a resting but fully functional state. We examine the signaling interplay between endothelial cells as well as interactions of endothelial cells with pericytes and tumor cells. Using cell culture and animal models, our research will help to better understand how genetic factors coordinate angiogenesis in the adult organism. We investigate the role of Delta-Notch signaling and other genes, which are implicated in the formation of vascular malformations and vascular tumors. Other projects in our group focus on barrier functions of blood vessels, which are essential to control the passage of tumor cells and fluids through the vessel wall. A novel research approach deals with the question of how genetic alterations in the endothelium affect metabolism and are implicated in the pathogenesis of cardiovascular diseases. Our research work aims at identifying critical molecular and cellular mechanisms of cardiovascular diseases and tumor progression. These findings will help to lay the foundation for the development of innovative pharmacological strategies. ESSENTIAL PUBLICATIONS: (1.) Wüstehube J. et al. (2010). Cerebral cavernous malformation protein CCM1 inhibits sprouting angiogenesis by activating DELTA-NOTCH signaling. Proc Natl Acad Sci U S A., 28, 12640–12645. (2.) Brütsch R. et al. (2010). Integrin cytoplasmic domain-associated protein-1 attenuates sprouting angiogenesis. Circ Res., 5, 592–601. (3.) Adam M.G. (2013). Synaptojanin-2 binding protein stabilizes the Notch ligands DLL1 and DLL4 and inhibits sprouting angiogenesis. Circ Res., ePub Sep. 11. (4.) Fischer A. et al. (2004). The Notch target genes Small blood vessels of the retina with some covered by pericytes (black). 54 Research Program Hey1 and Hey2 are required for embryonic vascular development. Genes Dev., 8, 901–911. Cell and Tumor Biology Stress-induced Activation of Hematopoietic Stem Cells HI-STEM Junior Research Group Head: Dr. Marieke Essers Tissue stem cells are responsible for the maintenance and repair of most organs and tissues. In the hierarchically organized blood system, dormant hematopoietic stem cells (HSCs) with life long self-renewal capacity are at the top of this hierarchy of cell types which give rise to active HSCs that typically control the blood cell production during healthy homeostasis. However, under conditions of stress, such as during virus infections or after blood loss, where large amounts of mature blood cells are lost, feedback signals are thought to signal back to the dormant HSCs, leading to their activation and thus production of new mature blood cells. However, the molecular and cellular mechanisms, including those cytokines as a part of these feedback loops, remain largely unexplored. Our work has recently demonstrated that the cytokine IFNα which is produced by virally infected immune cells to block the infection of more mature blood cells, is able to activate the entire HSC pool including dormant ones. One of the goals of our research is to investigate the mechanism of IFNα-mediated activation of HSCs and the potential role of the surrounding bone marrow stem cell niche in this process. Furthermore, we are currently exploring feedback loops in response to other stress situations, like bacterial infection and response to chemotherapy induced cytopenia. Future Outlook: Leukemias are initiated and maintained by leukemic stem cells (LSCs), which can transplant the disease and show unlimited self-renewal activity. Most importantly, LSCs appear to be resistant to conventional therapies including anti-proliferative chemotherapy. The mechanisms responsible for this resistance remain unclear, however, their often dormant status as well as their localization in protecting stem cell niches are likely critical components. In our group we address whether LSCs can be targeted by driving them out of dormancy and mobilize them out of their niche. Our finding that IFNα activates normal HSCs to self-renew by putatively altering their niche interactions, may open new possibilities to combine this Research at DKFZ 2014 drug with tyrosine kinase inhibitors such as Imatinib/Gleevec. This class of targeted therapies can achieve long term remission by eliminating progenitor and mature leukemic cells (as with chemotherapy alone), but spare the LSCs (see figure) and thus do not lead to cure. Using mouse models for leukemia and by testing leukemic patient samples, we are currently exploring whether combination therapies with IFNα or other activators can be developed to also target LSCs and thus potentially cure the disease. ESSENTIAL PUBLICATIONS: (1.) Essers M.A. et al. (2009). IFNalpha activates dormant haematopoietic stem cells in vivo. Nature, 458, 904–908. (2.) Trumpp A. et al. (2010). Awakening dormant haematopoietic stem cells. Nat Rev Immunol., 10, Stress-induced Activation of Hematopoietic Stem Cells (A011) 201–209. German Cancer Research Center and (3.) Essers M.A. et al. (2010). Targeting leukemic stem cells by breaking their dormancy. Mol Oncol., 4, 443– 450. (4.) Glauche I. et al. (2012). Therapy of chronic myeloid leukaemia can benefit from the activation of stem cells: simulation studies of different treatment combinations. Br J Cancer, 106, 1742–1752. Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3919 [email protected] a. dHSC dLSC +chemotherapy G0 dHSC dLSC G0 ‘resistant’ b. dLSC +IFNα +chemotherapy aLSC ??? G0 Like normal hematopoietic stem cells (HSCs), most leukemic stem cells (LSCs) are resistant to antiproliferative chemotherapy (a). Their resistance is believed to be the cause of relapse of the leukemia. Several reasons for this resistance have been suggested, one of them being the dormant status of LSCs. Thus, if dormancy is a main reason for LSC resistance to chemotherapy, one can postulate a two-step therapy model by which the dormant LSCs can be targeted; activation of dormant LSCs by activators of quiescence such as IFNa, followed by targeted chemotherapy (b). Such a therapy would not only reduce the bulk of the leukemia, but also eliminate the dormant LSCs, thus reducing the chances of a relapse of the leukemia. 55 Cell and Tumor Biology Experimental Hematology HI-STEM Junior Research Group Head: Dr. Michael Milsom Experimental Hematology (A012) German Cancer Research Center and Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) Im Neuenheimer Feld 280 69120 Heidelberg Transplantation of hematopoietic stem cells (HSC) is a potential curative therapy for many inherited blood disorders and, in concert with high dose chemo- or radiotherapy, can be effective in the treatment of a range of cancers. A major limitation of this approach is the lack of availability of an immunologically matched HSC donor. The work of the Experimental Hematology Group focuses on dissecting the biology of HSC in order to facilitate the production of transplantable HSC from novel sources, and to better understand the regulation of both normal and leukemic stem cells at the molecular level. To these ends, we have developed several novel model systems to screen for cellular factors that either have a major impact on the formation of HSC during development (HSC specification); or which regulate the ability of HSC to give rise to daughter cells that have the same stem cell properties as the parent cell (HSC self-renewal). The latter process is essential for the maintenance and expansion of HSC numbers and is also deregulated in leukemic stem cells. In order to interrogate HSC self-renewal, we primarily focus upon the comparative biology of HSC isolated from normal wild type mice versus those from mice that are deleted for genes in the Fanconi anemia sig- nalling pathway. This model system allows us to directly compare normal versus deregulated HSC self-renewal. Future Outlook: As we gradually dissect the mechanisms that regulate HSC biology, we anticipate that this knowledge will have a direct impact upon both our understanding of cancer and its treatment in the clinic. Normal adult stem cells and cancer cells have a number of features in common (unlimited proliferation capacity, restricted differentiation, drug resistance) and understanding which signalling pathways mediate these biological processes should allow us to identify new therapeutic targets to eliminate or restrict tumor cell growth. Our focus on how normal stem cells regulate their genetic integrity (using the Fanconi anemia model) gives us new insight into how tumor cells may evolve from normal healthy cells, which in turn may allow us to advance strategies employed in preventative medicine. Finally, by developing new methodologies to manipulate, expand and differentiate stem cells, we can significantly contribute to the emerging field of cell and gene therapy, which is showing some promise in early clinical trials directed against a number of diseases, including cancer. Phone: +49 6221 42 3920 ESSENTIAL PUBLICATIONS: [email protected] (1.) Geiselhart A. et al. (2012). Disrupted signalling through the Fanconi anemia pathway leads to dysfunctional hematopoietic stem cell biology: underlying mechanisms and potential therapeutic strategies. Anemia, 2012: 265790. The in vitro specification of hematopoietic progenitor cells from murine embryonic stem cells. Using this methodology, ES cells are able to differentiate into a range of hematopoietic progenitor cell types including myeloid precursors such as colony forming unit granulocyte/macrophage (CFU-GM) and erythroid precursors such as erythroid burst forming units (BFU-E). 56 Research Program (2.) Müller L.U.W. et al. (2012). Overcoming reprogramming resistance of Fanconi anemia cells. Blood. 119 (23):pp5449-57. (3.) Milsom M.D. et al. (2009). Ectopic HOXB4 overcomes the inhibitory effects of tumor necrosis factor-α on Fanconi anemia hematopoietic stem and progenitor cells. Blood, 113 (21): pp5111-20. (4.) Milsom M.D. et al. (2009). Fanca-/- hematopoietic stem cells demonstrate a mobilization defect which can be overcome by administration of the Rac inhibitor NSC23766. Haematologica, 94 (7): pp1011-15. Cell and Tumor Biology Biomarker Discovery HI-STEM Junior Research Group Head: Dr. Christoph Rösli Targeted cancer therapeutics, such as imatinib and rituximab, have shown striking success in the therapy of blood cancers. Unfortunately, the majority of cancer patients still have to be treated with conventional, unspecific chemotherapeutics. Due to their systemic distribution, these therapies carry severe side effects. The disadvantages of conventional chemotherapeutics could be circumvented by the targeted delivery of bioactive molecules to the tumor. Drugs can be exclusively delivered to disease sites by conjugation to molecules specifically binding to tumor-associated biomarkers. Such ligand-based vascular targeting strategies crucially rely on: 1) the identification of robust vascular-accessible tumor biomarkers, 2) the availability of antibodies or fragments thereof with high affinities to these tumorspecific biomarkers and 3) the coupling of these antibodies to bioactive moieties. The HI-STEM/DKFZ-Junior Research Group “Biomarker Identification” is focusing on the mass spectrometry-based identification of novel biomarkers expressed in tumorous tissue and/or metastases using advanced cell culture systems, xenograft tumor models and clinical samples. Furthermore, the selection of human monoclonal antibodies against these biomarkers for the development of targeted cancer therapies and novel diagnostic tools is a core technology in the laboratory. re-occurrence of tumors years after successful treatment. Due to the lack of information about the cell surface proteome of cancer stem cells, no current therapeutic specifically affects this highly aggressive but well-protected cancer cell population. Our group will use its established chemical proteomics-based methods for the identification of cell surface biomarkers on the rare population of cancer stem cells. The resulting biomarkers are then used to develop high affinity human monoclonal antibodies by means of the phage display technology. These antibodies are then not only used for basic research, but also for the development of diagnostics and novel innovative targeted therapeutics. Future cancer therapies might then be based on a two phase protocol: a first debulking phase for the reduction of the tumor burden, followed by a targeted attack on remaining, dormant cancer stem cells hidden elsewhere in the body. Biomarker Discovery (A013) ESSENTIAL PUBLICATIONS: (1.) Fugmann T. et al. (2010). DeepQuanTR: MALDI-MSbased label-free quantification of proteins in complex biological samples. Proteomics, 10, 2631–2643. (2.) Schliemann C. et al. (2010). In vivo biotinylation of the vasculature in B-cell lymphoma identifies BST- German Cancer Research Center and Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) Im Neuenheimer Feld 280 2 as a target for antibody-based therapy. Blood, 115, 69120 Heidelberg 736–744. Phone: +49 6221 42 3917 (3.) Fugmann T. et al. (2011). Proteomic identifica- [email protected] tion of vanin-1 as a marker of kidney damage in a rat model of type 1 diabetic nephropathy. Kidney Int., 80, 272–281. Future Outlook: During recent years, the concept of cancer stem cells has evolved and is now widely accepted. Cancer stem cells (or tumor initiating cells) are a small subpopulation of cancer cells able to promote new tumors and to induce metastases. Importantly, these cells are usually not reached by current cancer therapeutics since they can reside (just like their healthy counterparts), at least transiently, in a dormant, therapy-resistant phase. The population of transiently dormant cancer stem cells is furthermore most likely responsible for the Research at DKFZ 2014 (4.) Rösli C. et al. (2009). Comparative analysis of the membrane proteome of closely related metastatic and nonmetastatic tumor cells. Cancer Res., 69, 5406–5414. Following the proteomics-based identification of a tumor-associated biomarker, human monoclonal antibodies are selected and used for the development of novel diagnostic tools and/or targeted therapeutics. 57 Cell and Tumor Biology Metastatic Niches HI-STEM Junior Research Group Head: Dr. Thordur Oskarsson Metastatic Niches (A014) German Cancer Research Center and Heidelberg Institute for Stem Cell Technology and Experimental Medicine (HI-STEM gGmbH) Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3903 [email protected] Metastasis is the spread of cancer cells from their site of origin leading to outgrowth in distant organs and is the cause of most cancer related deaths. To progress into overt metastasis, disseminated cancer cells must resist a non-permissive environment and maintain viability and growth at distant sites. Increasing evidence suggests that cancer cells adapt by engaging and manipulating the microenvironment generating a metastatic niche that promotes cancer cell fitness. To study the metastatic niche the Oskarsson lab utilizes 3D culture systems of primary cancer cells, RNA interference, transcriptomic and proteomic screens and various mouse models of cancer progression and metastasis. We have shown that tenascin C (TNC), an extracellular matrix (ECM) protein expressed in normal stem cell niches, is an important component of the metastatic niche and advances metastatic progression in breast cancer. The production of TNC promotes viability of metastasis initiating cells by enhancing the expression of musashi-1, a positive regulator of Notch signaling and by inducing the Wnt target gene LGR5. We are currently dissecting further the pathways modulated by TNC and studying the surface receptors that TNC engages. Moreover, we are analyzing the signaling and functional role of other metastatic niche components in cancer progression with a focus on the ECM. These studies may provide valuable insights into cancer progression and could reveal new targets for therapeutic intervention. Future Outlook: Our aim is to identify new components of the metastatic niche and to characterize the interaction of cancer stem cells with the niche. The objective is to determine how the niche supports and maintains metastatic stem cell characteristics and to study the possible role of the niche in resistance to cancer therapy. It is increasingly evident that stem cell properties play an important role in metastasis development and the niche may support and maintain these features. We will pay particular attention to the extracellular matrix that has been demonstrated by us and others to be an essential component of the metastatic niche. The function of the ECM extends greatly beyond a structural scaffold and has been shown to be important for cell regulation and modulation of signaling pathways. The ECM components of the metastatic niche support essential functions in cancer progression and effectively help cancer cells to colonize distant organs. Moreover, the metastatic niche may be a mode for disseminated cancer cells to resist therapeutic intervention. We will analyze the role of niche components in resistance to cancer therapy, an attribute that is tightly linked to metastatic progression. The dissection of the metastatic niche and the ECM mediated signaling within the niche, could provide new avenues to therapeutically impair the competence of disseminated cancer cells and prevent metastatic relapse. ESSENTIAL PUBLICATIONS: (1.) Acharyya S. et al. (2012). A CXCL1 paracrine network links cancer chemoresistance and metastasis. Cell. 150, 165–178. (2.) Oskarsson T. et al. (2011). Breast cancer cells produce tenascin C as a metastatic niche component to colonize the lungs. Nat Med. 17, 867–874. (3.) Oskarsson T. et al. (2010). Diverted total synthesis leads to the generation of promising cell-migration inhibitors for treatment of tumor metastasis: in vivo and mechanistic studies on the migrastatin core Immunostaining of lung metastasis in breast cancer xenograft showing expression of the metastatic niche component tenascin-C at the invasive front (arrow heads). 58 Research Program ether analog. J Am Chem Soc., 132, 3224–3228. (4.) Tavazoie S.F. et al. (2008). Endogenous human microRNAs that suppress breast cancer metastasis. Nature., 451, 147–152. Cell and Tumor Biology Synaptic Signalling and Neurodegeneration DZNE-Junior Research Group Head: Dr. Jakob von Engelhardt Our group investigates glutamatergic synaptic transmission in the hippocampus and cortex. We are particularly interested in what role different glutamate receptors (AMPA- and NMDAreceptors) and glutamate receptor-interacting proteins play in physiological and pathophysiological processes. AMPA receptors mediate most of the fast excitatory transmission in the central nervous system. NMDA receptors are important for synaptic plasticity and thus for learning and memory. In addition, excessive activation of NMDA receptors is detrimental for neurons (excitotoxicity) and contributes to the pathophysiology of brain diseases such as stroke and neurodegenerative diseases. of great importance for all cognitive processes. AMPA-receptor interacting proteins (TARPs, CKAMP44, cornichons and SynDig1) regulate receptor localization and function. We will use heterologous expression systems and transgenic mice to analyze the influence of those proteins on the electrophysiological properties and localization of AMPA-receptors. ESSENTIAL PUBLICATIONS: (1.) von Engelhardt J. et al. (2011). 5-HT3A Receptor-Bearing White Matter Interstitial GABAergic Interneurons Are Functionally Integrated into Cortical and Subcortical Networks. J Neurosci, 31, 16844– 16854. Future Outlook: 1. Mechanisms of Amyloid β pathology: One of the hallmarks of Alzheimer’s disease is the accumulation of amyloid beta-peptide (Aβ) in the brain and its deposition as plaques. However, the current prevailing view is that soluble oligomeric Aβ is one of the main mediators of Alzheimer neurotoxicity, rather than the plaques. There are indications that glutamate receptors play a role in Aβ-mediated neurotoxicity. We will use glutamate receptor transgenic mice to investigate the influence of this interaction on the physiology and anatomy of hippocampal and cortical neurons. 2. Regulation of synaptic communication via AMPA-receptor interacting proteins: Precise control of AMPA receptor number and localization on the cell membrane regulates synaptic strength and is thus Research at DKFZ 2014 (2.) von Engelhardt J. et al. (2010). CKAMP44: a brainspecific protein attenuating short-term synaptic plasticity in the dentate gyrus. Science, 327, 1518–1522. (3.) Korotkova T. et al. (2010). NMDA receptor ablation on parvalbumin-positive interneurons impairs hippocampal synchrony, spatial representations, and working memory. Neuron, 68, 557–569. (4.) von Engelhardt J. et al. (2008). Contribution of Synaptic Signalling and Neurodegeneration (A300) hippocampal and extra-hippocampal NR2B-contain- German Cancer Research Center ing NMDA receptors to performance on spatial learn- Im Neuenheimer Feld 280 ing tasks. Neuron, 60, 846–860. 69120 Heidelberg DZNE = German Center for Neurodegenerative Diseases within the Helmholtz Association Phone: +49 6221 423105 [email protected] Schematic representation of the 424 residue CKAMP44 protein, with signal peptide (SP), extracellular domain with cysteine-rich region (C’s), single transmembrane region (TM) and intracellular domain containing a PDZ domain interaction site at the C-terminus. The extracellular cysteinerich region with proposed disulfide bridges of a Cystine-knot is shown below. The in situ hybridizations illustrate that CKAMP44 mRNA is expressed in the brain of embryonic day 19 (E19), postnatal day 15 (P15) and adult mice. The immunocytochemical analyses of cultured neurons show that CKAMP44 is expressed in dendritic spines and co-localizes with AMPA receptor subunits GluA2/3. 59 Coordinator PROF. DR. ROLAND EILS Structural and Functional Genomics Cancer arises when genes in a cell are changed in such a way that they cause the cell to divide uncontrollably or to resist cell death. However, for this to occur a multitude of specific changes have to coincide. It is the task of this research program to analyze the genome, i.e., the complete set of genes and its products, in order to lay the foundation for developing new diagnostic and treatment methods. This involves mapping the genome, localizing genes within the genetic material, and investigating the functions of cancerrelevant genomic areas. The vast amounts of data accumulated in the process are being captured and evaluated using bioinformatic methods. By combining approaches from mathematics, statistics, physics, and computer sciences with computer-assisted simulation techniques, the theoretical groups within the research program are bridging the gap to experimental research. The methods developed are then directly utilized in many areas within collaborations between numerous DKFZ divisions, other external research groups and clinical partners. 60 Research Program Research at DKFZ 2014 61 Structural and Functional Genomics Biophysics of Macromolecules Division Head: Prof. Dr. Jörg Langowski Biophysics of Macromolecules (B040) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3390 [email protected] Gene activity is not determined by the DNA sequence alone, but also by its three-dimensional organization in the cell: DNA and chromatin global structure play a crucial role in the regulation of many important biological processes, such as cell differentiation or cancerogenesis. The main goal of our research is to study the three-dimensional structure and dynamics of the genome in normal and tumor cells and to describe it by quantitative models. This will help us understand the connection between genome structure and normal or pathological states of the cell. To this aim, we study longrange interactions in DNA when genes are regulated by transcription factors, the structure of nucleosomes and chromatin fiber, and the organization of chromosome territories in the living cell nucleus. The experiments are supplemented by advanced computer simulation techniques that describe the organization of DNA and chromatin as a flexible polymer. Biophysical methods used include in particular single-molecule techniques (fluorescence correlation spectroscopy, single pair FRET, scanning force microscopy), advanced imaging (single plane illumination microscopy), light and neutron scattering, analytical ultracentrifugation, absorption and fluorescence spectroscopy, and stopped flow kinetics. We also provide biophysical methods for the characterization of other systems of biological macromolecules, especially in protein-protein and protein-DNA interaction and intermediate filament proteins. Future Outlook: In the future, we shall develop our activities in the fields of nucleosome and chromatin dynamics and of intermediate filament (IF) biophysics. Three major lines of research will be followed: 1. the role of histone tails and their modifications in chromatin packaging (“molecular epigenetics”), using single molecule FRET as a tool to characterize structural transitions in nucleosomes; 2. the dynamics of protein transport in the living cell nucleus, using our newly developed SPIM microscopy techniques with ultra-fast detection; 3. the dynamics of assembly of IF proteins and the biophysical characterization of their structure and flexibility. We shall continue to build up our computer simulation activities, ranging from modelling biomolecules in atomic detail to coarsegrained models of the genome architecture in entire cell nuclei. This theoretical aspect will always form an important complement to our experimental research. The ultimate goal is to design a physical model of the entire cell in time and space, which can contribute to the understanding of cancer development and to its therapy. Our research shall be a step on the way there. ESSENTIAL PUBLICATIONS: (1.) Fritsch C. et al. (2011). Chromosome dynamics, molecular crowding and diffusion in the interphase cell nucleus: A Monte-Carlo lattice simulation study. Chromosome Research, 19, 63–81. (2.) Böhm V. et al. (2010). Nucleosomal DNA accessibility governed by the dimer/tetramer interface. Nucleic Acids Research, 39, 3093–3102. (3.) Gansen A. et al. (2009). Nucleosome disassembly intermediates characterized by single-molecule FRET. Proc. Natl. Acad. Sci. USA 11, 15308–15313. (4.) Vámosi G. et al. (2008). Conformation of the c- Mobility map of EGFP-protein in a living HeLa cell (Source: Dross N, Spriet C, Zwerger M, Müller G, Waldeck W, Langowski J. (2009) Mapping eGFP Oligomer Mobility in Living Cell Nuclei. PLoS ONE 4(4): e5041). 62 Research Program Fos/c-Jun complex in vivo: a combined FRET, FCCS, and MD-modeling study. Biophys J., 94, 2859–2868. Structural and Functional Genomics Systems Biology of Cellular Signal Transduction Division Head: Prof. Dr. Ursula Klingmüller The goal of the division is to gain insights into molecular mechanisms that regulate cellular decisions and to address their impact on behavior at the tissue and organ level. When these control mechanisms fail, cancer and other diseases arise. Cellular responses are regulated by a multitude of extracellular signals received by cell surface receptors. Within cells the information is processed through complex intracellular signaling networks that in turn impinge on gene regulation and affect metabolism to finally coordinate physiological responses such as proliferation, survival and differentiation. These responses operate on very different time scales ranging from minutes to hours and days. Thus, it is essential to examine key dynamic properties of biological systems, which can be addressed by combining the generation of quantitative time-resolved data with mathematical modeling. Data-based mathematical models enable rapid testing of hypotheses to uncover deregulation in cancer and to predict strategies of intervention in diseases. In close collaboration with modeling partners, methods for quantitative analysis of signaling networks were developed and multiple dynamic pathway models were established yielding unexpected insights into regulatory mechanisms of signaling pathways. The main projects of the division address: 1. 2. 3. Unraveling principal mechanisms of erythropoietin (Epo)-mediated cellular decisions in the hematopoietic system. Bridging from the cellular to the whole organ level during liver regeneration. Insights into altered regulation in cancer and prediction of strategies for efficient intervention in diseases (cancer, drug-in duced liver injury, viral infection). Research at DKFZ 2014 Future Outlook: This knowledge will be used to establish integrated models of signaling pathways, to link them to gene regulation as well as cellcell communication and to include cell cycle progression and cell survival. Finally, integration into multi-scale models and whole body models is aspired. Translational aspects are strengthened through intensive collaborations with clinical partners and companies in the frame of large third party funded research networks. ESSENTIAL PUBLICATIONS: (1.) Schilling M. et al. (2009). Theoretical and experimental analysis links isoform-specific ERK signalling to cell fate decisions, Mol Sys Biol, 334: 119–136. (2.) Becker V. et al. (2010). Covering a broad dynamic Systems Biology of Cellular Signal Transduction (B200) range: information processing at the erythropoietin German Cancer Research Center receptor. Science, 328: 1404–1408. Im Neuenheimer Feld 280 (3.) Raia V. et al. (2011). Dynamic mathematical mode- 69120 Heidelberg ling of IL13-induced signaling in Hodgkin and primary mediastinal B-cell lymphoma allows prediction of therapeutic targets. Cancer Res., 71: 693–704. Phone: +49 6221 42 4481 [email protected] (4.) Bachmann J. et al. (2011). Division of labor by dual feedback regulators controls JAK2/STAT5 signaling over broad ligand range. Mol Syst Biol. 7: 516. In erythroid progenitor cells the cell membrane is visualized by staining for transferrin receptor expression (green) and the nucleus by staining for DNA content (blue). 63 Structural and Functional Genomics Molecular Genome Analysis Division Head: Prof. Dr. Stefan Wiemann Molecular Genome Analysis (B050) German Cancer Research Center Cancer and other human diseases arise from genetic aberrations that are either inherited or occur – as in most cancers – spontaneously in somatic cells. These defects cause abnormal activities of gene products that lead to malfunctioning of molecular and cellular interactions which, in consequence, may induce tumors and cause cancer progression. The central objective of our division is to understand the complex molecular mechanisms that have evolved in the regulation of signaling networks and how these impact on cancer development, metastasis, and drug resistance. To this end, we generate and maintain resources for large-scale experimentation, apply high-throughput functional genomics and proteomics technologies, and analyze candidate genes using in vitro as well as in vivo systems. Effects of perturbations (gene gainand loss-of-function, miRNA, drugs) imposed on the signaling processes are experimentally tested and then computationally modeled. This generates mechanistic knowledge that is exploited to identify new diagnostic and prognostic markers as well as to develop novel Im Neuenheimer Feld 580 69120 Heidelberg Phone: +49 6221 42 4646 [email protected] strategies for therapeutic intervention. Our major focus here is on breast cancer, where we investigate protein and non-protein factors that are involved in the progression of different subtypes via their activities in interrelated signaling networks. Future Outlook: Our future research is mostly in two directions. We have already seen from our current data that signaling is not regulated in isolated pathways, but rather in complex networks. Therefore, in the future we will investigate the impact individual perturbations have in a variety of cellular pathways and at different levels (DNA, RNA, protein, metabolite, …, phenotype). This should provide us with a better understanding of the connectivity in multi-layer interaction systems. Such information will be essential, for example, to identify strategies that should help to overcome drug resistance While much of our current knowledge is based on in vitro experiments, we need to validate findings in vivo in order to prove their relevance. To this end, we will generate and test animal models and challenge our hypotheses with patient samples. Collaborations to this end have been established and first promising results have already been obtained. ESSENTIAL PUBLICATIONS: (1.) Ward A. et al. (2013). Re-expression of microRNA375 reverses both tamoxifen resistance and accompanying EMT-like properties in breast cancer. Oncogene, 32, 1173–82, doi:10.1038/onc.2012.1128. Elucidating the regulation of signaling via miRNAs. Breast cancer cells were transfected with a library of 810 human miRNA mimics and induced effects were analyzed by quantitative analysis of proteins in the EGFR signaling network. Thus activating and inhibiting effects on protein abundance could be identified (A). This led to the identification of proteins (blue) being co-regulated by several miRNAs (orange), as well as miRNAs co-regulating several proteins (B). Activating edges are in red, inhibiting edges in green. 64 Research Program (2.) Götschel F. et al. (2013). Synergism between Hedgehog-GLI and EGFR Signaling in HedgehogResponsive Human Medulloblastoma Cells Induces Downregulation of Canonical Hedgehog-Target Genes and Stabilized Expression of GLI1. PLoS One, 8(6): e65403. (3.) Uhlmann S. et al. (2012). Global microRNA level regulation of EGFR-driven cell-cycle protein network in breast cancer. Mol Syst Biol, 8, 570. (4.) Keklikoglou, I. et al. (2012). MicroRNA-520/373 family functions as a tumor suppressor in estrogen receptor negative breast cancer by targeting NF-kappaB and TGF-beta signaling pathways. Oncogene, doi:10.1038/onc.2012.1128. Structural and Functional Genomics Molecular Genetics Division Head: Prof. Dr. Peter Lichter Our laboratory applies oncogenomic approaches for the elucidation of pathomechanisms of tumor etiology and progression and for the identification of prognostic and predictive genes and gene-signatures. To this end, we perform large screens by using comprehensive molecular profiling technologies revealing tumor-cell alterations at the level of the genome, the transcriptome and the epigenome. Integration of such data sets with clinical data allows us to identify candidate genes which are subsequently tested for their i) possible role in tumor pathomechanisms, ii) potential as target for novel therapy-strategies, iii) prognostic value to stratify patient subgroups for risk-adapted therapy regimens and iv) potential to predict therapy response or resistance in cancer patients. Major accomplishments of the last 5 years: We have greatly contributed to novel tumor sub-classification schemes that allow stratification of cancer patients for different therapy regimens on the basis of the genetic tumor profiles. We have assessed predictive gene signatures in a clinical treatment trial testing neo-adjuvant protocols in breast cancer. Through the identification of pathogenically relevant genes, we have identified candidate targets for the development of novel therapies, in particular in human leukemia, head and neck tumors, gliomas and colorectal cancer. Through the functional characterization of candidate genes we also developed pre-clinical models for the testing of novel therapies. also extended to other tumor entities. Furthermore, we wish to implement a strategy for the establishment of cancer genome sequencing in a clinical diagnostic setting, following a three-step procedure: i) sequencing of 50 to 100 candidate genes of oncogenic relevance in large series of tumors accompanying existing treatment trials, ii) sequencing of the entire exome of respective tumor cases, and iii) sequencing of whole genomes of selected cases and assessment of the conditions for whole genome sequencing in future comprehensive diagnostic setting. Candidate genes, for which we have established a pathogenic role in carcinogenesis, are currently being tested in preclinical in vitro and in vivo models using known inhibitors. We plan to complement these studies by the isolation of novel inhibitors exploiting the DKFZ/EMBL core facility for the screening of small molecular libraries as well as the screening of biological extracts through dedicated scientific collaborations. A third focus is the transfer of biomarkers in gene signatures into clinical settings through prospective diagnostic trials, preferably associated to current treatment trials. ESSENTIAL PUBLICATIONS: Molecular Genetics (B060) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4619 [email protected] (1.) Gronych J. et al. (2011). An activated mutant BRAF kinase domain is sufficient to induce pilocytic astrocytoma in mice. J Clin Invest, 121, 1344–1348. (2.) Barbus S. et al. (2011). Differential retinoic acid signaling in tumors of long- and short-term glioblastoma survivors. J Natl Cancer Inst, 103, 598–606. (3.) Seiffert M. et al. (2010). Soluble CD14 is a nov- Future Outlook: One of our major goals is to apply sequencing of the genomes of cancer cells to identify the entire spectrum of genetic alterations that may occur in a given tumor entity and to assess their clinical relevance. This is done with special focus on pediatric brain tumors, but el monocyte-derived survival factor for chronic lymphocytic leukemia cells, which is induced by CLL cells in vitro, and present at abnormally high levels in vivo. Blood, 116, 4223–4230. (4.) Pfister S. et al. (2008). BRAF gene duplication constitutes a novel mechanism of MAPK pathway activation in low-grade astrocytomas. J Clin Invest, 118, 1739–1749. Research at DKFZ 2014 65 Structural and Functional Genomics Pediatric Neurooncology Division Head: Prof. Dr. Stefan Pfister Pediatric Neurooncology is currently a vibrant field of research, with countless critical achievements in recent years in understanding the molecular biology of childhood brain tumors and translating molecular findings into clinical practice. This is desperately needed from a clinical perspective, since brain tumors have become the number one cause of cancerrelated mortality in children. Our group aims to bridge the gap between generating genomic screening data (microarray-based as well as next-generation sequencing) and exploiting these data for the sake of our patients. The first goal includes the identification, validation and clinical application of prognostic and predictive biomarkers in different childhood brain tumors, including medulloblastoma, ependymoma, pilocytic astrocytoma and glioblastoma. The second major focus involves the systematic pre-clinical testing of novel smart drugs, often in combination with established cytotoxic drugs and/or chemotherapy, to treat models (in vitro and in vivo), and ultimately patients, based on the genetic/molecular signature of the individual tumor (“personalized cancer care”). Pediatric Neurooncology (B062) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4618 [email protected] and Department of Pediatric Hematology and Oncology, Heidelberg University Hospital Future Outlook: The immense biological heterogeneity of childhood brain tumors between and within tumors, which is a prerequisite for targeted treatment approaches, is still poorly understood und thus currently hindering such approaches on a regular basis in the clinic. To overcome this shortcoming, we will continue to comprehensively investigate the entire genetic diversity of childhood brain tumors within and across histopathological entities. A large and continuously growing repertoire of preclinical models will allow us to specifically test biological hypotheseses gained from genome-wide primary tumor analyses in vitro and in vivo, before they are recommended for use in patients. Another focus will be the analysis of clonality within tumors, their respective metastases, and tumor relapses, by ultra-deep next-generation sequencing techniques. This should allow us to appropriately consider the biological importance of subclones already in the primary tumor that confer tumor dissemination, local re-growth, and therapy resistance. As a third major focus, we have started focusing on the detection of tumor-specific alteration in body fluids, such as cerebrospinal fluid and plasma, which can be exploited for molecular diagnostics, tumor cell clearance (minimal residual disease), detection of molecular targets, and primary resistance mechanisms. ESSENTIAL PUBLICATIONS: (1.) Bender S. et al. (2013). Reduced H3K27me3 and DNA hypomethylation are major drivers of gene expression in K27M-mutant pediatric high-grade gliomas. Cancer Cell, accepted. (2.) Jones DT. et al. (2013). Recurrent somatic alterations of FGFR1 and NTRK2 in pilocytic astrocytoma. Nat Genet, 45, 927–932. (3.) Sturm D. et al. (2012). Hotspot mutations in H3F3A and IDH1 define distinct epigenetic and biological Medulloblastoma showing high level amplifications of MYCN (red signal) and GLI2 (green signal) in different cells of the same tumor. 66 Research Program subgroups of glioblastoma. Cancer Cell, 22, 425–437. (4.) Jones D.T. et al. (2012). Dissecting the genomic complexity underlying medulloblastoma. Nature, 488, 100–105. Structural and Functional Genomics Functional Genome Analysis Division Head: Dr. Jörg D. Hoheisel Research at the Division of Functional Genome Analysis focuses on the development and immediate application of new technologies for analysis, assessment and description of both the realisation and regulation of cellular function from genetic information. Analysis of tumour material is the prime focus, with a particular emphasis on pancreatic cancer. Parallel studies on an international scale are under way, for example, on the epigenetic modulation of gene promoters, variations in transcription factor binding, changes at transcript levels of coding and non-coding RNAs, differences in the actual protein expression and the occurrence and ratio of protein isoforms, as well as the intensity of protein interactions. From the resulting data, we strive to understand cellular regulation and its biological consequences. In combination with clinical data, this knowledge is used for the creation of a means of reliable, possibly early and non-invasive diagnosis, accurate prognosis and patient stratification, monitoring of treatment results and the establishment of new therapeutic approaches. As a consequence of the immense amount of information available at the level of nucleic acids, developments and applications in the field of affinity-based analysis of the proteome have become a technology focus, since technological and analytical processes in this area are still inadequate for many, in particular biomedical, purposes. Future Outlook: A more recent line of work aims at in vitro implementation of complex biological processes. Our goal is utilisation in the area of synthetic biology for the production of molecules and the establishment of artificial molecular systems. Cell-free biosynthetic production will be critical for many biotechnological and pharmacochemical challenges ahead. Artificial experi- Research at DKFZ 2014 mental systems, on the other hand, will complement current systems biology, evaluating biological models experimentally. Similar to physics, insight into cellular functioning will be gained by an iterative processing of information by experimental and theoretical systems biology. Eventually, this may lead to the establishment of a fully synthetic self-replicating system and, ultimately, an archetypical model of a cell. ESSENTIAL PUBLICATIONS: (1.) Schröder C. et al. (2010). Dual-color proteomic profiling of complex samples with a microarray of 810 cancer-specific antibodies. Mol. Cell. Prot., 9, 1271– 1280. (2.) de Souza Rocha Simonini P. et al.(2010). Epigenetically de-regulated microRNA-375 activates Estrogen Receptor alpha activity in breast cancer. Cancer Res., 70, 9175–9184. (3.) Holtrup F. et al. (2011). Nemorosone specifically inhibits growth of pancreatic cancer cells and induces Functional Genome Analysis (B070) apoptosis via activation of the unfolded protein re- German Cancer Research Center sponse (UPR). Brit. J. Pharmacol., 162, 1045–1059. Im Neuenheimer Feld 280 (4.) Fredebohm, J. et al. (2013). Depletion of RAD17 sensitizes pancreatic cancer cells to gemcitabine. J. Cell Sci. ,126, 3380–3389. 69120 Heidelberg Phone: +49 6221 42 4680 [email protected] Protein profile of urine samples from cancer patients and healthy donors. Samples are depicted as squares coloured according to disease-state and gender; black spots represent proteins that contribute to the diagnosis. As can be seen from the plot, discrimination between cancer and healthy is nearly as good as discrimination between men and women. 67 Structural and Functional Genomics Theoretical Bioinformatics Division Head: Prof. Dr. Roland Eils Theoretical Bioinformatics (B080) German Cancer Research Center Im Neuenheimer Feld 580 69120 Heidelberg Phone: +49 6221 42 3600 [email protected] Using current DNA sequencing methods, it is today feasible to determine the sequence of a human individual (e.g. a patient suffering from cancer) in a single day. Other complementary technologies, such as epigenome, transcriptome, proteome or metabolome analysis, deliver additional data with a great potential for precise diagnostics. Given the enormous technological advances in data generation, the integration of these data in order to generate new insights into complex biological functions is still a major challenge and can only be achieved with interdisciplinary approaches. Our division is developing computer-assisted methods for interpreting complex genomic and other biological data, as well as methods for modeling and simulation of biological processes. Major activities include the development of integrated bioinformatic approaches for the interpretation and management of cancer genome and accompanying clinical data, the application of state-of-the-art technologies in automated live-cell imaging and image analysis, experimental and theoretical systems biology approaches addressing key cellular mechanisms and their distortions in cancer cells, as well as the development of new synthetic biology tools to manipulate cellular processes. For this purpose, the division is integrating systems biology, automated image processing, state of the art light-microscopy, cell biology and bioinformatics. Scheme representing the phenomenon of X chromosome hypermutation. Cancer cells from female patients carry significantly more mutations (orange triangles) on the inactive X-chromosome (left) than on the active X-chromosome (right). 68 Research Program Future Outlook: Our overarching aim is the development of new insights linking alterations in cancer, or other diseased cells, with biological functions in order to find new potential targets for improved diagnostics and treatment. Therefore, we develop integrated platforms combining bioinformatic data analysis and mathematical modeling of complex diseases processes. In the future, these systems medicine platforms will provide computer-assisted diagnostics and therapy decision tools to support medical doctors in patient care. ESSENTIAL PUBLICATIONS: (1.) Jäger N. et al. (2013). Hypermutation of the Inactive X Chromosome Is a Frequent Event in Cancer. Cell , 155, 1–15. (2.) Jones DTW. et al. (2013). Recurrent somatic alterations of FGFR1 and NTRK2 in pilocytic astrocytoma. Nat Genet, 45, 927–932. (3.) Jones DTW. et al. (2012). On behalf of the ICGC PedBrain Tumor Project. Dissecting the genomic complexity underlying medulloblastoma. Nature, 488, 100–105. (4.) Neumann L. (2010). Dynamics within the CD95 death-inducing signaling complex decide life and death of cells. Molecular Systems Biology, 6, 352. Structural and Functional Genomics Theoretical Systems Biology Division Head: Prof. Dr. Thomas Höfer The division of Theoretical Systems Biology pursues multidisciplinary research to understand how biological function emerges from interacting components – molecules within a cell and cells within an organism. Our work is essentially collaborative and characterized by a tight interplay between experimentation, data analysis and mathematical modeling. We dissect the molecular switches that regulate the proliferation and differentiation of T lymphocytes and thus, orchestrate adaptive immune responses. The second focus of the division is on growth-factor signaling and cell-cycle control. We study the interplay of these processes in human tumor models to understand how therapy resistance arises from synergistic oncogene action. From both strands of work common principles at the systems level are emerging. Our work aims at identifying the functional behavior of molecular networks in the cell and at quantifying the control exerted by individual components to inform novel therapeutic approaches. Future Outlook: A key challenge of quantitative biology is to understand the interplay between molecular modules – such as those controlling the induction and maintenance of expression of master transcription factors for cell fate – and genome-wide programs that mediate coordinated cell function. ESSENTIAL PUBLICATIONS: (1.) Rand U. et al. (2012). Multi-layered cellular stochasticity and paracrine amplification shape the type-I interferon response. Mol. Syst. Biol., 8, 584. (2.) Luijsterburg M.S. et al. (2010). Stochastic and reversible assembly of a multiprotein DNA repair complex ensures accurate target site recognition and efficient repair. J. Cell Biol.,189, 445–463. (3.) Busse D. et al. (2010). Competing feedback loops shape IL-2 signaling between helper and regulatory T cells in cellular microenvironments. Proc. Natl. Acad. Theoretical Systems Biology (B086) Sci. USA, 107, 3058–3063. German Cancer Research Center (4.) Schulz E. et al. (2009). Sequential polarization Im Neuenheimer Feld 267 and imprinting of T-helper type 1 differentiation by interferon-γ and interleukin-12. Immunity, 30, 678– 688. 69120 Heidelberg Phone: +49 6221 54 51380 [email protected] Tracking of individual tumor cells in the fluorescence microscope. Research at DKFZ 2014 69 Structural and Functional Genomics Signaling and Functional Genomics Division Head: Prof. Dr. Michael Boutros Signaling and Functional Genomics (B110) German Cancer Research Center Im Neuenheimer Feld 580 69120 Heidelberg Phone: +49 6221 42 1951 [email protected] Cellular signaling systems control many key decisions during development, stem cell maintenance and tumorigenesis. The focus of our group is on the systematic dissection of signaling pathways to identify novel molecular processes and to understand how pathways connect in cellular networks. We use genetic and genomic approaches for this purpose, but also study specific processes at the molecular level to probe underlying mechanisms. We pursue two main lines of research: 1. Systematic analysis of Wnt signaling in model organisms and tumor cells. Canonical and non-canonical Wnt signaling play key roles during development and tumorigenesis. Aberrant regulation of Wnt signaling has been implicated in cancer, as exemplified by mutations in APC, a negative regulator of Wnt signaling. During the past years, our laboratory has contributed to the molecular understanding of Wnt signaling by identifying novel components and by the characterization of Wnt-ligand specific cargo receptors. 2. Systems genetics and synthetic lethality. Genetics underlying many phenotypes, including most common diseases, are complex with contributions from multiple loci. The analysis of synthetic genetic interaction networks reveals how biological systems achieve a high level of complexity with a limited repertoire of components. We have established high-thoughput methodologies to measure synthetic genetic interaction in model organisms and cancer cells by RNAi. Future Outlook: We are interested in the systematic analysis of synthetic genetic interactions to dissect genotype-phenotype relationships, with a particular focus on combinatorial mapping approaches using RNAi and small molecules. Interactions between genetic variants may be one important explanation for the ‘missing heritability’ in genome-wide association studies. Extensive interactions between different genetic alleles with large effects on many phenotypes have been documented in many model systems. We will use quantitative phenotyping by highthroughput microscopy to measure synthetic genetic interactions. Genetic interaction data will be used to model cellular networks with a particular focus on oncogenic signaling pathways. We will also develop novel technologies required for miniaturization of cellular assays and high-throughput imaging, for reproducible cell-based RNAi in primary cell types and novel approaches to data integration. A second area of interest is the in-depth analysis of Wnt and interacting signaling networks in development, stem and tumor cells. We use a spectrum of model systems, from Drosophila to mouse and human cancer cells to identify key components and understand how they are embedded into physiological processes. For more information, visit us at www.dkfz.de/signaling ESSENTIAL PUBLICATIONS: (1.) Horn T. et al. (2011). Mapping of signaling networks through synthetic genetic interaction analysis by RNAi. Nature Methods, 8, 341–346. (2.) Gross, J. C. et al. (2012). Active Wnt proteins are secreted on exosomes. Nature Cell Biology, 14, 1036– 1045. (3.) Boutros M. & Ahringer J. (2008). The art and design of genetic screens: RNA interference. Nature Reviews Genetics, 9, 554–566. (4.) Bartscherer, K. et al. (2006). Secretion of Wnt ligands requires Evi, a conserved transmembrane protein. Cell, 125, 523–33. 70 Research Program Research at DKFZ 2014 By silencing genes using RNAi we can analyse the genes’ effect in a quantitative and high-throughput manner. In this microscopy image of human cancer cells, nuclei are shown in red, cell membranes in green, and the cellular scaffolding in blue. 71 Structural and Functional Genomics Signal Transduction in Cancer and Metabolism Division Head: Dr. Aurelio Teleman Signal Transduction in Cancer and Metabolism (B140) When cancer cells proliferate to form a tumor, they need to grow and to divide. Regulation of cell division (i.e. the cell cycle) has been extensively studied. In comparison, the mechanisms regulating cell growth (i.e. the accumulation of cell mass) are less well understood. The Teleman lab studies cell growth and its regulation. For cells to grow, they need to produce biosynthetic building blocks such as nucleotides, amino acids and lipids. Consequently understanding cell growth requires understanding metabolism. Cells decide to grow, however, based on information coming from outside the cell, such as the presence of nutrients and growth factors. Cells receive and process this information via signaling pathways such as the insulin pathway. Consequently understanding cell growth also requires understanding signaling pathways. Finally, the signaling pathways regulate the metabolic pathways, therefore the lab also studies the interface between signaling and metabolism. Both the metabolic pathways, as well as the signaling pathways, are complex and intricate networks. These pathways, however, are conserved amongst animals. The Teleman lab studies these pathways using a combination of human tissue culture together with the fruitfly Drosophila, since Drosophila is simplified and genetically tractable compared to mammals. Future Outlook: The aim of our work is to understand the processes regulating cell growth so that this knowledge can be used in the future for cancer therapy. Unlike other cells in the body, cancer cells have mutations that promote cell growth. Blocking this process will hopefully be a powerful method to specifically and efficiently inhibit tumor progression. ESSENTIAL PUBLICATIONS: German Cancer Research Center (1.) Xu X. et al. (2012). Insulin signaling regulates fat- Im Neuenheimer Feld 580 ty acid catabolism at the level of CoA activation. PLoS Genetics, 8, e1002478. 69120 Heidelberg (2.) Pallares C. et al. (2012). Tissue-specific coupling Phone: +49 6221 42 1620 between insulin/IGF and TORC1 signaling via PRAS40 [email protected] in Drosophila. Developmental Cell, 22, 172–182. (3.) Hahn K. et al. (2010). PP2A regulatory subunit PP2A-B’ counteracts S6K phosphorylation. Cell Metabolism, 11, 438–444. (4.) Francis V. et al. (2010). dDOR is an ecdysone receptor coactivator that forms a feed-forward loop connecting insulin and ecdysone signaling. Current Biology, 20, 1799–1808. Location of adipose tissue in an adult fly revealed by GFP expression. 72 Research Program Structural and Functional Genomics Molecular RNA Biology and Cancer Helmholtz University Junior Research Group Head: Dr. Sven Diederichs A large fraction of the human genome is transcribed into RNA (more than 70%), while only 2% are protein-encoding. These recent insights into RNA biology induced a paradigm shift towards the recognition of RNAs as functionally important molecules – beyond serving as messengers for protein-encoding genes. Non-protein-coding RNAs execute important functions in the cell. Short non-coding RNAs, the microRNAs, play important roles in gene regulation. The tumor-suppressive or oncogenic role of many microRNAs and their frequent deregulation in tumors allow a first glimpse of the striking role that non-coding RNAs can play in cancer. Novel long non-coding RNAs (ncRNA, lncRNA, lincRNA) fulfill important functions ranging from epigenetic gene regulation to scaffolding functions in the cytoplasm. Taken together, the human cell contains many more RNAs than previously anticipated and many of them might just await their discovery as functionally important molecules. Since cancer is – in most cases – a disease of the genome, that is caused by the deregulation of oncogenes and tumor suppressor genes, we are convinced that all parts of the human genome are important to study in tumor biology, not restricted to the 2% protein-coding information. Our research focuses on the new and innovative research area of long non-coding RNAs and their role in cancer. We elucidate the expression patterns, regulatory mechanisms and cellular and molecular functions of lncRNAs relevant to cancer. The fascination as well as the major challenge in lncRNA research is driven by the fact that each lncRNA can have a different function and a different mechanism, so that many important discoveries and insights into the molecular mechanisms underlying tumorigenesis can be expected from this field. silence lncRNAs in cancer cells and RNA Affinity Purification to identify the interactomes of cancer-associated lncRNAs. To further generate hypotheses on the lncRNA functions, we use bioinformatic guilt-by-association studies. To accelerate our discoveries of novel lncRNAs in cancer, we have developed an siRNA library specifically targeting 638 cancer-associated lncRNAs identified in our screen and allowing their rapid functional characterization. One example nicely illustrates our research approach: We identified the lncRNA MALAT1 (Metastasis-Associated in Lung Adenocarcinoma Transcript 1) as a biomarker associated with a poor prognosis and the development of distant metastasis in lung cancer (Oncogene 2003). We then developed a novel approach to quantitatively silence this lncRNA in lung cancer cells by genome editing (Genome Res 2011). This loss-of-function revealed that MALAT1 was essential for cell migration and metastasis in a xenograft mouse model. Joining forces with ISIS Pharmaceuticals, we developed an inhibitor for MALAT1, an Antisense Oligonucleotide (ASO), which effectively reduced MALAT1 in the mouse model and suppressed lung cancer metastasis (Cancer Res 2013). At the molecular level, we identified MALAT1 as an epigenetic regulator inducing a signature of metastasisassociated genes. In summary, MALAT1 can serve as a biomarker and is an essential player and promising therapeutic target for metastasis prevention in lung cancer. ESSENTIAL PUBLICATIONS: (1.) M Hämmerle M.* et al. (2013). Post-transcriptional destabilization of the liver-specific long non-coding RNA HULC by the IGF2 mRNA-binding protein 1 (IG- Molecular RNA Biology and Cancer (B150) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4380 [email protected] The lncRNA MALAT1 is a marker for metastasis development in lung cancer and associated with poor survival (Oncogene 2003). Its suppression using a novel silencing approach based on genome editing (Genome Res 2011) prevents the development of lung cancer metastasis in MALAT1KO cells (Cancer Res 2013). F2BP1). Hepatology, 58, 1703–1712. (2.) Liu M. et al. (2013) The IGF2-intronic miR-483 selectively enhances transcription from IGF fetal pro- Future Outlook: As a thriving research area, we analyze long non-coding RNAs (lncRNA) and their role in cancer. After profiling the expression of thousands of lncRNAs in three tumor entities – lung, liver and breast cancer – we elucidate the cellular and molecular function of lncRNAs regulated in cancer. Here, we use innovative techniques like Genome Editing to Research at DKFZ 2014 moters and enhances tumorigenesis. Genes Dev., in press. (3.) Gutschner T. et al. (2013). The non-coding RNA MALAT1 is a critical regulator of the metastasis phenotype of lung cancer cells. Cancer Res., 73, 1180–1189. (4.) Gutschner T. et al. (2011). Non-coding RNA gene silencing through genomic integration of RNA destabilizing elements using zinc finger nucleases. Genome Res., 21, 1944–1954. 73 Structural and Functional Genomics Systems Biology of Cell Death Mechanisms Junior Research Group Head: Dr. Nathan Brady Systems Biology of Cell Death Mechanisms (B170) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 54 51322 [email protected] 74 We are investigating the control and crosstalk between programmed cell death (PCD) mechanisms of apoptosis, autophagy and necrosis in pancreatic, breast and brain cancer cells. Apoptosis, the most studied PCD mode (Type I), is activated by either the death receptor or the mitochondrial pathway. Autophagy is a process by which intracellular components are sequestered by autophagosomes, which then fuse with and are degraded by lysosomes. In the cancer cell autophagy can paradoxically act as either an alternative cell death pathway (Type II PCD) or as a potent survival response to stress, e.g. hypoxia and chemotherapies. Although considered a passive cell death, many pathways are common to necrosis and PCD modes. In contrast to apoptosis, necrosis is inflammatory due to the rupture of the plasma membrane and the release of specific cytosolic components. As apoptosis does not generate an immune response, the strict focus on apoptosis-inducing therapies may not be fully productive. Furure Outlook: The group “Systems Biology of Cell Death Mechanisms (B170)” is part of the SBCancer network within the Helmholtz Alliance on Systems Biology and is located in BioQuant, Heidelberg University’s center for quantitative biology. Furthermore the group is closely cooperating with the European Pancreas Center at Heidelberg University Hospital headed by Prof. Dr. Markus Wolfgang Büchler. ESSENTIAL PUBLICATIONS: (1.) Zhu Y. et al. (2013). Modulation of serines 17 and 24 in the LC3-interacting region of Bnip3 determines pro-survival mitophagy versus apoptosis. J Biol Chem., 288, 1099–1113. (2.)Hundeshagen P. et al. (2011). Concurrent detection of autolysosome formation and lysosomal degradation by flow cytometry in a high-content screen for inducers of autophagy. BMC Biol, 9, 38. (3.) Wild P. et al. (2011). Phosphorylation of the Autophagy Receptor Optineurin Restricts Salmonella Growth. Science. 333, 228–233. (4.) Hamacher-Brady A. et al. (2011). Artesunate acti- Our research is aimed at revealing how individual pathway activities and crosstalk between PCD pathways can be tuned to optimize intrinsic and extrinsic pancreatic cancer cell death. Using high-resolution imaging of high-content biosensors we quantitatively map activities and interdependencies of PCD modes. This approach achieves superior information content than commonly reported population-averaged and representative responses. Measured activities and dependencies, including proteinprotein interactions, inter and intra-organellar communication, and bi-directional cell-to-cell signaling are analyzed using computational modeling approaches, with the aim of integrating qualitative and quantitative multi-parametric, multivariate datasets. Our overall goal is to predict and test chemotherapies which will optimize both initial PCD responses, as well as promote an immunogenic response to induce secondary killing of cancer cells by the immune system. Research Program vates mitochondrial apoptosis in breast cancer cells via iron-catalyzed lysosomal reactive oxygen species production. J Biol Chem, 286, 6587–6601. 3D reconstruction of mitochondria (green), lysosomes (red) and nuclei (grey). In response to artesunate, lysosomes cluster asymmetrically at the nucleus. Pro-death signaling from lysosomes induces mitochondrial fragmentation and convert mitochondria into inducers of cell death via cytochrome c release. Research at DKFZ 2014 75 Structural and Functional Genomics Proteostasis in Neurodegenerative Disease CHS Junior Research Group (in Cooperation with Heidelberg University) Head: Dr. Thomas Jahn Proteostasis in Neurodegenerative Disease (B180) CHS Research Group at CellNetworks Heidelberg University and DKFZ German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42-1551 [email protected] One of the essential characteristics of living systems is the ability of their molecular components to self-assemble into functional structures and to balance their organisation within the cellular environment through the mechanism of homeostasis. It is clear that protein homeostasis, or proteostasis, is closely coupled to many other biological processes ranging from the trafficking of molecules to specific cellular locations to the regulation of the growth and differentiation of cells. In addition, only correctly folded proteins have the ability to remain soluble in crowded biological environments and to interact selectively with their natural partners. It is, therefore, not surprising that the failure of proteostasis mechanisms underpins the pathogenesis of common diseases of old age, most notably, cancer and neurodegenerative diseases such as Alzheimer’s and Parkinson’s disease. In many such diseases proteins self-assemble in an aberrant manner into large molecular aggregates, including soluble oligomeric species and amyloid fibrils. Arguably, strategies to ameliorate misfolding and aggregation will depend on a detailed understanding of manipulators of the proteostasis network. Future Outlook: The main interest of our lab is to advance our understanding of the molecular events triggered by protein misfolding and the subsequent impact of protein aggregation on cellular integrity. We combine biochemical and molecular biological studies to tackle questions such as: What are the characteristics of aggregated protein species accumulating in vivo? How are specific species toxic to cells? Which cellular mechanisms can be modified to rescue proteostasis? To address these questions we combine protein engineering with the wide range of genetic and molecular techniques available in cell culture and Drosophila melanogaster. We are also very interested in establishing novel experimental tools, which include for example the quantitative analysis of Drosophila models and the in vivo characterisation of protein-protein interactions. Hopefully, understanding the detailed molecular processes leading to protein misfolding will open new routes towards the design and development of rational treatments for these debilitating diseases. ESSENTIAL PUBLICATIONS: (1.) O’Sullivan et al. (2012). Reticulon-like-1, the Drosophila orthologue of the Hereditary Spastic Paraplegia gene reticulon 2, is required for organization of endoplasmic reticulum and of distal motor axons. Hum Mol Genet. 21, 3356–3365. (2.) Jahn T.R. et al. (2011). Detection of Early Locomotor Abnormalities in a Drosophila Model of Alzheimer’s Disease by a Three-Dimensional Tracking System. J. Neuroscience Methods. 197, 186–189. (3.) Jahn T.R. et al. (2008). A common β-sheet archi- Schematic energy landscape for protein folding and aggregation (see Jahn & Radford FEBS J. 2005). The competition between unimolecular folding and aggregate formation is intricately balanced by the cellular proteostasis network. tecture underlies in vitro and in vivo β2-microglobulin amyloid fibrils. J. Biol. Chem., 283, 17279–17286. (4.) Jahn T.R. et al. (2006). Amyloid formation under physiological conditions proceeds via a native-like folding intermediate. Nature Struct. Mol. Biol., 13, 195–201. This Junior Research Group is generously supported by the Chica-and-Heinz-SchallerFoundation (CHS). 76 Research Program Structural and Functional Genomics Lysosomal Systems Biology Junior Research Group Head: Dr. Anne Hamacher-Brady Programmed cell death (PCD) is regulated by the spatially- and temporally- co-ordinated interplay of genetically defined signaling pathways. The understanding of PCD is of central importance, in that its successful execution is the key to cancer therapy. As fundamental discoveries concerning PCD mechanisms, or even new modes of PCD, are still being reported, addressing the complexity of PCD signaling is a growing challenge. Systems biology offers tools to utilize such biological complexity through full data integration and mathematically-derived non-intuitive hypothesis generation. Intriguingly, PCD undergoes substantial positive and negative regulation by the endolysosomal compartment. logical modeling approaches, and are translating the achieved results to the organism level. Primary goals are the systemic identification of regulatory mechanisms governing lysosomal and PCD signaling pathways and confirmation of in vivo functionality. Our research will yield insights into specific mechanisms for optimizing cancer cell death. This junior research group is funded by the Federal Ministry of Education and Research (BMBF). ESSENTIAL PUBLICATIONS: (1.) Zhai Z. et al. (2012). Antagonistic regulation of differentiation and apoptosis by the Cut transcription factor represents a tumor suppressing mechanism in Drosophila. PLoS Genet., 8(3):e1002582 . (2.) Hamacher-Brady A. et al. (2011). Artesunate acti- Future Outlook: This junior research group is dedicated to the elucidation of lysosomal control of PCD in cancer versus non-cancer cells, with an emphasis on the cell culture experiments-based generation of theoretical model predictions, and testing of the in vivo-functionality in the model organism C. elegans. To that end, we are integrating quantitative fluorescence microscopy and biochemical methods with systems bio- vates mitochondrial apoptosis in breast cancer cells via iron-catalysed lysosomal reactive oxygen species Lysosomal Systems Biology (B190) production. J Biol Chem., 285,6587–6601. BMBF e:Bio Junior Research Group (3.) Hamacher-Brady A. et al. (2007). Response to my- German Cancer Research Center ocardial ischemia/reperfusion injury involves Bnip3 BIOQUANT and autophagy. Cell Death Differ., 14, 146–157. (4.) Hamacher-Brady A. et al. (2006). Enhancing mac- Im Neuenheimer Feld 267 roauto-phagy protects against ischemia/reperfusion 69120 Heidelberg injury in cardiac myocytes. J Biol Chem., 281, 29776– Phone: +49 6221 54 51357 29787. [email protected] Metabolic stress-induced, E3 ligasemediated mitochondrial K63 ubiquitin chaining in breast cancer cells. In this image mitochondria are labeled in red, K63 ubiquitin chains in green, E3 ligase in blue. Research at DKFZ 2014 77 Coordinator Prof. Dr. Kari Hemminki Cancer Risk Factors and Prevention About 210,000 people in Germany die of cancer each year. 470,000 new cancer cases are diagnosed yearly. Significant progress in prevention, diagnosis, and treatment of cancer has been made possible through recent research results in the field of molecular biology. Our research program is concerned with identifying risk factors (primary prevention), early detection (screening), and approaches to prevent disease progression (chemoprevention). The German Cancer Research Center occupies a leading position in the area of epidemiological studies as well as in nutrition sciences, biostatistics, and the application of biomarkers (characteristic biological features that are key for the prognosis or diagnosis of cancer). We expect that it may be possible to prevent up to 30 percent of new cancer cases within the next 20 to 30 years. To reach this goal, the main activities of the research program are focused on: • • • • • • • 78 integrating laboratory research, epidemiology, and clinical studies compiling and extending collections of biological samples and databases integrating genome, proteome, and biomarker research into epidemiological and clinical studies on the causes and prevention of cancer studies to identify causal connections such as between diet and cancer educational measures research and quality control related to tests and early detection programs research in the fields of biostatistics and methodological consulting Research Program Research at DKFZ 2014 79 Cancer Risk Factors and Prevention Epigenomics and Cancer Risk Factors Division Head: Prof. Dr. Christoph Plass Epigenomics and Cancer Risk Factors (C010) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3300 [email protected] Aberrant DNA methylation is an early event in tumorigenesis and a major contributor in the development of solid tumors as well as leukemias. As an epigenetic alteration, DNA methylation does not change the sequence of a gene and thus offers the exciting possibility for therapeutic removal of the methylation group by demethylating drugs. Deregulation of mechanisms that control the establishment of normal DNA methylation patterns leads to both extensive aberrant hypo- and hypermethylation and has been described for several human malignancies. Global DNA hypomethylation in human cancers was one of the earliest changes associated with tumor progression. Our group has shown that human malignancies are characterized by extensive promoter CpG island methylation with non-random and tumor-type specific patterns. It is currently unknown how tumors acquire aberrant DNA methylation patterns. Our division is interested in the molecular mechanisms underlying the initiation and progression of malignant cell growth. In particular, we are focusing our attention on the contribution of epigenetic alterations in this process and to determine how epigenetic and genetic alterations cooperate during tumorigenesis. In our studies we are utilizing current state-of-the-art high throughput epigenomic assays (e.g. Methylation arrays, Next generation sequencing and MassARRAY) on clinical samples, cell culture models or mouse tumor models. Future Outlook: Epigenetics is a fast evolving field with links to many research directions in cancer research. A challenge here will be to integrate epigenetic questions with other data sets. For example, the profiling of cancer genomes relied heavily in the past on the description of genetic alterations. Now epigenetic datasets will need to be integrated in order to completely understand the molecular defects in cancer. Our division will focus on four major research directions: • Evaluation of genome-wide epigenetic patterns in tumor genomes • Identification of novel cancer genes and pathways targeted by epigenetic alterations • Determining the role of epigenetics in cancer risk and progression • Evaluate the role of epigenetics in the regulation of DNA repair ESSENTIAL PUBLICATIONS: (1.) Raval A. et al. (2007). Downregulation of death-associated protein kinase 1 (DAPK1) in chronic lymphocytic leukemia. Cell, 129, 879–890. (2.) Chen S.S. et al. (2009). Epigenetic changes during disease progression in a murine model of human chronic lymphocytic leukemia. Proc. Natl. Acad. Sci., 106, 13433–13438. (3.) Plass C. et al. (2013). Mutations in regulators of the epigenome and their connections to global chromatin patterns in cancer. Nat Rev Genet., 14, 765–780. (4.) Wang Q. et al. (2013). Tagmentation-based wholegenome bisulfite sequencing. Nat Protoc., 8, 2022– 2032. DAPK1 Mass Array 80 Research Program Cancer Risk Factors and Prevention Cancer Epidemiology Division Head: Prof. Dr. Rudolf Kaaks Our division studies the causes of cancer in population groups with the aim of identifying and, if possible, avoiding risk factors so as to prevent cancer. Our key focus is on the quantification of risks associated with lifestyle, nutrition and metabolism. In addition, we address the question of how lifestyle may interact with genetic susceptibility factors in cancer development. ESSENTIAL PUBLICATIONS: (1.) Hüsing A. et al. (2012), Prediction of breast cancer risk by genetic risk factors, overall and by hormone receptor status. J Med Genet. 49, 601–608. (2.) Ritte R. et al. (2012). Adiposity, hormone replacement therapy use and breast cancer risk by age and hormone receptor status: a large prospective cohort study. Breast Cancer Res., 14, R76. (3.) Grote V.A. et al. (2011). Diabetes mellitus, glycated haemoglobin and C-peptide levels in relation to pan- On the basis of established, genetic and nongenetic risk factors, we build quantitative risk models for the identification of individuals who have an increased risk of developing cancer compared to others, and who may have increased benefit from targeted prevention measures, such as regular cancer screening. A further focus is exploring new routes for prevention and early diagnosis of cancer, as well as quality control of introduced measures. Due to the population-related approach, statistical methods and their further development are of particularly high relevance in epidemiology. A major part of our research takes place within the setting of large-scale prospective cohort studies, such as the European Prospective Investigation into Cancer and Nutrition (EPIC), and the Scandinavian Consortium of Maternity Cohorts. For future studies, our division has a central role in the development and set-up of the “National Cohort” – a new, large-scale prospective cohort study in Germany. Research at DKFZ 2014 creatic cancer risk: a study within the European Prospective Investigation into Cancer and Nutrition (EPIC) cohort. Diabetologia, 54, 3037–3046. (4.) Campa D. et al. (2011). Genetic variability of the mTOR pathway and prostate cancer risk in the European Prospective Investigation on Cancer (EPIC). PLoS One, 6, e16914. Cancer Epidemiology (C020) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2200 Fax: +49 6221 42 2203 [email protected] 81 Cancer Risk Factors and Prevention Molecular Genetic Epidemiology Division Head: Prof. Dr. Kari Hemminki Molecular Genetic Epidemiology (C050) German Cancer Research Center Im Neuenheimer Feld 580 69120 Heidelberg Phone: +49 6221 42 1800 [email protected] Genome-wide association study (Manhattan plot) on Hodgkin lymphone (Enciso-Mora et al. Nature Genet 2010). The strongest association with many SNPs is shown for the MHC complex on chromosome 6. 82 For common cancers, such as breast, prostate, colorectal and lung cancers, familial risk for a person who has an affected family member is typically around 2.0; approximately 5 to 20% of cases are familial when two generations are considered. Known susceptibility genes are estimated to explain some 15 to 30% of the familial clustering of breast, prostate and colorectal cancers but only about 1% of the familial clustering of lung cancer. The recently identified low-penetrance genes/loci explain a large proportion of cancer occurrence (population-attributable fraction) but explain only a small proportion of the known familial risks for these cancers. This apparent paradox is explained by the high allele frequency of the loci and the low conferred risk. However, the true functional gene variants may be much rarer and their contribution to familial risk would be higher. For many relatively common cancers, such as bladder cancer and non-Hodgkin lymphoma, only low-penetrance genes are known, and they have negligible contribution to the familial risk. Thus, there are large gaps in knowledge on the genetic basis of familial cancer that the Molecular Genetic Epidemiology division is addressing on two fronts. It is using the world’s largest family dataset, the Swedish Family-Cancer Database to assess familial cluster in all cancers. It is characterizing gene underlying susceptibility to cancer through genetic association studies, increasingly using genome-wide approaches. relatives. In due course, the aim is to develop software packages that would provide relative and absolute risk estimates for a given family structure, age of onset of the diagnosed cancers, presentation of related tumors and other relevant data. There are several ongoing genome-wide association studies, for example on myeloma, Hodgkin disease, childhood leukemia, for which new low-penetrance genes have been described. There is a future interest to associate the findings with clinical parameters, such as survival and response to therapy. Genome-wide association studies have been conducted on breast cancer and melanoma with a special reference to survival. In collaborative association studies on breast and colorectal cancers genetics of cancer prognosis and gene-environment interactions are under focus. ESSENTIAL PUBLICATIONS: (1.) Prasad R. et al. (2010). Verification of the susceptibility loci on 7p12.2, 10q21.2 and 14q11.2 in childhood precursor B-cell acute lymphoblastic leukemia. Blood, 15, 1765–1767. (2.) Enciso-Mora V. et al. (2010). A genome-wide association study of Hodgkin Lymphoma identifies new susceptibility loci at 2p16.1 (REL), 8q24.21, and 10p14 (GATA3). Nature Genet., 42, 1126–1130. (3.) Hemminki K. et al. (2011). Familial risks in cancer of unknown primary: tracking the primary sites. J Clin Oncol., 29, 435–440. (4.) Hemminki K. et al. (2011). Familial mortality and familial incidence in cancer. J Clin Oncol., 29, 712–718. Future Outlook: The Swedish Family Cancer Database includes increasingly older generations whereby case numbers increase and it is possible to study familial risks in rare and histology-specific cancers. As one example, familial clustering of cancer of unknown primary site is offering interesting insights into metastatic phenotype. The database is being used to analyze age-group-specific familial risks, which will be turned into user-friendly algorithms for clinical genetic counseling of cancer patients and their Research Program Cancer Risk Factors and Prevention Biostatistics Division Head: Prof. Dr. Annette Kopp-Schneider The main tasks of the Biostatistics Division are service and research in the field of biostatistical methods and their application in cancer research. We provide statistical support for all scientific activities of the DKFZ from in vitro and animal studies to human subject research including clinical trial, linking methodical research and biomedical disciplines. Our support covers experimental design, sample size estimation, data analysis and preparation of results for publication. It ranges from brief statistical consultations to long-term collaborations and covers standard statistical analysis approaches as well as the development of complex statistical methods tailored to specific questions. The ongoing evolution of novel measurement techniques and platforms and the development of new research questions make it necessary to continuously refine the biostatistical and biomathematical methodology and to develop and implement new methods for analysis. Our current research areas reflect the requests we are confronted with from collaborators. We develop and assess efficient and valid methods for visualizing, integrating and analyzing data, in particular high-dimensional molecular data. We develop optimized biometrical designs in experimental cancer research and in clinical studies. We devise methods of quantitative risk assessment. Future Outlook: One focus of interest of our research is the evaluation of molecular data in biomarker studies. We will extend our research to find associations with clinico-pathological factors, prognosis or response to therapy with the aim to identify diagnostic, prognostic or predictive factors. We will develop and validate statistical methods for classification and prediction using low- and high-dimensional data. The development of methods for data integration is becoming an important aspect of our work, e.g. the development of Bayesian hierarchical models for classification and prediction, which can make use of multiple data sources, while prop- Research at DKFZ 2014 erly accounting for biological inter-relations between these data. Another area of research is the development and application of statistical and stochastic models for dose-response relationships. In this context, we investigate non-linear regression models. A special focus lies on the description of cellular processes using stochastic models to understand the process of carcinogenesis or the effect of toxic compounds on cell systems. ESSENTIAL PUBLICATIONS: (1.) Hielscher T. et al. (2010). On the prognostic value of survival models with application to gene expression signatures. Statistics in Medicine, 29, 818–829. (2.) Renner M.. et al. (2013). Stochastic time-concentration activity models for in vitro neurotoxicity. Theor. Biol. Med. Model., 10, 19. (3.) Weimer M. et al. (2012). The impact of data transformations on concentration-response modeling. Toxicol.Lett., 213, 292–298. (4.) Wunder C. et al. (2012). An adaptive group se- Biostatistics (C060) quential phase II design to compare treatments for German Cancer Research Center survival endpoints in rare patient entities. J. Biop- Im Neuenheimer Feld 280 harm. Stat., 22, 294–311. 69120 Heidelberg Phone: +49 6221 42 2391 [email protected] The Principle of Statistical Inference 83 Cancer Risk Factors and Prevention Clinical Epidemiology and Aging Research Division Head: Prof. Dr. Hermann Brenner Clinical Epidemiology and Aging Research (C070) German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 1301 [email protected] The Clinical Epidemiology and Aging Research Division’s main areas of research include clinical cancer epidemiology, epidemiology of chronic age-related diseases and epidemiological methods. In the field of clinical cancer epidemiology, the group conducts large-scale epidemiological studies on new avenues of more effective cancer prevention and early detection, and on issues of quality of medical care, prognosis and quality of life of cancer patients. Further large-scale epidemiological studies focus on detection of risk factors, risk markers and prognostic factors of cardiovascular disease, diabetes mellitus and arthritis, thereby aiming to explore new avenues of enhanced prevention and management of these common and strongly age-related diseases. Most of the Division’s studies are conducted in interdisciplinary, often international collaboration with cancer registries, clinical partners and partners from the basic biological sciences. Apart from application of the highest methodological standards in these studies, a major area of research conducted in the Division is devoted to further development and enhancement of methods in epidemiological research. Future Outlook: The Division will expand its research on early detection and screening for colorectal cancer to focus on questions of high relevance to the implementation of early detection programs at the population level. Future research in early detection and screening will also be directed towards other gastrointestinal cancers. Due to demographic aging, along with steadily increasing cancer survival rates, the number and prevalence of cancer survivors in the population will continue to increase. The Division will therefore intensify its research on additional outcomes, such as quality of life and the occupational and social participation of cancer survivors. An area of increasing interest in aging research will be to enhance the empirical evidence for preventive and therapeutic interventions in old age. Epidemiological aging research in the Division will increasingly address integrative and functional endpoints that have received comparatively little attention thus far, such as indicators of multimorbidity and frailty, or indicators of functional limitations, as these are often more relevant for the elderly than single medical diagnoses. The Division will also contribute its expertise in recruitment and follow-up of population-based cohorts and in the areas of clinical epidemiology, aging research and epidemiological methods to the planning and build-up of the National Cohort of 200,000 older adults to be recruited from 201 on and followed over many years thereafter. ESSENTIAL PUBLICATIONS: (1.) Brenner H. et al. (2013). Colorectal cancer. Lancet. doi: 10.1016/S0140-6736(13)61649-9. [Epub ahead of print]. (2.) Brenner H. et al. (2012). Risk of colorectal cancer after detection and removal of adenomas at colonoscopy: population-based case-control study. Journal of Clinical Oncology, 30, 2969–2976. Study assessing the potential to enhance stool tests for early detection of colorectal neoplasms. The bold line indicates improved detection of advanced adenomas by immunochemical fecal occult blood tests among men using low-dose aspirin (Brenner et al, JAMA 2010). (3.) Breitling L.P. et al. (2011). Tobacco smoking-related differential DNA methylation: 27k discovery and replication. American Journal of Human Genetics, 88, 450–457. (4.) Jansen L. et al. (2011). Health-related quality of life over 10 years after diagnosis of colorectal cancer – a population-based study. Journal of Clinical Oncology, 29, 3263–3269. 84 Research Program Cancer Risk Factors and Prevention Molecular Epidemiology Research Group Head: Prof. Dr. Barbara Burwinkel One of the group’s main research interests in the past five years has been the identification of genetic and epigenetic risk factors for breast and colorectal cancer. A special focus has been on familial cancer, because genetic risk factors are supposed to be enriched in this population and the power to detect risk variants is enlarged in comparison to sporadic study populations. After accepting the foundation professorship at the Department of Obstetrics and Gynaecology in 2008, the group’s research interests have shifted to reveal molecular and cellular factors (e.g. miRNA profiles, methylation signatures, genetic variants, mutations and circulating tumor cells (CTCs)) associated with prognosis and therapeutic response, as well as to uncover molecular serum markers, as early detection markers for breast or colorectal cancer and for the recurrence or metastasis of breast and colorectal cancer. This is done in cooperation with Hermann Brenner and Jenny Chang-Claude (DACHS study), Jenny Chang-Claude (MARIE study) and Andreas Schneeweiß (University Womens Clinic and NCT). By developing peptide aptamers against ID proteins, which are overexpressed in several solid cancers including breast and ovarian cancer and have been shown to be associated with poor prognosis, the group is testing biomarkers as therapeutic targets. One peptide aptamer against ID1 and ID3 that the group has isolated has been shown to counteract the oncogenic activities of ID1 and ID3 in vitro. • • • • and Claus Bartram from the Institute of Human Genetics and the German Consortium of Hereditary Breast and Ovarian Cancer (GC-HBOC). The group will also evaluate the possibility of inherited epigenetic markers as cancer risk factors. using methylation signatures, splice variants, mutations and miRNAs as prognostic and predictive markers and early detection markers. identifying genetic germline variants that alter therapeutic response. detecting genetic germline variants affecting the target gene, its metabolizing enzymes, and proteins involved in drug absorption, transport, metabolism and excretion that might be associated with therapeutic response. This project will be done in cooperation with Andreas Schneeweiß and Frederik Marmé (University Womens Clinic and NCT). performing the molecular characterization of circulating cancer (stem) cells. The group has started a collaboration with Andreas Schneeweiß (University Womens Clinic, Heidelberg, and NCT), Andreas Trumpp (Division Stem Cells and Cancer, A010) and has built up a metastatic breast cancer study (MBSUCH). ESSENTIAL PUBLICATIONS: (1.) Ghoussaini M. et al. (2012). Identification of three new loci associated with breast cancer susceptibility. Nat Genet. 44, 312–318. Molecular Epidemiology (C080) German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 1461 [email protected] 12p12.3 deletion identified in two familial CRC cases using Affymetrix SNP 6.0 array (x axis: logR intensity ratio, blue bars; y axis: B allele frequency, red circles). Deletion regions are in black boxes. (2.) Wirtenberger M. et al. (2006). Identification of Future Outlook: The major aims of the group are: • identifying rare intermediate and high breast cancer risk variants that might contribute more to familial cancer risk than previously assumed via capture techniques and next-generation sequencing methods, combined with the well characterized familial breast cancer study population collected by Christian Sutter Research at DKFZ 2014 frequent chromosome copy-number polymorphisms by use of high-resolution single-nucleotide-polymorphism arrays. Am J Hum Genet., 78, 520–522. (3.) Frank B. et al. (2008). Association of a common AKAP9 variant with breast cancer risk: a collaborative analysis. J Natl Cancer Inst, 100, 437–442. (4.) Stein S. et al. (2010). Genomic Instability and Myelodysplasia with Monosomy 7 Consequent to EVI1 Activation after Gene Therapy for Chronic Granulomatous Disease. Nat Med., 16, 198–204. 85 Coordinator Prof. Dr. Hans-Reimer Rodewald Tumor Immunology The immune system is our body’s most powerful weapon to combat pathogens and cancer cells. However, tumor cells have a repertoire of tricks to evade the immune response. The divisions of the Research Program Tumor Immunology investigate the mechanisms regulating the behavior of immune cells. Research work focuses on cell proliferation and programmed cell death (apoptosis) as well as on the activation and regulation of immune cells. Also under investigation are cancers affecting the immune system as such. The aim is to better understand the role of the immune system in cancer, AIDS, and autoimmune diseases. The findings will be translated into new approaches for clinical application to utilize the potential of the immune system for fighting cancer. 86 Research Program Research at DKFZ 2014 87 Tumor Immunology Translational Immunology Division Head: Prof. Dr. Philipp Beckhove Translational Immunology (D015) German Cancer Research Center and NCT Im Neuenheimer Feld 460 69120 Heidelberg Phone: +49 6221 56 5466 [email protected] The immune system is characterized by its capability to recognize and eliminate malignant tumors. Immunotherapies exploit this unique ability and promise to become an efficient complement to standard tumor treatments in the future. The objective of the division “Translational Immunology" is to gain new insights into the immune defence system of cancerous cells and to evolve the results from basic research through to clinical treatments. The pursuit of this is based on close interdisciplinary collaboration with the oncological departments of the university hospital. New therapeutic concepts developed by the division are being “translated” into clinical application under the auspices of the National Center for Tumor Diseases (NCT) Heidelberg. Effective immune responses are based on a variety of active principles. The division is looking for options to draw on the immune system´s functions as a complementary treatment in the battle against cancer within the framework of synergystic projects. The project “T Cell Tumor Immunity” (Prof. Dr. Beckhove) describes formative and regulative mechanisms of T cell tumor responses. The project group “Tumorantigens” (Prof. Dr. Eichmüller) investigates the immunogenicity of tumor-associated antigens and develops strategies for tumor-specific immunization using preclinical model systems. their clinical application (project “Antibody Therapy", Dr. Moldenhauer). The role cell adhesion molecules play as target structures for immunotherapies related to metastasis and their role during tumor metastasis are the central topics of the project “Adhesion and Metastasis" (Prof. Altevogt). Particular glycosylation patterns on tumor cells and tumor vessels are not only decisive preconditions of tumor angiogenesis and tumor progression, but they also represent ideal target antigens for new anti-tumor strategies via mimetics with analogue structure and glycan-specific cytotoxic antibodies (project “Glycoimmunology" , PD Dr. Schwarz-Albiez). ESSENTIAL PUBLICATIONS: (1.) Ge Y. et al. (2012). Metronomic cyclophosphamide treatment in metastasized breast cancer patients: immunological effects and clinical outcome. Cancer Immunol Immunother. 61, 353–362. (2.) Bonertz A. et al. (2009). Antigen-specific Tregs control T cell responses against a limited repertoire of tumor antigens in patients with colorectal carcinoma. J Clin Invest. 11, 3311–3321. (3.) Domschke C. et al. (2009). Intratumoral cytokines and tumor cell biology determine spontaneous breast cancer-specific immune responses and their correlation to prognosis. Cancer Research. 21, 8420– 8428. (4.) Beckhove P. et al. (2004). Specifically activat- Future Outlook: The examination of conditions and activation of tumorlytic T and NK lymphocytes are the focus of the project “Antigen Presentation and T Cell Activation" (PD Dr. Momburg). Both projects are complemented by the construction of virus-like particles (VLP) aimed to stimulate immune responses against cancer (project “VLP" , Dr. Cid). In the past decade, monoclonal antibodies, either on their own or in combination with chemotherapy, have proven to be an effective therapeutic agent in the treatment of different tumor diseases. New therapeutic antibodies are being developed with the help of antibody engineering and tested before 88 Research Program ed CD45R0+ central and effector memory but not CD45RA+ naïve T cells from bone marrow of cancer patients selectively home to and reject xenotransplanted autologous tumors. J. Clin. Invest. 114, 67–76. Tumor Immunology Immunogenetics Division Head: Prof. Dr. Peter Krammer The division of Immunogenetics has made several groundbreaking contributions to the field of programmed cell death (apoptosis). The group established that the CD95 receptor does not only act as a death receptor that induces apoptosis, but also triggers the NF-kB pathway involved in tumor proliferation, invasion and metastasis. Together with APOGENIX, a company founded with DKFZ, the group has developed the biological APG101, a soluble fusion protein consisting of two extracellular domains of the CD95 receptor and an antibody Fc fragment (CD95-Fc). APG101 has therapeutic effects in many diseases, e.g. in cancer. Two TCM anti-cancer compounds, Wogonin and Rocaglamide could be shown to preferentially induce apoptosis in tumor cells. The cyclin-dependent kinase 9 (CDK9) was identified as the direct molecular target of Wogonin, and Prohibitin 1 and 2 were identified as the target of Rocaglamide. These studies point to the potential use of these compounds as an adjuvant for anti-cancer therapy. Annexins were shown to be involved in induction of peripheral tolerance against antigens from apoptotic cells. Members of the annexins protein family are transferred early upon induction of cell death to the surface of apoptotic cells. By inhibition of NF-κB signaling, annexins suppress dendritic cell (DC) maturation. Finally, a redox-regulating molecule, AF-1, was identified that is associated with aging of human cells. Knock down of AF-1 can also substantially extend stress resistance and life span in drosophila. AF-1 seems to be involved in a general aging mechanism. mechanisms of novel NF-κB regulating phosphatases will be characterized. Since the enzymes identified influence cell death of tumor cells, the ultimate goal is to find ways to manipulate them to treat patients. Annexins on the surface of apoptotic tumor cells suppress the anti-tumor immune response. Therefore, manipulation of the annexin system promises benefits for tumor therapy. The group will focus on the identification of the annexin receptor and the molecular mechanism by which annexin treatment inhibits proinflammatory signaling. Future directions of the group´s work in redox regulation will involve the investigation of the role of AF-1 as a putative master switch in aging. Here, the focus of the division will be on AF-1´s molecular mechanism, its drugability, and its role in age-related diseases. ESSENTIAL PUBLICATIONS: (1.) Kamiński M.M. et al. (2012). T cell activation is driven by an ADP-dependent glucokinase linking en- Immunogenetics (D030) hanced glycolysis with mitochondrial reactive oxy- German Cancer Research Center gen species generation. Cell Rep., 2, 1300–1315. (2.) Brechmann M. et al. (2012). A PP4 holoenzyme Im Neuenheimer Feld 280 balances physiological and oncogenic nuclear fac- 69120 Heidelberg tor-kappa B signaling in T lymphocytes. Immunity. 37, Phone: +49 6221 42 3718 697–708. (3.) Kiessling M.K. et al. (2011). High-throughput mu- [email protected] tation profiling of CTCL samples reveals KRAS and NRAS mutations sensitizing tumors toward inhibition of the RAS/RAF/MEK signaling cascade. Blood. 117, 2433–2440. (4.) Schleich K. et al. (2012). Stoichiometry of the CD95 death-inducing signaling complex: experimental and modeling evidence for a death effector domain chain model. Mol Cell. 47, 306–319. Future Outlook: Future work will be directed at trying to block the CD95 death pathway. In addition, CD95 mediated non-death pathways will be addressed by two approaches: resensitization towards apoptosis by drugs, and blocking of CD95 receptor signaling by drugs and/or soluble CD95 receptors. Further trials with the soluble CD95 receptor APG101 are currently planned. The binding of Wogonin and Rocaglamide to their targets will be elucidated at the atomic level. The insight into these molecular interactions will serve as a platform for further drug screening. Furthermore, the molecular Research at DKFZ 2014 CD95 signaling: A death inducing signaling complex (DISC) assembles upon binding of the CD95 ligand (CD95L) to its receptor CD95. The proteins FADD, procaspases-8/10 and c-FLIP have been shown to be key components of this structure (for details see Krammer et al. 2007, Nat Rev Immunol). The signal can either lead to cell death (apoptosis) or to proliferation and invasion. 89 Tumor Immunology Molecular Immunology Division Head: Prof. Dr. Bernd Arnold The Division of Molecular Immunology investigates basic mechanisms that are important for immunological tumor rejection with the aim to exploit this knowledge for the development of novel immunotherapeutic strategies. Our research groups focus on the following topics: Molecular Immunology (D050) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3731 [email protected] Antigen presentation: For successful destruction of tumor cells T lymphocytes need to be activated by dendritic cells presenting tumor antigens. Therefore, we are studying homeostasis and stimulatory capacity of dendritic cells, and measure the precise biophysical interaction forces between antigen-presenting cells and T cells. Peripheral tolerance: T lymphocytes are often rendered tolerant by tumors and, therefore, fail to attack the tumor. By investigating the molecular pathways leading to tolerance induction we identified a novel immune-modulator, Dickkopf-3, that can down-regulate T cell responses and may represent a novel tumor escape mechanism. Tumor microenvironment: The tumor vasculature can restrict the access of T lymphocytes into the tumor, thereby preventing tumor eradication. We succeeded in strongly improving infiltration and tumor rejection by strategies that modulate the tumor microenvironment, including local irradiation, efficient depletion of regulatory T cells, and targeting of vasculature-associated genes. These strategies will be translated into the clinic. Future Outlook: We investigate basic mechanisms that are crucial for immunological tumor rejection. We are focusing on the following aims: Peripheral tolerance: Tissues particularly sensitive to inflammatory damage, like the brain and the eye, create an immune-suppressive microenvironment to limit immune responses. Likewise, developing tumors can generate a tolerogenic milieu, which facilitates tumor progression and antagonizes the efficacy of vaccination strategies. Our understanding of the key cellular and molecular players responsible for the induction and maintenance of tolerance is yet to be completed. Therefore, we will address the molecular basis of immune silencing by healthy organs and tumor cells and will focus on the identification of new molecular targets suitable for therapeutic reprogramming of the immune system. Tumor microenvironment: Normalization of the tumor vasculature is likely to play a major role in T cell infiltration, which is a prerequisite for tumor rejection. Therefore, we will analyze the cellular and molecular mechanisms resulting in modulation of the tumor microenvironment, vessel normalization, and T cell infiltration. In particular, we will focus on regulatory T cells and polarized macrophages that shape the tumor microenvironment (in collaboration with P. Beckhove). Identification of factors enhancing T cell infiltration will have important implications for clinical immunotherapy. ESSENTIAL PUBLICATIONS: (1.) Papatriantafyllou M. et al. (2012). Dickkopf-3, an immune-modulator in peripheral CD8 T cell tolerance. Proc Natl Acad Sci USA, 109, 1631–1636. (2.) Hamzah J. et al. (2008). Vascular normalization in RGS5-deficient tumors promotes immune destruction. Nature, 453, 410–414. (3.) Hochweller K. et al. (2010). Dendritic cells control T cell tonic signalling required for responsiveness to We identified Dickkopf 3 as a novel immune modulator which is mainly expressed in tissues termed immune-privileged, such as brain and eye. It dampens T cell reactivity in such tissues protecting them against immune destruction. Here the expression of Dickkopf 3 is shown in neurons in the mouse brain. 90 Research Program foreign antigen. Proc. Natl. Acad. Sci., 107, 5931–5936. (4.) Klug F. et al. (2013) Low-dose irradiation programs macrophage differentiation to an iNOS+/M1 phenotype that orchestrates effective T cell immunotherapy. Cancer Cell, doi: 10.1016/j.ccr.2013.09.014 (epub ahead of print). Tumor Immunology Developmental Immunology Division Head: Prof. Dr. Bruno Kyewski selection of promiscuously expressed genes in mTECs at the single cell and population level. We expect the different and complementing avenues of inquiry to provide us with a more comprehensive understanding of the functional organization of the thymic- microenvironment in the context of self-tolerance, and new insights into gene (co)-regulation in case of pGE and beyond. In addition, we will continue to directly apply our findings in basic research to human disorders, i.e. further explore the interrelationship between pitfalls of pGE and human autoimmune diseases and identify underlying molecular mechanisms controlling the intra-thymic expression of prominent auto-antigens. In the context of pGE, we also study the developmental biology of thymic epithelial cells, with the future aim to follow their full course of differentiation in vitro and in vivo from the tissue-resident bi-potent stem cell to the terminally differentiated stage. This topic entails the identification and characterization of TEC stem cells and the development of appropriate in vitro culture. Finally, we will exploit our acquired knowledge on the biology of human thymic epithelial cells to develop new diagnostic tools for human thymoma subtypes. Developmental Immunology (D090) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3734 [email protected] A ESSENTIAL PUBLICATIONS: capsule (1.) Derbinski J. et al. (2001). Promiscuous gene expression in medullary thymic epithelial cells mirrors the peripheral self. Nat. Immunol., 2, 1032–1039. cortex Self/non-self discrimination is a hallmark of the immune system of multi-cellular organisms. The thymus of higher vertebrates plays a central role in the induction of T cell tolerance (“central tolerance”). During self-tolerance induction, the highly diverse T cell receptor repertoire is probed against an unknown array of self-antigens mirroring the “immunological self” of the body. These interactions rid the repertoire of auto-reactive T cells. Our discovery of promiscuous gene expression (pGE) and its essential function in preventing organ-specific autoimmunity has led to a reappraisal of the role of central tolerance in self/non-self discrimination. The diversity of self-ligands in the thymus is to a large extent generated by ectopic or promiscuous expression of numerous tissue-restricted antigens in medullary thymic epithelial cells (mTECs). This gene pool encompasses > 25 % of all known genes and represents virtually all tissues of the body. Promiscuous gene expression allows self-antigens, which otherwise are expressed in a spatially or temporally restricted manner, to become continuously accessible to developing T cells thus rendering them tolerant. Specific failure of promiscuous gene expression can lead to severe organ-specific autoimmune diseases like type 1 diabetes mellitus. This gene pool also includes tumor-associated antigens, thus imposing immunological tolerance towards tumors, a fact to be considered in the selection of tumor antigens for clinical vaccination trials. cortical epithelial cell (2.) Kyewski B. and Klein L. (2006). A central role for Research at DKFZ 2014 central tolerance. Annu. Rev. Immunol., 24, 571–606. thymocyte (3.) Lv H. et al. (2011). Impaired thymic tolerance to al- macrophage pha-myosin directs autoimmunity to the heart in mice and humans. J. Clin. Invest., 121, 1561–1573. (4.) Pinto S. et al. (2013). Overlapping gene coexpression patterns in human medullary thymic epithelial cells generate self-antigen diversity. Proc. Natl. Acad. Sci. 110, E3497–E3505. trabecule medulla Future Outlook: PGE represents one of the most fascinating and arcane aspects of T cell tolerance. In future we will further pursue our studies on the cellular and molecular regulation of this phenomenon in experimental in vitro and in vivo models. In particular, we would like to understand how a terminally differentiated epithelial cell type generates such a diverse self-antigen repertoire in a mosaic fashion, such that the expression patterns of individual mTECs faithfully add up to the full complement of selfantigens at the population level. In this context we will search for rules which guide the subcapsular epithelial cell medullary epithelial cell (mTEC) B-cell dendritic cell The thymus is the site where central T cell tolerance is imposed. It consists of an outer cortex and a central medulla. The medulla is densely packed with various antigen-presenting cells, which present a plethora of self-antigens to developing T cells and thus induce self-tolerance. Medullary thymic epithelial cells (shown in red) have the unique property to express numerous tissue-restricted self-antigens in a promiscuous fashion and thus are essential for the prevention of autoimmunity. 91 Tumor Immunology Cellular Immunology Division Head: Prof. Dr. Hans-Reimer Rodewald Cellular Immunology (D110) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4120 [email protected] The Division of Cellular Immunology is investigating physiological and pathological processes of the development of cells and organs in the immune system as well as their immunological functions. We generated reporter knockin mice to demonstrate that T cells and myeloid cells (e.g. dendritic cells and granulocytes) arise in the thymus from distinct progenitors under physiological conditions. Moreover, a genetic block of Notch1 signals in T cell progenitors leads to their developmental deviation to dendritic cells instead of T cells. T cell development and maturation occur in a discrete primary immunological organ, the thymus. Previous projects focussed on thymus organogenesis while in current projects we investigate functions of the transcription factor FoxN1 in thymic epithelial cells (TECs). A central area of our research is the investigation of the roles of mast cells in the immune system. Different knockout mice enabled us to characterize an enzyme of the heparin biosynthesis pathway and to elucidate the mechanism by which mast cell proteases can degrade endothelin, a blood pressure regulating factor, and detoxify structurally related snake toxins. origins of different tissue resident macrophages like osteoclasts, Kupffer cells in the liver, and microglia in the central nervous system. We are extending our thymus research towards unravelling mechanisms of acute T cell leukaemia (T-ALL) development. We discovered that thymocytes undergo transformation if they non-physiologically persist in the thymus. This occurs with surprisingly high incidence if the influx of fresh progenitors into the thymus is interrupted. We hope that this new T-ALL model shall enable us to investigate the cellular and molecular mechanisms of T-ALL formation in the thymus. Comprehensive investigations of mast cell functions remain a central area of our research. We have generated a mouse mutant, which is completely mast cell deficient but has an otherwise normal immune system. This new mouse represents an excellent model to clarify the question in which infections or diseases beyond allergy mast cells play immunological roles. Specifically, we will test the roles of mast cells in wound healing, asthma, responses to infections and in tumour models. ESSENTIAL PUBLICATIONS: (1.) Schlenner S.M. et al. (2010). Fate mapping reveals separate origins of T cells and myeloid lineages in the Future Outlook: Members of our team study the dynamic processes of stem cell differentiation and the plasticity of the development of mature immune cells. To this end, we develop mouse models in which stem cells and their progeny are inducibly labelled at a certain time point. Furthermore, we have generated ‘universal stem cell recipient’ mice which can be transplanted with bone marrow stem cells without the need for myeloablation, e.g. by irradiation. In another fate mapping project we are investigating the Immunfluorescence staining of lymphocytes (red) and osteoclasts (green) in bone marrow of a mouse femur. 92 Research Program thymus. Immunity, 32, 426–436. (2.) Martins VC et al. (2012). Thymus-autonomous T cell development in the absence of progenitor import. J Exp Med, 209, 1409–1417. (3.) Feyerabend T.B. et al. (2011). Cre-Mediated Cell Ablation Contests Mast Cell Contribution in Models of Antibody- and T Cell-Mediated Autoimmunity. Immunity, 35, 832–844. (4.) Rodewald H.R. et al. (2012). Widespread immunological functions of mast cells: fact or fiction? Immunity, 37, 13–24. Tumor Immunology Innate Immunity Boveri Junior Research Group Head: PD Dr. Adelheid Cerwenka The innate immune response serves as the first line of immune defence and does not only directly lead to tumor cell destruction, but also to efficient subsequent activation of the adaptive immune system. The Boveri Junior Group “Innate Immunity" investigates Natural Killer (NK) cells and myeloid cell subsets in cancer with the goal to improve therapeutic anti-tumor strategies. NK cells potently kill tumor cells and produce inflammatory cytokines. Their activation is determined by a delicate balance between signals delivered by inhibitory receptors, most of which are specific for self-MHC class I, and activating receptors. Many tumors lose expression of MHC class I molecules and frequently escape from direct recognition by CD8+ T cells, but become highly susceptible to NK cell-mediated killing. Thus, we believe that it is of major importance to explore NK cell-based therapies against cancer. Our research focuses on three strategies to amplify innate immune cell-mediated antitumor responses. 1.) It is our goal to guide high numbers of highly active, persistent NK cells to the tumor site. 2.) We attempt to increase the visibility of tumor cells to NK cells by the upregulation of ligands for activating NK cell receptors on tumors. 3.) We aim at exploring inflammatory pathways in myeloid cells and their functional importance in the context of cancer. Future Outlook: Our future projects will further continue to develop strategies aiming at harnessing NK cells against tumors. In addition, candidates in inflammatory signalling pathways in myeloid cells and their functional importance in the context of cancer inflammation will be investigated. Our overall program is designed to gain novel insight in mouse and human NK cell and myeloid cell biology building the basis for innovative strategies of immunotherapy against cancer. ESSENTIAL PUBLICATIONS: (1.) Cerwenka A., Lanier LL. (2001). NK cells, viruses and cancer. Nature Immunol. Rev., 1, 41–49. (2.) Schlecker E. et al. (2012). Tumor-infiltrating monocytic myeloid-derived suppressor cells mediate CCR5dependent recruitment of regulatory T cells favouring tumor growth. J.Immunol., 189, 5602–5611. (3.) Ni J. et al. (2012). Sustained effector function of IL12/15/18 preactivated NK cells against established tu- Innate Immunity (D080) German Cancer Research Center mors. J Exp Med, 209, 2351–2365. Im Neuenheimer Feld 280 (4.) Fiegler N. et al. (2013). Downregulation of the ac- 69120 Heidelberg tivating NKp30 ligand B7-H6 by HDAC inhibitors impairs tumor cell recognition by NK cells. Blood, (epub ahead of print). Phone: +49 6221 42 4480 [email protected] CD56-positive NK cells (brown) infiltrating cervical carcinoma. Research at DKFZ 2014 93 Tumor Immunology Immune Tolerance Helmholtz University Junior Research Group Head: Dr. Markus Feuerer Immune Tolerance (D100) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 1530 [email protected] The immune system has evolved over time to defeat external threats such as bacteria and viruses as well as internal threats like cancer. The ability of the immune system to destroy such a diverse number of foreign invaders is a tribute to its flexibility. However, this comes at a price and the complexity can lead to severe autoimmune diseases. In addition, misguided or deregulated immune responses have recently been implicated in non-classical immune disorders such as obesity. To minimize such collateral damage, powerful mechanisms of immune tolerance have evolved to keep unwanted immune responses at bay. These mechanisms must be tightly controlled as overactive immune tolerance can specifically counteract desirable immune reactions (e.g. anti-tumor or anti-microbial). Peripheral immune regulation is maintained by specialized cells, including T cells and myeloid-derived cells. The ability to actively suppress an immune response makes regulatory T (Treg) cells important elements to consider. Treg cells are a specialized lineage of CD4+ T cells, characterized by expression of the transcriptional regulator Foxp3. Treg cells are essential for the maintenance of self-tolerance. Our goal is to explore Treg cell biology in the context of autoimmunity and anti-tumor-immunity. What are the molecules behind these specialized cells? In addition, we are interested in how the local microenvironment shapes the function of Treg cells. ways that control the development and function of Foxp3+ Treg cells. Peripheral immune regulation is not only maintained by adoptive immune cells but also by innate cells such as myeloid cells. As a second main project, we are focusing on understanding the role that myeloid cells play in immune regulation. Myeloid cells are a heterogeneous group of cells involved at the interface of inflammation and wound-healing. Some members promote inflammation whereas others have suppressive or regulatory functions. We are especially interested in investigating how monocytes and their progenies (– for example, tumor-associated macrophages) can contribute to inflammation or productive immunity on one hand and tolerance or tissue repair on the other. What is their relationship to inflammation that promotes cancer formation or progression? ESSENTIAL PUBLICATIONS: (1.) Hettinger J. et al. (2013). Origin of monocytes and macrophages from a committed progenitor. Nature Immunology, 14, 821-830. (2.) Feuerer M. et al. (2009). How punctual ablation of Foxp3+ T cells unleashes an autoimmune lesion within the pancreas islets. Immunity, 31, 654–664. (3.) Feuerer M. et al. (2009). Lean, but not obese, fat is enriched for a unique population of regulatory T cells that affect metabolic parameters. Nature Medicine,15, 930–939. (4.) Feuerer M. et al. (2001). Therapy of human tumors in NOD/SCID mice with patient-derived reac- Future Outlook: Harnessing the potential of Treg cells is one of the most promising new immune system based approaches to control immune function and treat autoimmune diseases and cancer. However, future strategies to bring Treg-based therapies into clinical application will rely on a better understanding of the molecular path- Immune cells infiltrate and destroy pancreatic insulin producing islet cells. 94 Research Program tivated memory T cells from bone marrow. Nature Medicine, 7, 452–458. Structural and Functiona Genomics Applied Tumor-Immunity Clinical Cooperation Unit Head: Prof. Dr. Dirk Jäger In 2013, Dirk Jäger became head of the Clinical Collaboration Unit “Applied Tumor Immunity” at DKFZ. His research team focuses on the development of advanced analytical methods to characterize tumor host interactions in the immunological tumor microenvironment and the periphery. In particular whole-slide imaging of histological sections coupled with automatic image processing, laser microdissection and multiplex protein quantification technologies as well as multiplex serological assays have been established. The goal is a comprehensive mechanistic analysis of immunological pathomechanisms in the tumor microenvironment and to develop individualized immunological therapy approaches that are then translated into clinical care of individual patients. These insights have led to a successful phase I clinical trial (NCT00001) that can be seen as the blueprint for individualized immunological approaches. As the department of medical oncology is the main unit for cancer patient care at the NCT, the direct link between research in the Clinical Cooperation Unit and translation into clinical trials and care is highly efficient. will improve our understanding of cancer at different levels. In a recently funded project by the Heidelberg Center for Personalized Oncology (HIPO), we aim at revealing the mutational landscape of colorectal cancer liver metastases and the immunological specificities of infiltrating immune cells. Bioinformatical epitope predictions complement this analysis and will identify novel immunotherapeutic targets, which can then be evaluated in vitro and prospectively in early clinical trials. ESSENTIAL PUBLICATIONS: (1.) Klug F. et al. (2013). Low-Dose Irradiation Programs Macrophage Differentiation to an iNOS(+)/M1 Phenotype that Orchestrates Effective T Cell Immunotherapy. Cancer Cell. 24, 589–602. (2.) Halama N. et al. (2011). Localization and density of immune cells in the invasive margin of human colorectal cancer liver metastases are prognostic for response to chemotherapy. Cancer Res. 71, 5670–5677. (3.) Halama N. et al. (2011). Natural Killer Cells are German Cancer Research Center Scarce in Colorectal Carcinoma Tissue Despite High Im Neuenheimer Feld 460 Levels of Chemokines and Cytokines. Clin Cancer Res, 69120 Heidelberg 17, 678–689. (4.) Gnjatic S. et al. (2010). Seromic profiling of ovari- Future Outlook: The future goal of this Clinical Cooperation Unit is to develop and apply powerful tools to better stratify patients, analyze the microenvironment, and offer tailored treatments for individual patients. The further development of advanced technologies will allow an unparalleled insight into the makeup of the immunological pathomechanisms in serum samples, archival and fresh cancer specimens, as well as in new non-rodent explant models from patients. Extending immunological data sets by analyzing the mutational repertoire of tumors Applied Tumor-Immunity (D120) Phone: +49 6221 56 7228 an and pancreatic cancer. Proc Natl Acad Sci U S A, 107, [email protected] 5088–5093. and Director of the Medical Oncology, NCT CD3 positive T cells (brown) at the invasive margin of a Colorectal Cancer Liver Metastasis. Research at DKFZ 2014 95 Coordinator Prof. Dr. Heinz-Peter Schlemmer Imaging and Radiooncology It is the task of the Research Program “Imaging and Radiooncology" to introduce new findings, methods, and technologies into the diagnosis and treatment of cancer. Our goal is to detect early and comprehensively understand the specific tumor biology and to tailor radiooncologic treatment to the individual patient for improving cure rates and quality of life. Knowledge gained from basic research in the fields of imaging, radiation physics, engineering, radiopharmacy, as well as radiation- and tumor biology are translated in systematic preclinical and clinical studies and finally applied in clinical studies for improving diagnostic and therapeutic strategies. The multidisciplinary Research Program is centred around the development and implementation of imaging and radiotherapy technology, which is achieved through intensive collaboration between the fundamental research divisions of the Research Program and the Clinical Cooperation Units. Based on the complexity of the matter, different medical specialists are collaborating with scientists of various disciplines, including physicists, mathematicians, computer scientists, engineers, chemists and biologists. 96 Research Program Research at DKFZ 2014 97 Imaging and Radiooncology Radiology Division Head: Prof. Dr. Heinz-Peter Schlemmer Radiology (E010) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2563 [email protected] The Division of Radiology is developing imaging methods for early detection of cancer and characterizing their functional and biologic features, e.g. blood supply, metabolism and molecular mechanisms. In close cooperation with the other divisions of the research program Ultrasonography (US), Computed tomography (CT), Magnetic Resonance Imaging (MRI) and Positron Emission Tomography Hybrid Imaging Devices (PET/CT and PET/MR) are advanced and evaluated in patient studies. For this purpose, up-to-date technologies are available including ultra-high field MRI, dualenergy CT and PET/CT. Methodic developments are conducted in cooperation with partners from medical-technical and pharmaceutic industries. Clinical studies are performed in close cooperation with clinics and institutes of the Heidelberg University hospital and the National Center for Tumor Diseases (NCT) Heidelberg. The Devision is furthermore a partner of the German Consortium for Translational Oncology and the German Center for Lung Research. Scientific fields of application include e.g. early detection and characterization of prostate cancer, lung cancer and multiple myeloma. A novel biopsy system combining preinterventional MRI with peri-interventional ultrasound for perineal prostate biopsies is applied in co-operation with the Department of Urology at Heidelberg University Hospital, enabling precise diagnosis of prostate cancer. In addition, tools for quantifying individual therapy response are developed and applied in patients with e.g. rectal carcinoma or malignant melanoma. Further activities include the computer-aided image handling for implementation of the complex image information in patient care, e.g. for improving radiotherapy. A clinical phase 1 study with MR-guided intra- urethral thermotherapy using high-intensity focused ultrasound (HIFU) is currently going on. A simultaneous PET/MR system has been installed last year and successfully. It is used to improve tumour characterisation, individualised therapy planning and therapy monitoring, while concurrently reducing radiation burden for the patient. Future Outlook: Our Goal is the progress of individualized diagnostics and therapy and image-guided therapy. Ultra-high field MRI is currently applied for advanced imaging of brain tumors. Novel contrast media (CEST agents) will be developed. Diffusion-weighted MRI for staging and therapy control is applied in patients with multiple myeloma. A cohort study supported by the Jose-Carreras-foundation for evaluating prognostic significance of perfusion data from dynamic MRI is currently in progress. In patients with bronchogenic carcinoma, novel approaches are developed for metabolic MRI, 4D-CT imaging and PET with new radiotracers. The CT-based “lung cancer screening and intervention trial” (LUSI study) for early detection of bronchogenic carcinoma has been running over 5 years. Novel tools are developed to quantify therapy response, e.g. dual-energy CT for assessing changes in tissue composition. ESSENTIAL PUBLICATIONS: (1.) Re T.J. et al. (2011). Enhancing pancreatic adenocarcinoma delineation in diffusion derived intravoxel incoherent motion f-maps through automatic vessel and duct segmentation. Magn. Reson. Med., 66, 1327–1332. (2.) Bauman G. et al. (2011). Pulmonary Functional Imaging: Qualitative Comparison of Fourier Decomposition MR Imaging with SPECT/CT in Porcine Lung. Radiology, 260, 551–519. (3.) Hillengass J. et al. (2011). Diffusion-weighted imaging for non-invasive and quantitative monitoring of bone marrow infiltration in patients with monoclonal plasma cell disease: a comparative study with Patient with a cerebral glioblastoma of the left hemisphere. Axial high-resolution T2-weighted MR at 7.0 Tesla demonstrating tumor localization and heterogeneity. 98 Research Program histology. Br. J. Haematol, 153, 721–728. (4.) Hadaschik B.A. et al. (2012). A novel Stereotactic Prostate Biopsy System Integrating Preinterventional MRI and Live US fusion. J. Urology, 26, 807–813. Imaging and Radiooncology Medical Physics in Radiology Division Head: Prof. Dr. Mark E. Ladd The Division of Medical Physics in Radiology plays a pivotal role in all imaging-based diagnostic and therapeutic procedures, developing new and optimizing existing methods. To improve and individualize cancer patient treatment, the acquisition of quantitative biomedical information about the metabolic, physiologic, and functional parameters of tumors and metastases is essential. We are, for example, expanding the diagnostic value of magnetic resonance imaging (MRI) by using a very powerful magnetic field (7 Tesla) to enable the depiction of the distribution of sodium (Na-23), oxygen (O-17), and even potassium (K-39) in vivo. Through the extension of MRI diffusion measurement techniques, we are able to gain additional information about cellular membranes and incoherent capillary flow in tumor tissue. Computed tomography (CT) techniques that allow dramatic reductions in radiation dose to enable CT fluoroscopy or that reduce motion-induced artifacts are also the focus of our work. Furthermore, we are developing noninvasive diagnostic methods for the in vivo detection and functional characterization of metastases on the micro-morphological level. New targeted contrast agent designs are being pursued that allow the attachment of different imaging tags in a modular manner. These concepts permit the use of multiple biophysical techniques (MRI, CT, Positron Emission Tomography (PET), optical imaging) to monitor molecular processes in a relevant pharmacological context. Future Outlook: The Division will continue its role as a center of excellence in oncologic imaging methodology and expand and strengthen its support of the clinical divisions. Novel acquisition and reconstruction strategies are in development for multiple tomographic modalities that are targeted toward improving diagnostics and therapy monitoring, and molecular imaging methodologies are being pursued with a focus on metastatic processes, including the further Research at DKFZ 2014 development of multimodal small-animal tomographic systems. Major objectives for the future involve research projects with the 7 Tesla system and the newly established hybrid MRI-PET system. For example, we have a major effort underway to overcome the technical challenges of imaging the human torso at 7 Tesla. Success would allow us to translate techniques from the brain and take advantage of the enhanced sensitivity of the high magnetic field in organs like the liver, kidneys, and prostate. As part of a concerted initiative across DKFZ divisions, we will be applying a multitude of imaging techniques to improve the characterization of prostate cancer and thus avoid unnecessary therapy. ESSENTIAL PUBLICATIONS: (1.) Kuder T.A. et al. (2013). Diffusion pore imaging by hyperpolarized xenon-129 nuclear magnetic resonance. Physical Review Letters, 111, 028101. (2.) Umathum R. et al. (2013). In vivo 39K MR imaging Medical Physics in Radiology (E020) of human muscle and brain. Radiology, 269, 569–576. German Cancer Research Center (3.) Flach B. et al. (2013). Low dose tomographic fluor- Im Neuenheimer Feld 280 oscopy: 4D intervention guidance with running prior. 69120 Heidelberg Medical Physics, 40, 101909. (4.) Mühlhausen U. et al. (2011). A novel PET tracer for the imaging of αvβ3 and αvβ5 integrins in experi- Phone: +49 6221 42 2550 [email protected] mental breast cancer bone metastases. Contrast Media & Molecular Imaging, 6, 413–420. Conventional gadolinium contrast-enhanced MRI (left) together with a pH-weighted amide CEST image (right) of a brain tumor patient (glioblastoma) obtained with the 7 Tesla MRI system. Chemical Exchange Saturation Transfer (CEST) imaging allows the detection of amide protons in protein backbones by indirect modulation of the water signal. The endogenous amide CEST contrast delineates the tumor region very similarly to the conventional image without the need of an intravenously applied contrast agent (Zaiss M. & Bachert P. (2013). Chemical exchange saturation transfer (CEST) and MR Z-spectroscopy in vivo: a review of theoretical approaches and methods. Physics in Medicine and Biology, 58, R221–R269). 99 Imaging and Radiooncology Radiopharmaceutical Chemistry Division Head: Prof. Dr. Klaus Kopka Radiopharmaceutical Chemistry (E030) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2432 [email protected] The Division Radiopharmaceutical Chemistry designs targeted radiotracers for the molecular imaging and diagnosis of cancer by means of positron emission tomography (PET) and by the en-vogue hybrid technologies PET/CT and PET/MRT, which are used for the highly sensitive non-invasive imaging of biological processes at the molecular level. The focus is the visualisation of rather early disease states or early inspection of treatment response after chemotherapy, radiation therapy or targeted internal radiation therapy (radioendotherapy) in vivo. One main task is thus the development of novel PET radiopharmaceuticals targeting receptors, transport systems and enzymes relevant in early tumorigenesis and tumor progression, to establish a tool for improving the clinical management of patients suffering from tumors, thereby advancing the identification or even the prevention of tumor dissemination. Radiopharmaceutical Chemistry reverts to interdisciplinary fields, such as nuclear chemistry using cyclotrons (see figure) and radionuclide generators. Sub-fields such as labelling chemistry, medicinal chemistry, organic and solidphase chemistry are further required. To fulfil the translation of new PET tracers into the clinical scenario, special laboratory environments are needed to set up Good Manufacturing Practice (GMP)-compliant automated radiosyntheses in highly sophisticated clean rooms which comply with radiation protection and also with the pharmaceuticals act. as 18F, 68Ga and others, targeting enzymes such as matrix metalloproteinases (MMPs) and the prostate-specific membrane antigen (PSMA), as well as membrane-associated receptors and biological targets playing key roles in neoangiogenesis. The tailor-made diagnostic tracers should be designed in such a way that they can also be used as therapeutic pharmaceuticals which bear corresponding particle emitters such as 90Y, 177Lu and others (i.e. “in vivo theranostic approach”, already established for [68Ga]Ga- and [177Lu]Lu-DOTATOC). We speculate that the non-invasive in vivo visualisation of these biological targets by those targetaffine radiotracers will elucidate still unsolved clinical oncological questions - benefiting the patient in any case. With respect to the aforementioned aspects, the Division Radiopharmaceutical Chemistry fits elegantly into the context of the research program Imaging and Radiooncology (FSE). The motivation is to directly link basic research expertise to the GMP-compliant production of corresponding PET tracers for clinical research, as is the case with [18F]FDG, [18F]FLT, [18F] FET, Na[18F]F, [68Ga]Ga-DOTATOC and [68Ga]GaPSMA, to support cancer research at dkfz. In this regard close cooperation with the clinical cooperation unit Nuclear Medicine is indispensable. ESSENTIAL PUBLICATIONS: (1.) Eder M. et al. (2013). Pharmacokinetic Properties of Peptidic Radiopharmaceuticals: Reduced Uptake Future Outlook: Notably, the Division Radiopharmaceutical Chemistry will focus on the development of peptidyl and non-peptidyl tracers, i.e. radiolabelled with PET-compatible radionuclides, such of (EH)3-Conjugates in Important Organs. J Nucl Med, 54, 1327–1330. (2.) Hugenberg V. et al. (2013).Inverse 1,2,3-triazole1-yl-ethyl substituted hydroxamates as highly potent matrix metalloproteinase inhibitors: (Radio)synthesis, in vitro and first in vivo evaluation. J Med Chem, 56, 6858–6870. Negative ion 32 MeV cyclotron MC32NI at dkfz for the production of radionuclides (length x width x height = 4.0 m x 3.5 m x 2.2 m; weight = 60 t). (3.) Waldmann C. et al. (2013). A Closer Look at the Bromine Lithium Exchange with tert Butyllithium in an Aryl Sulfonamide Synthesis. Org Lett, 15, 2954-2957. (4.) Schrigten D. et al. (2012). A New Generation of Radiofluorinated Pyrimidine-2,4,6-triones as MMP-targeted Radiotracers for Positron Emission Tomography. J Med Chem, 55, 223–232. 100 Research Program Imaging and Radiooncology Medical Physics in Radiation Oncology Division Head: Prof. Dr. Oliver Jäkel Because failure of local tumor control is still a problem in many cancer patients, there is an urgent need to optimize existing and to develop new and more effective radiotherapy techniques for localized tumors. Research at our devision is focusing on new conformal radiotherapy techniques with photons, electrons, protons and heavy ions. In the framework of ongoing projects in photon and ion therapy, the division future work will concentrate on the consideration of dynamic changes of target volumes and organs at risk under therapy, due to therapeutic response, organ movement or patient repositioning. Image-guided and time-adapted therapy is being developed to combine conformal dose delivery with online imaging of 3D anatomy and online monitoring of 3D dose distributions. The devision is furthermore integrating molecular imaging into treatment planning and dose delivery with the goals of boosting radio-resistant tumor subvolumes and avoiding radiosensitive normal tissue structures. Establishing mathematical and biological models of tumor and normal tissue response is a further tool to optimize treatment schemes and techniques. One of the strengths of the division is the direct transfer of prototypes of software and hardware development into clinical applications in close collaboration with the Clinical Cooperation Unit Radiation Oncology. Thus the devision is also active in testing and evaluating new techniques, as well as in establishing adequate quality assurance programs. eration of treatment machines. To support the general aim of a biologically guided radiotherapy at DKFZ, we will pursue the development of a unified treatment planning and optimization platform that specifically accounts for the information provided by biological input data. In heavy ion therapy, new dosimetric methods will be developed. A project for Monte Carlo simulation of the effects of secondary electrons in the dosimetry of heavy ions and the investigation of perturbation factors for ionization chamber dosimetry has been started. The possibility to use radiographic imaging or even MRI with ion beams will be investigated for ion beam treatment. A further essential development is a method to visualize ion tracks in cell layers on nuclear track detectors, as a tool to investigate radiobiological properties of clinical ion beams. ESSENTIAL PUBLICATIONS: (1.) Moser T. et al. (2013). Clinical Evaluation of a Laser Medical Physics in Radiation Oncology (E040) Surface Scanning System in 120 Patients for Improv- German Cancer Research Center ing Daily Setup Accuracy in Fractionated Radiotherapy. International Journal of Radiation Oncology Biolo- Im Neuenheimer Feld 280 gy Physics, 85, 846–853. 69120 Heidelberg (2.) Espinoza I. et al. (2013). A model to simulate the Phone: +49 6221 42 2540 oxygen distribution in hypoxic tumors for different vascular architectures. Med Phys. 40, 081703. doi: [email protected] 10.1118/1.4812431. (3.) Niklas M. et al. (2013). Ion track reconstruction using alumina-based fluorescent nuclear track detectors. Physics in Medicine and Biology, 58, N251–N266. (4.) Bangert,M. et al.: Analytical probabilistic modeling for radiation therapy treatment planning. Physics Future Outlook: The future research and development projects comprise the fields of image-guided radiotherapy (IGRT), biological adaptive radiotherapy, ion therapy and the physical parts of different radiation biology projects. Research related to IGRT with photons will be followed by a phase where the results are transferred to the clinical application at DKFZ. We want to accompany the development of real-time 3D-imaging of the patient in treatment position. Promising new approaches involve combinations of MRimaging or 3D x-ray imaging with a new gen- Research at DKFZ 2014 in Medicine and Biology, 58 (16), 5401-5419, 2013. A method of co-localization of ion beam irradiation and cellular response on a fluorescence nuclear track detector (FNTD) has been developed in the department (Niklas et al. PMB 2013). Microscopic images from the FNTD enable the investigation of particle tracks from ion beams (shown in red) and their biological effects in the cell nuclei (DSB= double strand breaks of the DNA, green). 101 Imaging and Radiooncology Radiation Oncology Clinical Cooperation Unit Head: Prof. Dr. Dr. Jürgen Debus Radiation Oncology (E050) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2515 [email protected] Intensity-modulated radiotherapy of a pelvic tumor. Individualized beams from 9 directions enable personalized treatment with sparing of sensitive structures such as small bowel, bladder and genitals (Raystation planning software, Raysearch Laboratories, Stockholm, Sweden). The Clinical Cooperation Unit Radiation Oncology treats cancer patients with new innovative technologies in challenging situations. It explores new approaches and pushes the boundaries of modern radiation oncology. This involves the combination of different radiotherapy techniques such as intensity modulated radiotherapy (IMRT), intraoperative radiotherapy and brachytherapy. New software solutions for optimzed combination of photon and particle treatment in cooperation with the Heidelberg Ion Therapy facility (HIT) are being established. One research focus is the treatment of moving tumors in the lung and upper abdomen. Breathing motion adjusted therapy is applied in so called gated therapy; Radiation is only delivered in the optimal breathing phase and thus safety margins can be minimized and dose exposure to surrounding tissues lowered. Different markers invasively placed around the tumor are evaluated to improve imaging of tumor motion and allow for gated or tracked therapy. This includes gold markers for x-ray based fluoroscopy imaging and electromagnetic markers for online tumor motion tracking. Another option in high precision radiotherapy is rotational intensity-modulated therapy (IMRT). Its possibilities alone or in combination with static gantry IMRT (hybrid arc) are being explored. Another research focus is the evaluation of functional imaging in the planning of radiotherapy. This includes metabolic and hypoxic tracers and their potential to individualize radiation treatment of non-small cell lung cancer. initial step two separate machines – a linear accelerator and an independant 1.5 T MR – are planned to be linked with a patient shuttle to allow MRI based position control and correction. The aim is to minimize additional dosage (especially in younger patients and children) and to improve soft tissue contrast for tumor position detection. The next step in this evolution of modern IGRT is going to be a linear accelerator-MRI combination in one machine for accelerated workflow and online tumor imaging. A clinical focus will be on the possibilities of radiosurgery of spinal tumors. While this is traditionally the domain of conventional radiotherapy, new options for radiosurgical approaches will be tested in a prospective, randomized manner. New radiotherapy options using a robotic arm approach for indiviualized and personalized targeted radiation oncology are also on the agenda. The expansion of radiosurgical and fractionated therapy options is the goal. In medical oncology a remarkable flood of new substances targeting specific tumor pathways has been seen. The combination of these drugs with radiation therapy and the implications for normal tissue toxicity is a major challenge in the future and shall be addressed in an experimental and clinical setting to ensure the safety of these multimodal cancer therapy approaches. ESSENTIAL PUBLICATIONS: (1.) Roeder F et al. (2012). Aggressive local treatment containing intraoperative radiation therapy (IORT) for patients with isolated local recurrences of pancreatic cancer:a retrospective analysis. BMC Cancer, 12, 295. Future Outlook: In cooperation with the department of diagnostic radiology, the use of an MRI/PET for target definition and treatment planning in radiation oncology will be explored. This includes new radiotracers and special MRI sequences for whole body imaging and the detection of lymph node metastases. In addition, the integration of MR imaging into image guided radiotherapy (IGRT) shall be established. In an 102 Research Program (2.) Roeder F. et al. (2011). Intensity modulated or fractionated stereotactic reirradiation in patients with recurrent nasopharyngeal cancer. Radiat Oncol, 6, 22. (3.) Zwicker F. et al. (2011). Reirradiation with intensitymodulated radiotherapy in recurrent head and neck cancer. Head Neck, 33, 1695–1702. (4.) Sterzing F. et al. (2009). Intensity modulated radiotherapy (IMRT) in the treatment of children and adolescents--a single institution’s experience and a review of the iterature. Radiat Oncol, 4, 37. Imaging and Radiooncology Molecular Radiooncology Clinical Cooperation Unit Head: Prof Dr. Dr. Peter Huber The goal of current molecular research in Radiation Oncology is to work towards a personalized medicine program, applying highthroughput methodologies in preclinical and translational research trials. Genetic key players in radioresistance and the determinants of recurrences after radiotherapy are being investigated to broaden the therapeutic window and improve clinical outcome in radiotherapy cancer patients. To this end, we are conducting investigations in preclinical and clinical research in the following areas: • Can radiation favorably be combined with specific signaling inhibitors to enhance therapeutic anti-tumor efficacy +/- CTX of VEGF, PDGF, EGF, Integrins, TGF-beta etc.? • Can combinations of signaling inhibitors (PDGF, TGF-beta, CTGF) attenuate radiotherapy-associated side effects such as lung fibrosis? • Prospective trials investigating the immune stimulatory effects of low dose irradiation in tumor patients (pancreatic cancer, liver metastases from CRC, lung cancer) • Translational clinical studies investigating if radiotherapy (IMRT) can be successfully combined with EGFR or other signaling inhibitors in NSCLC and pancreatic cancer • The molecular basis of the efficacy of carbon ion/particle radiotherapy • The network governing the angiogenic switch or other balanced systems in irradiated cancer • The feasibility of MRI-guided focused ultrasound induced tumor therapy • New clinical concepts of intensity-modulated radiotherapy treatment using biophysical/molecular/functional imaging strategies. gies, such as genomics, functional genomics, epigenetics, proteomics, siRNA screening, bioinformatics, systems biology approaches and molecular and macroscopic radiological imaging. These categories will be linked to classical cancer research expertise in areas such as apoptosis, immunology, stem cell biology, angiogenesis, fibrogenesis, and carcinogenesis or signal transduction. A major goal of Molecular Radiation Oncology is the clinical and biomedical analysis of radiation tumor/normal tissue biology. Key genetic players of radiation effects can be identified by global expression profiling (genomics/proteomics) and sequencing studies in tumor/blood samples in preclinical cell and animal studies, but also in cancer patients undergoing clinical trials. The promising “targets” can be further functionally evaluated for their ability to modulate radiotherapy response by knock outs or pharmacological intervention. The resulting data can then be used to rationally design “targeted drug cocktails” for preclinical cell and animal research and finally, for the translation to cancer patients. To optimize and personalize cancer therapies in the future, we will perform bench-to-bedside research including initiation and conduction of clinical studies. ESSENTIAL PUBLICATIONS: (1.) Klug F et al. (2013). Low-Dose Irradiation Programs Macrophage Differentiation to an iNOS+/M1 Phenotype that Orchestrates Effective T Cell Immunotherapy. Cancer Cell, 24, 589–602. (2.) Flechsig P. et al. (2012). LY2109761 attenuates radi- Molecular Radiooncology (E055) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 06221 42 2515 [email protected] Magnetic resonance imaging of a mouse brain with a glioblastoma tumor. Blockade of TGF-beta signaling by the TGFβR-I kinase Inhibitor LY2109761 (LY) enhances radiation response (RT) and prolongs survival in glioblastoma in an orthotopic mouse model. ation-induced pulmonary murine fibrosis via reversal of TGF-beta and BMP associated proinflammatory and proangiogenic signals. Clin Cancer Res, 18, 3616–3627. (3.) Zhang M. (2011). Blockade of TGF-beta signaling by the TGFβR-I kinase Inhibitor LY2109761 enhances Future Outlook: An important goal for Radiation Oncology in the future is the systematic analysis of molecular radiation effects. Aims are the integration of radiation research topics with high throughput biology and radiology platform technolo- Research at DKFZ 2014 radiation response and prolongs survival in glioblastoma. Cancer Research, 71, 7155–7167. (4.) Timke C. (2011). Randomized controlled phase I/II study to investigate immune stimulatory effects by low dose radiotherapy in primarily operable pancreatic cancer. BMC Cancer, 11, 134. 103 Imaging and Radiooncology Nuclear Medicine Clinical Cooperation Unit Head: Prof. Dr. Uwe Haberkorn The Clinical Cooperation Unit (CCU) Nuclear Medicine is involved in multiple projects on topics such as the planning and follow up of chemo- or radiation therapy, pharmacokinetic modelling of dynamic PET data, identification of new peptides with high affinity for tumor disease; the establishment of new endoradiotherapy approaches based on peptides and antibodies; the development of alternate panning strategies with phage and ribosome display using recombinant proteins, membrane fractions and cells; the design of combination therapy with endoradiotherapy and chemo-, immuno- or radiation therapy; and the establishment of new treatments for non-iodineconcentrating thyroid carcinoma. Future Outlook: One major topic for the CCU Nuclear Medicine’s future research will be the identification of possible targets for new radiopharmaceuticals. For this purpose, the gene array data obtained from correlative PET and tumor specimen evaluations are screened for receptors and cell surface proteins. Following the identification of possible targets, the partners at the MPI Saarbrücken are using their FLEXx software, a small molecule docking software, to identify substances with a high likelihood of binding to the identified structures. Nuclear Medicine (E060) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2477 [email protected] The identification of new ligands will be one of the main areas of research in the laboratory. The group intends to apply biotechnology methods such as display (phage and ribosome display) of libraries consisting of scaffold proteins. This project addresses the identification of specific binders to targets overexpressed in a variety of tumors by using peptide libraries. We will concentrate on target structures identified either by literature research or by gene profiling data available at the campus. In the last 18 months we started intra-arterial therapy with DOTATOC in patients with metastasized neuroendocrine tumors using 90Y, 177Lu and 213Bi. This program will be extended to other peptides/receptors. Furthermore, novel treatment strategies, using radiolabelled benzamides in melanoma patients and PSMA ligands in patients with prostate carcinoma, have been successfully transferred into clinical application. ESSENTIAL PUBLICATIONS: (1.) Kratochwil C. et al. (2010). Intraindividual comparison of selective arterial versus venous 68Ga-DOTATOC-PET/CT in patients with gastroenteropancreatic neuroendocrine tumors. Clin Cancer Res, 16, 2899– 2905. (2.) Strauss L.G. et al. (2011). Shortened acquisition protocols for the quantitative assessment of the 2-tissue compartment mod-el using dynamic PET/CT 18F-FDG studies. J Nucl Med, 52, 379–385. (3.) Zoller F. et al. (2013). A Disulfide-Constrained Miniprotein with Striking Tumor-Binding Specificity Developed by Ribosome Display. Angewandte Chemie Int Edition, 52, 11760–11764. (4.) Altmann A. et al. (2010). Therapy of thyroid carcinoma with the histone deacetylase inhibitor MS-275. Eur J Nucl Med Mol Imaging, 37, 2286-2297. prior 104 after Research Program PET/CT with a Ga-68 labelled PSMA ligand prior and after endoradiotherapy with a I-131 labelled PSMA ligand in a patient with biochemical recurrence and multiple lymph node metastases. After one cycle, a decrease in tracer accumulation and a reduction of the number of metastases was seen. Imaging and Radiooncology Medical and Biological Informatics Division Head: Prof. Dr. Hans-Peter Meinzer Research in our division aims at improving diagnostic methods and treatment planning based on imaging technologies, such as computer tomography, magnetic resonance tomography and ultrasound. The division is currently active in different research areas of medical imaging, including image analysis for tissue differentiation, simulation and diffusion imaging. A recently established junior group is working on new methods in the field of computer assisted interventions. Central to our work is the idea of translational research, i.e. translating our findings, methods and software to the patient in the clinic. Therefore, we are closely collaborating with a large number of national and international hospitals, as well as various engineering institutes. Furthermore, we established a quality management process for our central software platform MITK (Medical Imaging Interaction Toolkit). Future Outlook: Since 2002 MITK, which is the central element of our research, has been the basis for all developments of the devision of Medical and Biological Informatics and is undergoing continuous development. In a joint effort to facilitate the international collaboration between different research groups, the Common Toolkit (CTK) project was initiated in 2009 by Prof. Dr. Ron Kikinis (Harvard Medical School) and Prof. Dr. Hans-Peter Meinzer, head of the MBI division. In this initiative, different research groups and companies from around the world are together developing a new common basis for software development in medical imaging. Another central orientation is microstructural analysis of the brain based on diffusionweighted magnetic resonance imaging (dMRI). As an example dMRI can help in detecting Alzheimer disease at an early stage. In surgical navigation, we are focusing on markerless localization of patient and instruments by means of Time-of-Flight (ToF) cameras which provide depth information in addition to a Research at DKFZ 2014 standard two-dimensional image. Concerning image analysis, we are involved in an obesity study with over 1200 patients. Further work focuses on automated differentiation of fat tissue in whole body MR images, which allows for examining the influence of distinct fat tissue types. A very recent development in our division is the use of portable devices, such as tablet computers, as both a radiological viewer and to assist surgical navigation. Additionally, the division is part of the recently established collaborative research center “Cognition Guided Surgery”. ESSENTIAL PUBLICATIONS: (1.) Fritzsche K.H. et al. (2012). MITK Diffusion Imaging. Methods of Information in Medicine, Methods Inf Med., 51, 441–418. (2.) van Bruggen T. et al. (2012). Do Alzheimer specific microstructural changes in mild cognitive impairment predict conversion? Psychiatry Res, 203(2-3), 184–193. (3.) Wald D. et al. (2012). Automatic Quantification Medical and Biological Informatics (E130) of Subcutaneous and Visceral Adipose Tissue from German Cancer Research Center Whole-Body Magnetic Resonance Images suitable for Large Cohort Studies. Journal of Magnetic Resonance Im Neuenheimer Feld 280 Imaging, 36, 1421–1434. 69120 Heidelberg (4.) Maier-Hein L. et al. (2012). Convergent Iterative Phone: +49 6221 42 2354 Closest-Point Algorithm to Accomodate Anisotrop- [email protected] ic and Inhomogenous Localization Error. IEEE Transactions on Pattern Analysis and Machine Intelligence, 34, 1520–1532. Three-dimensional reconstruction of an individual liver. The blood supply through the portal vein (light blue), the hepatic veins (dark blue), arteries (red), gall bladder (green) and three tumors (red), including safety margins (yellow), are shown. 105 Imaging and Radiooncology Optical Nanoscopy Division Head: Prof. Dr. Stefan Hell The resolution of light microscopes has been generally limited by the wavelength of light to about 250 nanometers. We have developed the first fluorescence microscopes capable of providing images with a resolution of fractions of light’s wavelength from the interior of a cell. A combination of two of our approaches, namely 4Pi and STED microscopy, makes it possible to achieve resolutions under 40 nanometers in all directions. This enables us to observe biological structures that are 2000 times thinner than a human hair. We are now trying to find out how we can achieve and exploit resolutions in the range of a few nanometers to fundamentally advance biological and clinical research. Future Outlook: Our goal is to develop techniques such as STED (Stimulated Emission Depletion Microscopy) to unveil sub-cellular structures at a resolution level of a few 10 nm in a living cell. After all, every disease manifests itself first in the cells. We are now exploring how the breakthrough in light microscopy resolution can be translated into fundamental advancements in biological and clinical research. STED light microscopy makes it possible to study the causes of diseases more closely and thus to speed up development of medications. Optical Nanoscopy (E190) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 54 51210 and +49 551 201 2500 [email protected] and Max Planck Institute for Biophysical Chemistry in Göttingen, Department of NanoBiophotonics 106 Research Program ESSENTIAL PUBLICATIONS: (1.) Chojnacki J. et al. (2012). Maturation-Dependent HIV-1 Surface Protein Redistribution Revealed by Fluorescence Nanoscopy. Science, 338, 524–528. (2.) Vicidomini G. et al. (2012). STED with wavelengths closer to the emission maximum., Opt Express, 20, 5225–5236. (3.) Bingen P. et al. (2011). Parallelized STED fluorescence nanoscopy. Opt Express, 19, 23716–23726. (4.) Berning S. et al. (2012). Nanoscopy in a living mouse brain. Science, 335, 551. Vimentin network of mammalian cell revealed by STED fluorescence microscopy with subdiffraction spatial resolution. Research at DKFZ 2014 107 Imaging and Radiooncology Translational Radiation Oncology Max-Eder-Junior Research Group Head: Dr. Dr. Amir Abdollahi Translational Radiation Oncology (E210) German Cancer Research Center Im Neuenheimer Feld 450 69120 Heidelberg Phone: +49 6221 56 39604 [email protected] Abdollahi’s group was one of the first to employ genome-wide transcriptional analysis and protein phosphorylation analysis to systematically investigate the perturbation of the cellular homeostasis induced by ionizing radiation and anti-/pro-angiogenesis. These discoveries have built a foundation to better understand inter-cellular communication and intra-cellular signalling principles induced by radiation and angiogenesis modulators, and unravelled key mechanisms governing tumor therapy resistance – a major obstacle of cancer therapy. Their data indicate that tumor-stroma and tumor-vessel communication i.e., microvasculature endothelial cells, constitute a critical target of conventional cancer therapies, such as radiation and chemotherapy. Subsequently, molecular, cellular and physiological rationales for the beneficial use of trimodal cancer therapy (consisting of anti-angiogenesis, radiotherapy and chemotherapy) were provided. The translational impact of this research on the development of novel clinical protocols is evident from the growing number of trimodal trials in solid tumors initiated in Heidelberg and worldwide. Intriguingly, they could also show that inhibition of PDGF signaling ameliorates the development of radiation-induced lung fibrosis, a critical side effect and dose limiting normal tissue response of radiotherapy. In addition, this group has recently discovered the potential of peripheral blood transcriptome and miRs as a sentinel organ to properly detect tumor stage and predict clinical outcome. Future Outlook: A major goal of this group is to generate an integrative molecular biology platform for identification of cell-cell and intracellular signaling networks induced by photon, proton and carbon irradiation incorporating transcriptomics, miRNA, epigenomics, proteomics and functional genomics approaches. These data will be instrumental in identification of novel molecular targets for modulating the radiation response, i.e., enhancing the anti-tumor effects while sparing surrounding normal tissue from radiation induced damage. They further aim to better understand the mechanism of local invasion and distant metastasis of tumors. The field of radiotherapy still lacks powerful biomarker and molecular classifiers of therapy response. Accordingly, they seek to design peripheral blood transcriptome and miRNA based patient classifier that would assist clinicians in selecting those patients likely to benefit most from the local multimodal therapies. Finally, the group aims to optimize local tumor control via rational design of multimodal therapies consisting of radiotherapy and tumor stroma targeting agents. A critical step towards this goal is the systematic investigation of compensatory mechanisms that render tumors resistant to radiotherapy and targeted i.e., antiangiogenic, cancer therapies. ESSENTIAL PUBLICATIONS: (1.) Abdollahi A. et al. (2010). Evading tumor evasion: Current concepts and perspectives of anti-angiogenic cancer therapy. Drug Resist Updat., 13, 16–28. (2.) Almog N. et al. (2009). Transcriptional Switch of Dormant Tumors to Fast-Growing Angiogenic Phenotype. Cancer Research., 69, 836–844. (3.) Abdollahi A. et al. (2007). Transcriptional network governing the angiogenic switch in human pancreat- From left: establishment of first preclinical models of lung irradiation with carbon ions, examples for verification of carbon ion dose distribution by PET/CT, evaluation of radiation-induced lung toxicity and microvascular damage. Clinical translation (right): irradiation of the first lung cancer patient with carbon ions at HIT in fall 2011. 108 Research Program ic cancer. Proc Natl Acad Sci U S A., 104, 12890–1285. (4.) Abdollahi A. et al. (2005). Inhibition of plateletderived growth factor signaling attenuates pulmonary fibrosis. J Exp Med., 201, 925–935. Imaging and Radiooncology Computer-assisted Interventions Junior Research Group Head: Dr. Lena Maier-Hein Medical interventions involving minimallyinvasive access to the internal anatomy of the patient are continuously gaining importance in the diagnosis and treatment of cancer and other diseases. The safety, efficiency and success of such interventions crucially depend on the precise navigation of medical instruments through the patient’s body, while taking critical structures into account. However, mental fusion of the partially visible anatomy with high-resolution pre-operative tomographic images and/or surgical planning data in the presence of organ motion is extremely challenging. Our multidisciplinary research group, which is associated with the Division of Medical and Biological Informatics, combines expertise from computing, physics and medicine in order to develop new concepts for computer-assisted medical interventions. Our focus is on technological innovation with a strong emphasis on clinical translation and direct patient benefits. Current research topics include robust and fast 3D localization of the patient anatomy using range imaging techniques, such as Time-ofFlight, real-time fusion of multi-modal patient data based on surface registration and new tracking techniques, as well as innovative human-computer interfaces. Further core areas include the modeling and propagation of system errors as well as workflow optimized approaches to computer guidance that balance the patient benefits with the complexity and cost of the assistance system. actions in a knowledge-based manner. Computer assistance shall cover the entire medical workflow from treatment planning, to plan execution, to follow-up, thereby supporting the physician without adding complexity or time compared to the conventional procedure. To maximize patient safety, the uncertainties associated with the different sources of information applied in the course of computerassisted treatment shall be properly modeled, propagated and fused. Finally, a flexible technical infrastructure will allow straightforward integration of new algorithms and devices and fast adaption to the dynamic advances in surgical and interventional techniques. Eventually, holistic analysis of all relevant data, objectivity in data interpretation and context-aware assistance will lead to improved clinical outcome. ESSENTIAL PUBLICATIONS: (1.) Maier-Hein L. et al. (20.13). Optical Techniques for 3D Surface Reconstruction in Computer-assisted Lap- Computer-assisted Interventions (E131) aroscopic Surgery. Med Imag Anal, 17, 974–996. German Cancer Research Center (2.) Maier-Hein L. et al. (2012). Convergent iterative Im Neuenheimer Feld 280 closest-point algorithm to accomodate anisotropic and inhomogenous localization error. IEEE T Pattern 69120 Heidelberg Anal, 34, 1520–1532. Phone: +49 06221 42 2341 (3.) Seitel A. et al. (2011). Computer-assisted trajecto- [email protected] ry planning for percutaneous needle insertions. Med Phys, 38, 3246–3259. (4.) Maier-Hein L. (2008). In vivo accuracy assessment of a needle-based navigation system for CT-guided radiofrequency ablation of the liver. Med Phys, 35, 5385–5396. Future Outlook: In the field of computer-assisted medical interventions, the immense capabilities of computers in terms of storing and processing huge amounts of data have not yet been fully exploited. The vision of our group is to improve patient care by an objective, context-aware and combined analysis of all relevant data in the course of disease treatment. Dynamically acquired factual and practical knowledge (e.g. study results, clinical outcomes in similar cases) as well as individual patient data (e.g. laboratory data, preoperative images, intra-operative sensor data) shall be continuously accumulated and processed to support the physician’s decisions and Research at DKFZ 2014 Computer-assisted radiofrequency ablation (RFA) of the liver. 109 Coordinator Prof. Dr. Lutz Gissmann Infection and Cancer Viruses play a crucial role in a number of cancers. This Research Program investigates the mechanisms by which viruses cause cancer and the ways by which the body defends itself. In addition, researchers are isolating and characterizing unknown viruses from tumor material. Special attention is directed to the diagnosis, prevention, and treatment of such viral infections. Furthermore, scientists are working on methods using viruses to selectively kill cancer cells or as vehicles for introducing therapeutic genes into cells. Current focuses of tumor-virological research are: • • • • • 110 Papilloma viruses and their role in cancers of the genital organs, the mouth and throat, and the skin Parvoviruses as direct inhibitors of tumor growth and as gene vectors for cancer treatment Retroviruses (HIV, spumaviruses) for developing specific therapies Anelloviruses (TT viruses) and their effect on the host cell genome Herpesviruses (Epstein-Barr viruses) in the development of malignant tumors and as gene vectors for cancer therapy. Research Program Research at DKFZ 2014 111 Infection and Cancer Tumorvirology Division Head: Prof. Dr. Jean Rommelaere Tumorvirology (F010) German Cancer Research Center Im Neuenheimer Feld 242 69120 Heidelberg Phone: +49 6221 42 4960 [email protected] The Division Tumor Virology should actually be called “Anti-Tumor Virology” since its objective is to develop oncolytic viruses (preferentially killing tumor cells) and viral vectors (transferring therapeutic genes into diseased, including cancer, cells). Our activities have led to the launching of a clinical trial using the oncolytic parvovirus H-1PV to treat malignant gliomas, and the advanced validation of adeno-associated virus (AAV)-based vectors. Three main research axes are presently developed. 1. Investigation of the interactions of oncolytic parvoviruses (PV) with host cells, in particular (i) cellular markers predictive of tumor responsiveness to PV treatment, (ii) PV determinants of host range, (iii) molecular pathways involved in PV oncotoxic and immuno-modulating properties, (iv) PV-mediated delivery of cyto- and chemokines into tumors and their microenvironment. 2. Proofs of concept for future clinical trials using oncolytic parvoviruses, including (i) preclinical evaluation of the applicability of H-1PV therapy to malignancies in children and adolescents, (ii) development of novel anticancer strategies based on combining of H-1PV with epigenetic modulators, (iii) study of immuno-modulating effects of H-1PV to optimize its use to treat pancreatic carcinomas. 3. Our Virus Production & Development Unit standardizes protocols for virus application to humans, and supports trialaccompanying research. Future Outlook: Basic research will be pursued to unravel the cellular and parvoviral determinants of cell permissiveness and killing, respectively. This program is expected to contribute to identify patients susceptible to oncolytic virus-based treatments (“customized” therapy). Furthermore, our ambition is also to understand and optimize the interplay between parvovirus oncolytic effects and host anti-tumor immune responses (through parvovirus arming with chemokines or modulation of critical steps of the viral life-cycle, in particular egress). On the translational level, our work aims to broaden the range of indications for a potential H-1PVbased oncolytic virotherapy. In order to prepare future clinical trials, besides the glioma study already under way, optimal treatment strategies combining parvoviruses with different classes of antineoplastic and immunomodulating agents will be tested, using various in vitro and in vivo models. On the basis of promising pre-clinical data, priority will be given to clinical validation of treatment efficacy in pancreatic carcinoma patients and in patients with relapsed or refractory tumors in the field of pediatric neuro-oncology. ESSENTIAL PUBLICATIONS: (1.) Li J. et al. (2013). Synergistic combination of valproic acid and oncolytic parvovirus H-1PV as a potential therapy against cervical and pancreatic carcinomas. EMBO Molecular Medicine, 5, 1537–1555. Treatment of an intracerebral rat glioma with parvovirus H-1 (H-1PV). MRI of a rat brain bearing a glioma, at the time of infection with H-1PV (left), and 8 days later (right), showing disappearance of the tumor after infection. (2.) Bär S. et al (2013). Vesicular transport of progeny parvovirus particles through ER and Golgi regulates maturation and cytolysis. PLOS Pathogens, 9, e1003605. Doi:10.1371/journal.ppat.1003605. (3.) Nüesch J.P.F. et al (2012). Molecular pathways: rodent parvoviruses: mechanisms of oncolysis and prospects for clinical cancer treatment. Clinical Cancer Research, 18, 3516–3523. (4.) Geletneky K. et al (2010). Regression of advanced rat and human gliomas by local or systemic treatment with oncolytic parvovirus H-1 in rat models. Neuro-Oncology, 12, 804–814. 112 Research Program Infection and Cancer Genome Modifications and Carcinogenesis Division Head: Prof. Dr. Lutz Gissmann We have a long-standing interest in the immune response against Human Papillomaviruses (HPV) focusing on the question whether antibodies directed against certain viral proteins can influence the natural cause of an infection and whether they can predict its clinical outcome. At present we investigate the potential of an HPV vaccine to prevent recurrence of genital warts and are studying the possibility to cure chronic infections by activation of HPV-specific T cells. ESSENTIAL PUBLICATIONS: By the aid of a high-throughput platform for simultaneous detection of different antibodies or nucleic acids that has been developed in our laboratory, we are analyzing large sample collections from epidemiologic studies aiming at the identification of papillomaviruses and other infectious agents (viruses and bacteria) as causal factors for certain kinds of cancer where such an involvement has as yet not been demonstrated. Using our technology we will investigate whether specific HPV mRNAs are suitable biomarkers for early detection of HPVinduced cervical cancer. (4.) Schädlich L. et al. (2009). Analysis of modified (1.) Senger T. et al. (2010). Virus-like particles and capsomeres are potent vaccines against cutaneous alpha HPVs Vaccine. Vaccine, 28, 1583–1593. (2.) Schmitt M. et al. (2010). Diagnosing Cervical Cancer and High-Grade Precursors by HPV16 Transcription Patterns. Cancer Res, 70, 249–256. (3.) Dell K. et al. (2006). Intransasal immunization with human papillomavirus type 16 capsomeres in the presence of non-toxic cholera toxin-based adjuvants elicits increased vaginal immunoglobulin levels. Vaccine, 24, 2238–2247. HPV 16 L1 capsomeres: The ability to assemble into larger particles correlates with higher immunogenicity. J Virol, 83, 7690–7705. Genome Modifications and Carcinogenesis (F020) German Cancer Research Center Im Neuenheimer Feld 242 69120 Heidelberg The program on Foamy Viruses from different animal species deals with their host restriction and the evaluation of a possible inter-species transmission (zoonosis) thereby potentially acquiring transforming properties also in humans. Phone: +49 6221 42 46 03 [email protected] We also study the role two classes of molecules (cyclooxygenases and lipoxygenases) that are central in chronic inflammation which is a well-defined risk factor for cancer development. Instrumentation for multiplex serology and multiplex genotyping Research at DKFZ 2014 113 Infection and Cancer Viral Transformation Mechanisms Division Head: Prof. Dr. Frank Rösl Viral Transformation Mechanisms (F030) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4900 [email protected] Mitochondria staining in primary keratinocytes (orange). Courtesy of Dr. B. Rincon Orozco (F030) 1. Mechanisms of human papillomavirus (HPV)-induced carcinogenesis: Here we are investigating how transcription and viral RNA splicing of high-risk HPV is regulated during the different steps towards malignant transformation. Another focus is the function of epigenetic mechanisms (e.g. de novo methylation, nucleosomal organisation, micro-RNAs) in HPV-positive cells and their impact on viralhost interaction during persistence. 2. Immunological surveillance: In this context, we are studying the interferon/chemokine pathway to understand the innate response against viral and bacterial infections. Moreover, with respect to the role of inflammation in cancer, we are examining the function of individual HPV oncoproteins on the NALP3 inflammasome. 3. A natural rodent model system for papillomavirus (PV)-induced skin cancer: In this project we study the whole infection pathway, starting from primary infection till the final manifestation of a skin tumor in molecular and serological terms. We have also developed a “virus-like particle” (VLP) based vaccine to prevent PV-induced skin lesions. This vaccine is efficient both under normal and immunocomprimised conditions and may provide the basis for the clinical development of potent immunization strategies against cutaneous HPV infections and HPV-induced tumors, especially in patients awaiting organ transplantation. 4. Virus-Cell Interactome: Considering a cell as a functional regulatory network, tumorviruses always attack central hubs to overcome intracellular surveillance. It is therefore necessary to understand these viral-host interactions using both approaches of systems biology and high-throughput strategies. Particularly potential co-infections (e.g. with bacteria), their communication pathways and cross-talks are under investigation. already mapped the regulatory region of the LKB1 tumor suppressor gene, a central master kinase that controls the intracellular energy status. This gene is found to be dysregulated in HPV-positive cells. We have also dissected the mechanism whereby tumor cells sense their own metabolism. We will further analyse the innate immune response under hypoxic and energy-deprived conditions. 2. Cellular escape mechanisms: This study aims to understand the spatial and temporal interaction of immunological effector cells of the innate defence system with non-tumorigenic HPV-positive cells, in direct comparison with their tumorigenic counterparts in immunocompromized animals. In addition, we design experiments that allow the characterization of genes and intracellular regulatory pathways in transplanted HPV-positive cells responsible for tumor suppression. 3. Resistance mechanisms: Cancer cells are robust and highly adaptive against various therapeutic approaches. Although most of the tumor mass can be eradicated in vivo and in vitro, there are still cells which survive. Whether these represent cancer stem cells will be studied in further detail. ESSENTIAL PUBLICATIONS: (1.) Rincon-Orozco B. et al. (2009). Epigenetic silencing of interferon-κ in human papillomavirus type 16 positive cells. Cancer Research, 69, 8718–8725. (2.) Rosenberger S.J. et al. (2010). Alternative splicing of HPV16 E6/E6* early mRNA is coupled to EGF-signalling via Erk activation. Proc. Natl. Acad Sci. U.S.A., 107, 7006–7011. (3.) Lützner N. et al. (2012). FOXO3 is a Glucocorticoid Receptor Target Gene and Regulates LKB1 and FOXO3 Expression Dependent on Intracellular Energy Levels Via a Positive Autoregulatory Feedback Loop. PLoS One. 7: e42166. (4.) Niebler M. et al. (2013). Post-Translational Control of IL-1β via the Human Papillomavirus Type 16 E6 On- Future Outlook: Beside the current projects which will be followed up in greater detail, we will focus our future interest on the following topics: 1. Metabolism and cancer: Here we will especially determine the function of the viral oncoproteins on the metabolic pathway. We have 114 Research Program coprotein: A Novel Mechanism of Innate Immune Escape Mediated by the E3-Ubiquitin Ligase E6-AP and p53. PLoS Pathog. Aug;9(8):e1003536 Infection and Cancer Characterization of Tumorviruses Division Head: Prof. Dr. Ethel-Michele de Villiers It has not been possible to associate the ubiquitous TT viruses to a specific disease entity, despite initial intensive worldwide investigation. We conducted our investigations along several lines in order to address this problem: Serum samples and biopsies from healthy individuals, as well as from patients with multiple sclerosis, rheumatoid arthritis, colon carcinoma, leukemia and lymphoma were analyzed for the presence of TT virus DNA. Although TT virus DNA was present in the majority of these samples, we demonstrated the existence of additional intragenomic rearranged viral molecules: one comprising replication-defective and the other replication-competent episomes. The latter consisted of as little as 10% of the originating full-length TT virus genome and was termed µTTV. We developed an in vitro replication system for these viruses in which we confirmed the formation and existence of µTTV molecules, along with the replication of the respective full-length genomes. Intragenomic rearranged TT molecules, as well as in vitro transcripts revealed new open reading frames of which the putative proteins shared similarities to signature motifs present in cellular proteins involved in autoimmune diseases. The highly conserved region (71 bp) of TT viruses harboring the origin of replication was demonstrated in a spectrum of cell lines. Long distance PCRamplification based on this region led to the identification of circular chimeric molecules comprising TT virus sequences combined with cellular sequences. A large series 0f bovine sera was analyzed for TT sequences. Future Outlook: Proteins expressed by TT viral and subviral genomes are characterized and tested for a possible role in “molecular mimicry“ through their cross-reaction against antibodies involved in autoimmune diseases. The mechanism underlying the origin and function of cellular-TT virus chimeric molecules is being investigated. Specificity of the chimeric recombinant molecules for certain types of tumors and autoimmune diseases will be investigated. This may then, in addition, lead to their development Research at DKFZ 2014 and use as diagnostic markers. The origin and function of an unusual pattern of TT virus sequences identified in bovine serum samples will be analyzed, as well as possible transmission of TT virus originating from cattle (via serum, saliva and milk) to humans. An intensive search for putative new viruses involved in tumorigenesis is continuing, with transmission from cattle to humans being the main focus. Full-length genomes of newly identified TT virus are being isolated and characterized from serum samples from leukemia patients. Development of chimeric constructs for use as extra chromosomal vectors poses an important challenge. ESSENTIAL PUBLICATIONS: (1.) de Villiers E.M. et al. (2011). The diversity of Torque teno viruses: In vitro replication leads to the formation of additional replication-competent subviral Characterization of Tumorviruses (F070) Molecules. J Virol, 85, 7284–7295. German Cancer Research Center (2.) zur Hausen H. (2012). Red meat consumption and cancer: Reasons to suspect involvement of bovine in- Im Neuenheimer Feld 280 fectious factors in colorectal cancer. Int J Cancer, 130, 69120 Heidelberg 2475–2483. Phone: +49 6221 42 4655 (3.) de Villiers E.-M. et al. (2009). Intragenomic rearrangement in TT viruses: a possible role in the patho- [email protected] genesis of disease. Curr. Top. Microbiol. Immunol., 331, 91–107. (4.) de Villiers E-M. (2013). Cross-roads in the classification of papillomaviruses. Virology, 445, 2–10. Mechanisms under investigation for a role of TT viruses in the pathogenesis of disease 115 Infection and Cancer Pathogenesis of Virus Associated Tumors Division Head: Prof. Dr. Dr. Henri-Jacques Delecluse Pathogenesis of Virus Associated Tumors (F100) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4870 The Epstein-Barr virus is etiologically linked with 2% of all malignant tumors worldwide. Hence, a very substantial number of cancers could be prevented by vaccination against this virus. Our research interests are focused on the molecular mechanisms that allow multiplication, infection and ultimately, malignant transformation of B cells and epithelial cells. The large size of the viral genome precludes the use of conventional cloning techniques; instead we have developed a genetic system that allows modification of every single base pair within the viral genome. Over the years we have used this technology to construct a large panel of viral mutants that lack genes involved in multiple virus functions. More recently, we have focused our attention on viral non-coding RNAs, such as the first described v-snoRNA1 or the BHRF1 microRNA cluster. A virus that lacks all three members of this cluster displays a reduced propensity to transform B lymphocytes. Another avenue of research is the study of EBV interactions with primary epithelial cells. Although the virus mainly replicates in these cells, they also express the viral oncogene LMP1, suggesting links between between virus replication and epithelial transformation. We have also generated mutants that could be potentially used as vaccines. Indeed, these produce large amounts of viral DNA-free virus-like particles (VLPs). These particles elicit a strong immune response, yet have lost any pathogenic potential. Future Outlook: Future projects aim at pursuing the genetic analysis of EBV functions. In particular, we intend to identify the members of the BHRF1 miRNA cluster responsible for the phenotypic traits observed in the triple deletion mutant. We also intend to expand our projects on the molecular interactions between EBV and epithelial cells. ESSENTIAL PUBLICATIONS: (1.) Feederle R. et al. (2009). The Epstein-Barr virus alkaline exonuclease BGLF5 serves pleiotropic functions in virus replication. J Virol., 83, 4952–4962. (2.) Hutzinger R. et al. (2009). Expression and processing of a small nucleolar RNA from the Epstein-Barr virus genome. PLoS Pathog., 5(8):e1000547. (3.) Busse C. et al. (2010). Epstein-Barr viruses that express a CD21 antibody provide evidence that gp350’s functions extend beyond B-cell surface binding. J Virol., 84, 1139–1147. (4.) Feederle R. et al. (2011). A Viral microRNA cluster strongly potentiates the transforming properties of a Human Herpesvirus. PLoS Pathog, 7(2): e1001294. [email protected] Primary squamous epithelial cells infected with a recombinant EpsteinBarr virus tagged with a GFP gene. 116 Research Program Infection and Cancer Immunotherapy and -prevention Junior Research Group Head: PD Dr. Dr. Angelika Riemer At least 20% of human malignancies are caused by consequences of persistent infections. Cancers caused by infectious agents (e.g. human papillomavirus – HPV) are attractive targets for cancer vaccination approaches, as they provide the opportunity to target antigens that are immunologically non-self. Vaccination can be prophylactic, inducing antibodies that prevent infection, or therapeutic, stimulating the cellular immune system into eradicating established disease. Prophylactic immunization against HPV has become the paradigm for cancer immunoprevention. Unfortunately, current HPV vaccines have no therapeutic effect on existing infections. The aim of therapeutic vaccination is to stimulate the immune system into recognizing and destroying malignant cells. Cytotoxic T cells (CTL) kill infected cells after recognizing bits of viral proteins, so-called epitopes, which are presented on human leukocyte antigen (HLA) molecules on the cell surface. There are thousands of different HLA types, all presenting different epitopes. As every human being has a different set of HLA molecules, epitopes for all major HLA groups need to be defined. The overall aim of this group is to generate a therapeutic cancer vaccine against HPV-induced malignancies that is applicable to everyone, regardless of a person’s HLA type. We are currently working on the precise identification of which HPV epitopes are present on tumor cells using a specialized mass spectrometry (MS) approach. gate differences in the inflammatory status of early HPV-induced lesions between people who mount effective immune responses and those who do not. Since T helper cells are also crucially involved in HPV clearance, another project deals with the identification of naturally processed promiscuous HPV-derived HLAclass-II epitopes. The inclusion of such epitopes in therapeutic vaccine formulations is likely to enhance their efficacy. Future aims are to examine various vaccine delivery and adjuvant formulations. All these studies will contribute to an optimal formulation of a therapeutic vaccine, aiming at the effective induction of adaptive immune responses in persistently HPV-infected patients. The developed technology could then be applied to more high-risk HPV types, but also to low-risk types which are causing significant morbidity. If this approach using an epitope-specific, yet widely applicable, therapeutic vaccine is successful, it may be further developed into a platform technology against other malignancies. Insights gained during this process may be used in the further development of cancer vaccinology. Immunotherapy and Prevention (F130) German Cancer Research Center Im Neuenheimer Feld 280 ESSENTIAL PUBLICATIONS: 69120 Heidelberg (1.) Riemer A.B. et al. (2010). A conserved E7-derived Phone: +49 6221 42 3820 CTL epitope expressed on human papillomavirus-16 transformed HLA-A2+ human epithelial cancers. [email protected] J. Biol. Chem., 285, 29608–29622. (2.) Anderson K.S. et al. (2011). Impaired tumor antigen processing by immunoproteasome-expressing CD40-activated B cells and dendritic cells. Cancer Im- Future Outlook: As nearly every sexually active individual acquires a high-risk HPV infection during their lifetime, but only 1-2% develop persistent infection, there must be differences in the induction of effective immune responses. It has been shown that local inflammatory cytokines are needed for the generation of anti-HPV effector T cells. We therefore plan to investi- munol. Immunother., 60, 857–867. (3.) Riemer A.B. et al. (2005). Vaccination with cetuximab mimotopes and biological properties of induced anti-EGFR antibodies. J. Natl. Cancer Inst., 97, 1663–1670. (4.) Riemer A.B. et al. (2004). Generation of peptide mimics of the epitope recognized by trastuzumab on the oncogenic protein Her-2/neu. J. Immunol., 173, 394–401. Mechanisms under investigation for a role of TT viruses in the pathogenesis of disease Research at DKFZ 2014 117 Infection and Cancer Noroviruses CHS Junior Research Group (in Cooperation with Heidelberg University) Head: Dr. Grant Hansman Noroviruses (F150) CHS Research Group at CellNetworks Heidelberg University and DKFZ German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 1520 [email protected] Noroviruses are now known to be the dominant cause of outbreaks of gastroenteritis around the world. Currently, there are no vaccines for noroviruses and cross-protection from future norovirus infections is uncertain, and it is not uncommon for re-infection with a genetically similar strain. Although the disease is self-limiting, symptoms can persist for days or even weeks and transmission from personto-person is difficult to control once the outbreak has occurred. Noroviruses are an enormous problem in closed settings such as hospitals, nursing homes, cruise ships and schools. Human noroviruses are frequently associated with food-borne outbreaks of gastroenteritis. In a nutshell, human noroviruses are everywhere and infect all age groups. Human noroviruses are uncultivable, but expression of the capsid protein in a baculovirus expression system results in the self-assembly of virus-like particles (VLPs) that are morphologically and antigenically similar to the native virion. The X-ray crystal structure of the VLP shows the capsid is divided into two domains, shell and protruding (P) domains. The P domain is further divided into P1 and P2 subdomains, with the P1 subdomain interacting with the shell and the P2 subdomain residing on the outer surface of the capsid and likely containing the determinants for receptor binding and antigenicity. The human histo-blood group antigens (HBGAs) have been identified as potential co-factors for norovirus. A number of crystal structures have been determined for HBGAs in complex with P domains. Our group plans to express a panel of norovirus strains in order to better understand the interactions with the polymorphic HBGAs. Recently, we analyzed the interaction of citrate with GII noroviruses using X-ray crystallography and saturation transfer difference (STD) NMR. We found that the citrate interaction was coordinated with an almost identical set of capsid interactions involved in recognizing the terminal HBGA fucose, the saccharide which forms the primary conserved interaction between HBGAs and GII noroviruses. STD NMR showed the protruding domain to have weak affinity for citrate, but could compete against the soluble HBGAs for the HBGA binding site. Our group plans to screen other candidate drug molecules that bind and inhibit norovirus attachment to cells. We recently solved the cryo-EM structure of the non-infectious GII.10 VLPs and found that the overall capsid structure was very similar to the murine norovirus virion, including raised and rotated P domains. Surprisingly, for over 12 years, the prototype GI.1 human norovirus VLP was considered a good representative for all human norovirus capsid structures and the same group later demonstrated this with the structure of a GII.4 human norovirus VLP. The analysis of the GII.10 VLP cryo-EM structure indicated that the norovirus capsid was extremely flexible and this flexibility could be the underlying basis for receptor binding and antibody specificity. Our group plans to determine the structures of other human norovirus VLPs in order to describe the extent of the structural diversity and to better understand capsid flexibility. ESSENTIAL PUBLICATIONS: (1.) Hansman G.S. et al. (2012). Structural basis for broad detection of genogroup II noroviruses by a monoclonal antibody that binds to a site occluded in the viral particle. J Virol., 86, 3635–3646. (2.) Hansman G.S. et al. (2012). Structural basis for norovirus inhibition and fucose mimicry by citrate. J Virol., 86, 284–292. (3.) Hansman G.S. et al. (2011). Crystal Structures of GII.10 and GII.12 Norovirus Protruding Domains in Complex with Histo-Blood Group Antigens Reveal Details for a Potential Site of Vulnerability. J Virol., 85, 6687–6701. (4.) Ozawa K et al. (2007). Norovirus infections in symptomatic and asymptomatic food handlers in Japan. J Clin Microbiol., 45, 3996–4005. This Junior Research Group is generously Schematic representation of norovirus 118 Research Program supported by the Chica-and-Heinz-SchallerFoundation (CHS). Infection and Cancer Infection and Innate Immune Sensing Dynamics CHS Junior Research Group (in Cooperation with Heidelberg University) Head: Dr. Steeve Boulant Polarized cells have developed unique biosynthetic and sorting pathways to regulate intracellular trafficking and maintain polarity. Our laboratory is interested in how cellular polarity influences virus host interactions. Our research is focused on how enteric viruses enter human polarized intestinal epithelial cells (IECs) and how these cells respond to pathogen infection. Our model virus is reovirus, the prototype of the Reoviradae family, which contains the medically important virus Rotavirus. The main projects within the lab are: Virus Entry and membrane penetration Reovirus enters polarized cells by clathrin-mediated endocytosis after binding to the tight junction protein Jam-A and β1 integrin. Our goal is to characterize how viruses attach to their receptors and whether this interaction promotes their active uptake by the cell. Using single particle tracking approaches and live cell microscopy, we are particularly interested in the molecular aspects that allow the coupling of the viral particles to the endocytic machinery. After cellular uptake, reoviruses traffic through the early and late endosomes. These viruses require activation in the late endosomes to release the replication competent core into the cytoplasm. However, the exact mechanism of how a non-enveloped virus is able to breach the lipid membrane to reach the cytosol remains unclear. We are currently developing high resolution imaging and correlative microscopy techniques to shed light on how this process is orchestrated within the cell. Anti-viral innate immune response IECs constitute the primary barrier that enteric pathogens have to pass to establish infection originating in the gut. Indeed, despite being in constant contact with the commensal bacterial and viral flora, IECs in physiological conditions do not generate a constant pro-inflammatory response. As such, IECs have developed unique strategies to tolerate the commensal microbial flora and, at the same time, to effi- Research at DKFZ 2014 ciently protect against pathogens. We have shown that IECs can generate a different qualitative/quantitative innate immune response upon viral infection, depending on where the infection originates (apical vs basolateral). Our goal is to elucidate the molecular mechanisms that differentially regulate innate immune response in polarized epithelial cells infected by viruses. Ultimately, we aim to understand how the innate immune response in the intestine is regulated to maintain colonic homeostasis. Dis-regulation of this fine balance is responsible for gut inflammation which leads to the development of carcinoma. ESSENTIAL PUBLICATIONS: (1.) Boulant et al. (2013). Similar uptake but different trafficking and escape routes of reovirus virions and infectious subvirion particles imaged in polarized Madin-Darby canine kidney cells. Mol Biol Cell, 4, 1196–1207. (2.) Boulant S. et al. (2011). Actin dynamics counteract membrane tension during clathrin-mediated endocytosis. Nat Cell Biol, 13, 1124–1131. (3.) Cocucci E. et al. (2012). The first five seconds in the life of a clathrin-coated pit. Cell, 150, 495–507. (4.) Boulant S. et al. (2011). Recruitment of cellular Infection and Innate Immune Sensing Dynamics (F140) CHS Research Group at CellNetworks Heidelberg University and DKFZ German Cancer Research Center clathrin to viral factories and disruption of clathrin- Im Neuenheimer Feld 581 dependent trafficking.Traffic, 12, 1179–1195. 69120 Heidelberg This Junior Research Group is generously supported by the Chica-and-Heinz-Schaller- Phone: +49 6221 42 1560 [email protected] Foundation (CHS). Infection of polarized human intestinal cells (T84) by the enteric virus reovirus. (Red): JAMA, tight junction protein and the cellular receptor for reovirus (Green): Reovirus viral factories (Blue): Cell nuclei, which show a fragmentation pattern due to apoptosis/ necrotic state induced by the virus. 119 Coordinator Prof. Dr. Christof von Kalle Translational Cancer Research The DKFZ Translational Cancer Research Program serves an important bridging function between the DKFZ and cooperating clinical facilities at the Medical Center from bench to bedside. The research divisions contributing to this program are primarily headed by physician scientists. A significant number of the divisions is closely interacting with the National Center for Tumor Diseases (NCT). NCT, the first state-of-the- art comprehensive cancer center in Germany, was formed and built in close cooperation with the Heidelberg University Medical School (HUMS) and German Cancer Aid. NCT provides infrastructure and resources that integrate and support all of DKFZ’s and HUMS’s clinical and translational cancer research activities. NCT’s mission is to foster interdiscip- linary oncology for an optimized development of current clinical therapies and to rapidly transfer scientific knowledge into clinical applications. The Translational Cancer Research Program addresses the theme of Precision Oncology, combining clinical algorithms and state-of-the-art molecular profiling to create diagnostic, therapeutic and preventive strategies precisely tailored to patients’ individual disease requirements. This Program aims to: • • • DISCOVER molecular mechanisms of neoplastic transformation by patient-oriented high-throughput diagnostics and stratification; examination of molecular pathways, targets and biomarkers in tumor development and metastasis; analysis of molecular and functional heterogeneity within tumors. DEVELOP diagnostic markers and tests by development of small molecules in therapeutic model systems; identification of biomarkers of drug action and tumor responsiveness; examination of microenvironment and inflammatory processes; modulation of tumor immune responses. TREAT by validation of new drugs, vaccines and strategies; determination of outcomes in molecularly stratified patient cohorts; elucidation of mechanisms of resistance and recurrence in functional models; development of early-detection strategies and population-wide screening programs. NCT has implemented a highly innovative Precision Oncology Program (NCT POP). NCT POP is a center-wide master strategy that coordinates all translational activities and focuses resources towards individualized cancer medicine, including patient-oriented strategies in genomics, proteomics, immunology, radiooncology, prevention, and early clinical development. The NCT MASTER (Molecularly Aided Stratification for Tumor Eradication) umbrella protocol streamlines the entire diagnostic trial workflow to perform and evaluate molecular diagnostics on materials from all consenting NCT patients, with the explicit purpose of stratifying each patient for the best treatment or trial strategy. 120 Research Program Research at DKFZ 2014 121 Translational Cancer Research Translational Oncology Division Head: Prof. Dr. Christof von Kalle Translational Oncology (G100) German Cancer Research Center Im Neuenheimer Feld 460 69120 Heidelberg Phone: +49 6221 56 6990 [email protected] The division of Translational Oncology, lead by Christof von Kalle, coordinates all major aspects of creating and growing NCT and the translational research topics of DKFZ. The research program of the department focuses on the genetic diagnosis and modification of stem cell populations in cancer and other genetic diseases. Comprehensive mechanistic analysis of clonal dominance and proprietary high-throughput genomics are used to study the cellular and molecular mechanisms of disease initiation, progression and metastasis formation of cancer initiating cells, as well as equivalent mechanisms in leukemia, aiming at identification of new therapeutic targets. Molecular studies focus on mutations in inherited and acquired genetic diseases, including cancer, and serve as the basis of virus-derived therapeutics to treat them. This work has led the field internationally in important aspects of gene therapy, and has pioneered mechanistic investigations of vector integration using state-of-the-art high-throughput genomics and bioinformatics. The division guides the development of the NCT Precision Oncology Program (NCT POP), which aims to provide a comprehensive high-throughput molecular and cellular analysis of every patient treated at NCT, leading to therapeutic stratification according to specific molecular and cellular targets found in their individual tumors. Bone marrow infiltration, as determined by immunohistochemical staining for CD20 (top of panel A), was 70% before vemurafenib treatment and cleared with treatment. The size of the hairy-cell leukemia clone in the peripheral blood, as assessed by immunophenotyping (CD20 and CD103) (bottom of panel A), decreased rapidly with vemurafenib treatment. Future Outlook: The division of Translational Oncology will further develop its research program focus in the field of normal and cancerous stem cell biology, insertional mutagenesis in cancer and gene therapeutic approaches. It aims to decipher mechanisms of tumor initiation, self-renewal, metastasis and heterogeneity of tumor-initiating cells and of the step-wise malignant transformation in leukemogenesis. The division drives the development of NCT Precision Oncology Program (NCT POP) that aims at stratification of cancer patients based on molecular alterations, aimed at targeted treatment approaches and hypothesis-driven interventional trials. Structural and functional genomics and innovative treatment approaches target individual genetic lesions. Future clinical studies will include real-time high-throughput clonal monitoring of the T-lymphocyte repertoire in immunotherapy and of gene corrected cells. New vector systems allowing either reduced integration efficiency (integrase-deficient lentiviral vectors) and/or targeted integration in specific safe genomic locations (zinc finger nucleases) are being developed. Elucidation of genomic instability and the role of double-strand breaks in carcinogenesis are rapidly growing direct extensions of this work. Functional genomics studies aim at new therapeutic strategies breaking therapy resistance in high risk chronic lymphocytic leukemia. Furthermore, second-generation measles virus for oncolytic therapy will be tested with the objective of phase I clinical trial development. ESSENTIAL PUBLICATIONS: (1.) Kaeppel C. et al. (2013). A largely random AAV integration profile after LPLD gene therapy. Nat Med, 19, 889–891. (2.) Dietrich S. et al. (2012). BRAF inhibition in refractory hairy-cell leukemia. N Engl J Med, 366, 2038–2040. (3.) Dieter SM. et al. (2011). Distinct types of tumor-initiating cells form human colon cancer tumors and metastases. Cell Stem Cell, 9, 357–365. (4.) Gabriel R. et al. (2011). An unbiased genome-wide analysis of zinc-finger nuclease specificity. Nature Biotech, 29, 816–823. 122 Research Program Translational Cancer Research Applied Tumor Biology Clinical Cooperation Unit Head: Prof. Dr. Magnus von Knebel Doeberitz The Clinical Cooperation Unit Applied Tumor Biology is a clinical research cooperation unit with the Department of Applied Tumor Biology of Heidelberg University Hospitals and is part of the Molecular Medicine Partner Unit of the European Molecular Biology Laboratory (EMBL). Our major scientific interests relate to mechanisms of genomic instability triggered by human papillomavirus infections and DNA mismatch repair deficiency. We aim to identify novel diagnostic markers and potential therapeutic targets. We design and organize clinical trials, in cooperation with several clinical partners, to validate the clinical impact of respective markers and targets. We further successfully established “spin off” companies to guarantee the “clinical translation” of scientific concepts into commercially available certified products. Examples of diagnostic markers developed by our group are p16INK4a and the CINtec® product line used as diagnostic markers for HPV-induced lesions in histo- and cytopathology, that within a few years have become the new global gold standard in the diagnostics of HPV-associated neoplasms. We further developed a novel immune surveillance concept for DNA mismatch repair deficient cancers that led to the development of vaccines presently being tested in clinical trials. Current research activities of our group are focussing further on the epigenetic regulation of human papillomavirus infections. ESSENTIAL PUBLICATIONS: (1.) von Knebel Doeberitz M. et al. (2012). Biomarkers for cervical cancer screening: the role of p16(INK4a) to highlight transforming HPV infections. Expert Rev Proteomics, 9 ,149–163. (2.) Reuschenbach M. et al. (2012). Evaluation of cervical cone biopsies for coexpression of p16INK4a and Ki-67 in epithelial cells. Int J Cancer, 130, 388–394. (3.) Kloor M. et al. (2012). Prevalence of mismatch repair-deficient crypt foci in Lynch syndrome: a pathological study. Lancet Oncol, 13, 598–606. (4.) Kloor M. et al. (2011). Analysis of EPCAM protein Applied Tumor Biology (G105) expression in diagnostics of Lynch syndrome. J Clin German Cancer Research Center Oncol, 29, 223–227. Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 2487 [email protected] Example for HPV transformed cells in histology (a and c) and cytology (b and d) specimens stained for p16INK4a (a & c) and p16INK4a and Ki67 (b & d). Co-expression of both markers unequivocally indicates transformation of these cells even in a cytology sample. This results in a substantially better reproducible and more sensitive and specific identification of HPV-associated pre-cancer cells,thus helping to overcome most limitations of current cervical cancer early detection programs. Research at DKFZ 2014 123 Translational Cancer Research Preventive Oncology Division Head: Prof. Dr. Cornelia Ulrich Preventive Oncology (G110a) German Cancer Research Center Im Neuenheimer Feld 460 69120 Heidelberg Phone: +49 6221 56 5230 [email protected] As part of our interventions studies among hematopoietic stemcell transplantation patients we demonstrated that physical exercise significantly reduced cancer-related fatigue (Wiskemann et al. 2011, Blood). The division of Preventive Oncology reduces the burden of cancer by conducting cuttingedge research in three areas, (a) primary prevention (identification of risk factors and biologic mechanisms), (b) secondary prevention (early detection and screening), and tertiary prevention (improving clinical outcomes of cancer patients). Using state-of-the-art methods, including coordinated -omic strategies in high quality observational and intervention studies, we explore molecular pathways of risk and clinical outcome. Targets are high-impact areas including energy balance/adipose-tissue/metabolic syndrome, inflammatory/immune-modulatory processes, and lifestyle/microbial communities. Pioneering work focuses on genetically-targeted, personalized prevention strategies through highly effective nonsteroidal anti-inflammatory drugs. We collaborate closely with many colleagues at the Heidelberg University Clinic to define novel predictive and prognostic markers among cancer patients and to discern health behaviors with major impact on cancer prognosis. In uniquely designed clinical trials we test exercise as an adjuvant therapy in cancer and directly translate our findings into the clinic and population. Among other research initiatives, we lead the interdisciplinary ColoCare Study in Heidelberg as part of an international consortium with the Fred Hutchinson Cancer Research Center in Seattle and the Moffitt Cancer Center in Tampa. The study builds on a cohort of colorectal cancer patients and has as its main aim the improvement of prognosis among colorectal cancer patients through modifiable health behaviors as well as molecularly tailored therapies. analysis. Our approach is interdisciplinary in collaborating extensively with other groups and consortia. One particularly interesting new research area addresses the obesity epidemic, its impact on inflammatory processes and, in consequence, on cancer development. In a large cohort of colorectal cancer patients, we will address this topic on multiple interrelated levels: We will investigate the influence of gene-expression and proteome patterns of tumor-adjacent adipose tissue on the molecular characteristics of colorectal tumors, with a special focus on inflammation and angiogenesis. Clinicopathological and molecular tumor characteristics are investigated in relation to the patients’ systemic status of inflammation and oxidative damage, and to physiologic characteristics (e.g., amount, type, and distribution of body fat) and to health behaviors (e.g., exercise training/sedentariness, and sun exposure). Through these integrated, interdisciplinary investigations, we expect to gain novel insights into molecular pathways. By identifying in these multilevel investigations the factors that matter most in cancer progression, we can derive the most effective, targeted prevention strategies. ESSENTIAL PUBLICATIONS: (1.) Ulrich C.M. et al. (2007). Non-steroidal anti-inflammatory drugs for cancer prevention: promise, perils and pharmacogenetics. Nature Reviews Cancer, 6, 130–140. (2.) Pierce B.L. et al. (2009). Elevated biomarkers of inflammation are associated with reduced survival among breast cancer patients. Journal of Clinical Oncology, 27, 3437–3444. (3.) Imayama I. et al. (2012). Effects of a caloric re- Future Outlook: The most important goals of our division are to advance cancer prevention by identifying molecular mechanisms and developing strategies for personalized cancer prevention. In addition, we strive to develop evidence-based guidelines on health behavior interventions after cancer diagnosis. We apply state-of-the art methods in epidemiologic studies, devising new strategies for the statistical pathway 124 Research Program striction weight loss diet and exercise on inflammatory biomarkers in overweight/obese postmenopausal women: a randomized controlled trial. Cancer Res, 72, 2314–2326. (4.) Miller J.W. and Ulrich C.M. (2013). Folic acid and cancer – where are we today? The Lancet, 381, 1029– 1036. Translational Cancer Research Cellular and Molecular Pathology Division Head: Prof. Dr. Hermann-Josef Gröne The division performs research into the cellular and molecular mechanisms underlying rejection reactions in malignant tumors and transplanted solid organs. Rejection reactions are regularly mounted by the organism to defend itself against tumors. Using organ transplants as animal models we can observe the course and characteristics of rejection under defined conditions. Our interest is focused on monocytes/macrophages – inflammationpromoting immune cells of the recipient – and their main target, the endothelial cells lining the inside of the blood vessels of donor organs. Two main groups of substances are studied with regard to the function of monocytes/ macrophages, of endothelia and of parenchymal or tumor cells in rejection: lipid-activated nuclear receptors and glycosphingolipids (GSL). Our goal is to gain a better understanding of the processes underlying tissue rejection and to transfer these findings to tumor rejection. This may lead to novel diagnostic methods and treatment relating to tumor rejection. The division is also concerned with clinical surgical pathology and has established a reference center for renal diseases. Additionally, the department provides a service for histophathology of tissue samples, including tissues from animal experiments. The department is funded by the DFG (German Research Foundation) for specific projects and is part of concerted research activities of the DFG. tion, mainly by an effect on macrophages. By use of specific synthetic ligands and gene knock out mice we are analyzing the cellular and molecular pathways by which these transcription factors influence chronic fibrosing inflammation. Sphingolipids and glycosphingolipids: Membranes of all mammalian cells contain - in addition to phosphoglycerolipids and cholesterol-sphingolipids: i.e. sphingomyelins (SM) and glycosphingolipids. These sphingolipids are expressed in a cell type- and differentiation stage- specific manner. GSL influence neuronal, metabolic and immune functions. Interactions between glycoproteins and GSLs are pivotal to stabilize the brain and protect it against immune reactions. We have shown in a cell specific ganglioside-deficient animal that GSL are needed for an orderly differentiation of non immune cells and T-lymphocytes. We are currently using inducible cell specific knock outs of GSL to further define the differentiation- and immune-activity of GSL. ESSENTIAL PUBLICATIONS: (1.) Jennemann R, Gröne HJ. (2013). Cell-specific in vivo functions of glycosphingolipids: lessons from genet- Cellular and Molecular Pathology (G130) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 4350 [email protected] ic deletions of enzymes involved in glycosphingolipid synthesis. Prog Lipid Res. 52, 231–248. (2.) Stettner P. et al. (2013). Sulfatides are required for renal adaptation to chronic metabolic acidosis. Proc Natl Acad Sci U S A. 110, 9998–10003. (3.) Nordström V. et al. (2013). Neuronal expression of glucosylceramide synthase in central nervous system Future Outlook: Lipid-dependent transcription factors: Nonsteroid nuclear receptors such as retinoic acid receptors (RARs), are activated by lipid ligands; they have highly significant and long lasting effects on lipid and carbohydrate metabolism and on the immune system. We have been able to show that RAR- and LXR-receptors can potently inhibit chronic fibrosing inflamma- regulates body weight and energy homeostasis. PLoS Biol. 2013;11(3):e1001506. (4.) Traykova-Brauch M. et al. (2008). An efficient and versatile system for acute and chronic modulation of renal tubular function in transgenic mice. Nat. Med., 14, 979–984. Neurons, isolated from hippocampus. Neurons lacking GSLs show reduced dendritic processes and early pruning (right slide). Research at DKFZ 2014 125 Translational Cancer Research Molecular Tumor Pathology Clinical Cooperation Unit Head: Prof. Dr. Wilfried Roth Molecular Tumor Pathology (G150) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 56 4174 [email protected] Our group is located both at the DKFZ and the Institute of Pathology at University Hospital Heidelberg. Our cooperative unit aims at bringing together basic cancer research and clinical medicine. In this regard, the translational research is focussed on the primary human cancer tissue. We are specifically interested in the molecular mechanisms of therapy resistance in malignant tumors. Defects in the intracellular signaling cascades resulting in cell death are responsible for the therapy resistance in many types of cancer. Our research is focussed on the molecular mechanisms which allow tumor cells to evade apoptotic or non-apoptotic cell death. The identification of these resistance mechanisms is a prerequisite for the development of novel, effective therapy approaches and contributes to a better understanding of the molecular basis of therapy resistance in colon cancer, urological tumors, and malignant brain tumors. The second area of research is the identification of prognostic and predictive tumor markers. Due to their central biological relevance, cell death-regulating proteins are decisive for the therapy response in cancer. Therefore, we study the expression of cell death-regulating proteins in the primary human cancer tissue to identify tumor markers. This predictive approach in molecular pathology aims at the identification of biomarkers which is required for the development of individualized therapeutic approaches for cancer patients. Future Outlook: Regarding our first research area, the mechanisms of therapy resistance in cancer, we are working on the following projects: • Functional characterization of a novel type of cell death: giant mitochondriaassociated cytotoxicity by the HMGB1 protein. • Role of Bcl-2 family proteins for the resistance to cell death in colon carcinomas. • Apoptosis resistance by the stem cell factor Notch in glioblastomas. • Regulation of cell death by miRNAs. • Mechanisms of therapy resistance in renal cell carcinomas mediated by defects in the mTOR signaling pathway. • Functional relevance of alternative types of cell death for therapy resistance: necrosis and autophagy. Regarding our second research area, the identification of tumor markers, we will focus on the following projects: • Prognostic relevance of death ligands and death receptors in renal cancer. • Expression and prognostic relevance of apoptosis-regulating proteins in colon cancer. • G proteins as novel biomarkers in malignant brain tumors. ESSENTIAL PUBLICATIONS: (1.) Gdynia G. et al. (2010). Danger signaling protein HMGB1 induces a distinct form of cell death accompanied by formation of giant mitochondria. Cancer Research, 70, 8558–8568. (2.) Böck B.C. et al. (2010). The PEA-15 protein regulates autophagy via activation of JNK. J Biol Chem, 285, 21644–21654. (3.) Macher-Goeppinger S. et al. (2009). Prognostic value of Tumor Necrosis Factor-Related Apoptosis-inducing ligand (TRAIL) and TRAIL receptors in renal cell cancer. Clinical Cancer Research, 15, 650–659. (4.) Tagscherer K.E. et al. (2008). Apoptosis-based Electron microscopy of a cancer cell: Formation of giant mitochondria during the process of a specialized form of cell death. 126 Research Program treatment of glioblastoma with ABT-737, a novel small molecule inhibitor of Bcl-2 family proteins. Oncogene, 27, 6646–6656. Translational Cancer Research Dermato-Oncology Clinical Cooperation Unit Head: Prof. Dr. Jochen Utikal The Clinical Cooperation Unit “Dermato-Oncology” is engaged in the prevention, diagnosis, and therapy of skin tumors. Research results obtained are transferred directly into clinical practice. The main focus is malignant melanoma, a tumor that originates from the pigment cells of the skin. The Clinical Cooperation Unit “Dermato-Oncology” conducts several translational research projects including different Phase I–IV clinical trials with innovative melanoma therapies such as BRAF/MEK inhibition and anti-PD1 therapy. Basic science researchers at the department work on similarities of tumor cells such as melanoma cells and embryonic stem cells; on immunosuppressive mechanisms in tumors; on chronic inflammation and its impact on tumor development and progression; and on novel biomarkers for malignant melanoma. The Clinical Cooperation Unit Dermato-Oncology is part of the Research Program Translational Cancer Research and is associated with the Program Tumor Immunology. Future Outlook: The Clinical Cooperation Unit Dermato-Oncology will be engaged in the prevention, diagnosis and therapy of skin tumors, such as the malignant melanoma. Also, different clinical trials to improve the therapeutic options for the treatment of this tumor type will be conducted. In future an additional major focus of the department will be stem cell research. Embryonic stem cells and tumor cells have many aspects in common, including immortal cell growth and the potential of forming tumors. Furthermore, melanoma cells can be transformed via ectopic expression of these transcription factors into a pluripotent state. The mechanism behind this plasticity will be studied. In addition, we plan to study the reaction of the immune system towards the plasticity of different melanoma subpopulations. Accordingly, immune cells, such as myeloid derived suppressor cells, regulatory T cells and tolerogenic dendritic cells, will be studied in human melanoma lesions and our ret transgenic mouse melanoma model. Metabolic and signaling pathways in immunosuppressive cells, responsible for the production of mediators blocking anti-tumor activity of effector and memory T cells, will also be examined. Dermato-Oncology (G300) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 621 383 4461 [email protected] ESSENTIAL PUBLICATIONS: (1.) Utikal J. et al. (2009). Immortalization eliminates a roadblock during the reprogramming of somatic cells into iPS cells. Nature., 460, 1145–1148. (2.) Utikal J. et al. (2009). Sox2 is dispensable for the reprogramming of melanocytes and melanoma cells into induced pluripotent stem cells. J Cell Sci., 122, 3502–3510. (3.) Meyer C. et al. (2011). Chronic inflammation promotes myeloid-derived suppressor cell activation blocking antitumor immunity in transgenic mouse melanoma model. Proc Natl Acad Sci U S A.; 108, 17111– 17116. (4.) Flaherty K.T. et al. (2012). Improved Survival with MEK Inhibition in BRAF-Mutated Melanoma. N Engl J Med, 367, 107–114. Primary malignant melanoma Research at DKFZ 2014 127 Translational Cancer Research Molecular Hematology/Oncology Clinical Cooperation Unit Head: Prof. Dr. Alwin Krämer Molecular Hematology/Oncology (G330) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 1440 [email protected] 128 Numerical and structural chromosomal alterations and chromosomal instability are common features of human malignancies. In addition, intratumoral genetic heterogeneity and clonal evolution are major contributors to disease progression, relapse and treatment resistance. Despite chromosomal instability appears to be a major cause of tumor development and progression, only little is known about its molecular origins. The Clinical Cooperation Unit Molecular Hematology/Oncology is studying the molecular mechanisms responsible for the induction of chromosomal instability and clonal evolution in malignant neoplasias. One reseach topic focuses on causes and consequences of amplified centrosomes – the spindle pole organizers responsible for correct chromosome segregation during mitosis – in human malignancies. Another current topic centers around whole-genome sequencing approaches, aiming at the identification of mutations responsible for chromosomal instability in human acute myeloid leukemias with complex aberrant karyotypes and extremely poor prognosis. and induces myeloid leukemias via amplification of centrosomes. In collaboration with the Schiebel group from ZMBH it was shown that EGFR signaling impacts on centrosome separation and thereby mitotic progression and rates of chromosome missegregation. In addition, whole-genome siRNA screening enabled the group to identify the mechanisms leading to clustering of supernumerary centrosomes into two functional spindle poles in cancer cells and thereafter to target centrosomal clustering as a novel anti-cancer strategy. Small molecule screening led to the identification of compounds that inhibit centrosomal clustering and selectively kill cancer cells with supernumerary centrosomes. Generally, the aim of the department’s research is to better understand the processes leading to chromosomal instability and, consequently, to tumor development and progression. A further goal is to exploit the results of this work for establishing new ways of tumor classification and treatment. ESSENTIAL PUBLICATIONS: (1.) Bochtler T. et al. (2013). Clonal heterogeneity as de- As major contributions, the department has shown that both chromosomal instability and clonal evolution is associated with disease progression and poor prognosis in myeloid malignancies. Mechanistically, novel components of the centrosome replication machinery have been identified and mechanisms of normal centrosome replication and centrosome amplification in cancer cells and after DNA damage have been elucidated. Also, researchers from the group together with the Translational Oncology department (von Kalle) have demonstrated that activation of the transcription factor EVI1 causes chromosomal instability Research Program tected by metaphase karyotyping is an indicator of poor prognosis in acute myeloid leukemia. J. Clin. Oncol., 31, 3898–3905. (2.) Mardin B.R. et al. (2013). EGF induced centrosome separation promotes mitotic progression and cell survival. Dev. Cell, 25, 229–240. (3.) Leber B. et al. (2010). Proteins required for centrosome clustering in cancer cells. Sci. Transl. Med., 2, 33ra38. (4.) Stein S. et al. (2010). Genomic instability and myelodysplasia with monosomy 7 consequent to EVI1 activation after gene therapy for chronic granulomatous disease. Nat. Med., 16, 198–204. Research at DKFZ 2014 Multipolar cell division 129 Translational Cancer Research Pediatric Oncology Clinical Cooperation Unit Head: Prof. Dr. Olaf Witt The goal of the Clinical Cooperation Unit (CCU) Pediatric Oncology is to advance the therapy for children and adolescents with neural cancers. Since epigenetic regulation of gene expression is a key mechanism in stem cell biology, differentiation and development, it is likely that aberrant epigenetic programs play a particular role in the genesis and progression of undifferentiated pediatric cancers. Epigenetic programs are reversibly controlled by an array of enzymes, including the family of histone deacetylases (HDACs). Understanding the molecular biology and selective targeting of individual HDACs of pediatric neural cancer cells, including cancer stem cells, is one of the central molecular concepts of the CCU Pediatric Oncology. Our research groups headed by Ina Oehme, Till Milde and Hedwig Deubzer have identified particular HDAC family members controlling differentiation, cell survival mechanisms, developmental pathways and self renewal in neuroblastoma and brain tumors. As a consequence, we are now developing small molecule compounds specifically inhibiting distinct HDACs for therapeutic purposes in collaboration with pharma partners. A second research focus concerns the development of individualized, molecular based targeted treatment concepts from patient to bench and back. Finally, we translate our experimental findings into clinical practice through development of individual targeted treatment protocols for children and adolescents with relapsed cancers, as well as conducting phase I-III clinical trials in pediatric oncology based on rational molecular concepts. To this end, we have developed and are conducting a Phase I/ II trial with the HDAC inhibitor Vorinostat in relapsed pediatric cancers and have initiated a first nationwide clinical trial for personalized oncology in paediatrics (INFORM) together with cooperating partners from DKFZ and NCT. Pediatric Oncology (G340) German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 3570 [email protected] HDAC family members control hallmarks of pediatric neuronal cancers. anchorage independent growth HDAC8 HDACx developmental pathways pediatric cancer cell HDAC8 HDAC5 HDAC9 differentiation HDAC2 resistance to chemotherapy HDAC1 HDACx HDAC1 HDAC8 self renewal proliferation ESSENTIAL PUBLICATIONS: (1.) Oehme I. et al. (2013). Histone deacetylase 10 promotes autophagy-mediated cell survival. Proc Natl Acad Sci U S A.,110, E2592–601. (2.) Lodrini M. et al. (2013). MYCN and HDAC2 cooperate to repress miR-183 signaling in neuroblastoma. Nucleic Acids Res., 41, 6018–33. (3.) Milde T. et al. (2011). A novel human high-risk ependymoma stem cell model reveals the differentiation-inducing potential of the histone deacetylase inhibitor Vorinostat. Acta Neuropathol. 122, 637–650. (4.) Milde T. et al. (2012). HDAC5 and HDAC9 in medulloblastoma: novel markers for risk stratification and role in tumor cell growth. Clin Cancer Res. 16, 3240– 3252. apoptosis 130 Future Outlook: 1. Drug target validation: We will define the tumor biological function of individual HDACs with respect to regulation of the human acetylome and downstream pathways in pediatric neuronal cancers. To this end, we will include primary tumor material, cancer stem cell and animal models in our projects. This will facilitate the identification of potential biomarkers for treatment response prediction and establish the basis for patient selection in future trials involving selective HDAC inhibitors. 2. Drug development: We will pursue the development of selective small molecule HDAC-inhibitors towards phase I clinical trials. In addition, we aim for identification of synthetic lethal interacting pathways cooperating with selective HDAC inhibitors to facilitate rational combination therapies in the future. 3. Disease models: We will extend our primary tumor model bank for pediatric neuronal cancers. We will evaluate individualized targeted treatment concepts using primary brain tumor models and integrative genomic approaches. 4. Clinical trials: We will continue to expand our early phase I and II clinical trial efforts in pediatric oncology as well as conducting international phase III trials in low grade gliomas in children. Research Program Translational Cancer Research Molecular Oncology of Solid Tumors Clinical Cooperation Unit Head: Prof. Dr. Dr. Heike Allgayer In general, the group under Heike Allgayer focuses on key mechanisms driving metastasis, especially tumor-associated proteases and micro RNAs, and their translational relevance. They discovered major regulatory mechanisms of the urokinase receptor (u-PAR) and resulting molecular staging models. The group identified Cetuximab as a metastasis inhibitor, u-PAR being a novel biomarker of Cetuximab sensitivity. The group also implicated for the first time the anti-malaria agent Artesunate as a metastasis inhibitor, acting via u-PA/MMPs. Furthermore, the group pioneered Pdcd4 in its function as a novel metastasis suppressor by regulating u-PAR, and as an independent prognostic marker, which they showed to be essentially downregulated in cancer by microRNA-21. Recently, the Allgayer group extended their focus on microRNAs and metastasis. For the first time they described microRNA-21 post-transcriptionally downregulating Pdcd4 and stimulating three different steps of the metastastic cascade; a work currently cited more than 600 times since its publication. The group also implicated other microRNAs as novel regulators of metastasis, e.g. miR-200c, miR-34a, or the miR-30-family. Recently, within a DKFZ-MOST project, they suggested a metastatically critical network of miR-21, miR-34a, Pdcd4, Src, and PTEN. Current work suggests several novel miRs to be significantly deregulated in a systematic profiling approach of resected colorectal patient metastasis tissue. From these, the group functionally concluded a molecular network of miRs and their partly common targets which all culminate in EMT-regulation, representing a metastatically critical miR-network (in preparation for publication). tasizing to a particular organ regardless of the primary tumor type (“site-specific metastasis”). These projects will help us essentially to characterize the metastatically relevant cancer cell. Furthermore, we will continue with functional projects on novel miRs which we have detected in resected patient metastasis tissues and characterize those molecular targets and pathways enabling them to act as metastasis regulators. This will be strongly supported by head-to-head comparison with novel miRs indicated by microRNAs implicated in zebrafish and diverse mouse models of collaborators. Current activities on resected inflammatory and resulting colon cancer tissue of patients with Morbus Crohn or ulcerative colitis will look at miRs specifically relevant for colon carcinogenesis and metastasis arising from a chronic inflammatory background. Finally, in recently funded collaborations we will screen larger series of colorectal cancer patients prospectively for the expression of metastasisrelevant miRs identified by us, supporting the development of novel biomarkers and targets out of the miR metastasis field. Finally, Heike Allgayer has just established and coordinates a DKFZ-Metastasis Research Group (MRG) to combine forces accelerating innovative and high-risk projects in the essential, yet underrepresented, field of metastasis research. The group includes essential PIs of DKFZ and NCT. ESSENTIAL PUBLICATIONS: Molecular Oncology of Solid Tumors (G360) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 621 383 2226 [email protected] and Dept. of Experimental Surgery, Medical Faculty Mannheim, Ruprecht Karls University Heidelberg (1.) Asangani I.A. et al. (2009). MicroRNA-21 (miR-21) post-transcriptionally downregulates tumor suppressor Pdcd4 and stimulates invasion, intravasation and metastasis in colorectal cancer. Oncogene, 27, 2128– 2136. Future Outlook: The group under Heike Allgayer has initiated and rapidly advanced comparison of resected metastases against primary tumor- and normal tissues of gastrointestinal cancer patients using expression profiling and microRNA profiling, but also deep sequencing and especially genome sequencing. Further tumor entities will now be added to investigate tumor-type independence of essential (miR-driven) molecular networks found; seeking to suggest additional molecular pathways essential for metas- Research at DKFZ 2014 (2.) Nikolova D. et al. (2009). Cetuximab attenuates metastasis and u-PAR expression in non-small cell lung cancer: u-PAR and E-cadherin are novel biomarkers of cetuximab sensitivity. Cancer Res., 69, 2461–2470. (3.) Mudduluru G. et al. (2011). Regulation of Axl receptor tyrosine kinase expression by miR-34a and miR-199a/b in solid cancer. Oncogene, 30, 2888–2899. (4.) Rasheed SAK. et al.(2010). First evidence that the antimalarial drug artesunate inhibits invasion and in vivo metastasis in lung cancer by targeting essential extracellular proteases. Int. J. Cancer, 127, 1475–1485. Chicken chorioallantoic membrane (CAM) assay: Primary tumor in the upper CAM. 131 Translational Cancer Research Molecular Oncology of Gastrointestinal Tumors Division Head: Prof. Dr. Rienk Offringa Molecular Oncology of Gastrointestinal Tumors (G180) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 3140 [email protected] The Division Molecular Oncology of Gastrointestinal Cancers was founded in 2011 with support from the KH Bauer Foundation. The decision to direct research efforts to pancreatic cancer was based on the urgent unmet medical need this disease represents, with incidence and mortality rates still being almost equal, and the fact that Heidelberg University hosts the European Pancreas Center, one of the world’s leading clinics for the treatment of pancreatic cancer. Our research aims at the implementation of immunotherapy in conjunction with surgery, chemotherapy and/or small molecule inhibitors. The choice for immunotherapy was inspired by recent successes with this approach for other cancers in the clinic, as well as emerging pre-clinical evidence that redirection of immune pathways is one of the most promising avenues towards more effective non-surgical treatment of pancreatic cancer. Our therapeutic strategy primarily involves two approaches: • Stimulation of the endogenous immune potential, in particular in the tumor stroma, by means of agonist immunostimulatory monoclonal antibodies • Exploitation of the most powerful mode of immunotherapy: infusion of ex vivo engineered autologous T-lymphocytes Patient-based research is supported by the excellent availability of patient biopsies, including the tissue that represents the interface between tumor and immune system: tumordraining lymph nodes. Our research in mice focuses on genetically engineered, autochthonous tumor models. Future Outlook: It is essential that our research does not stop at the threshold between lab and clinic. This is why we, together with our partners in the University Hospital and at the National Center for Tumor Diseases (NCT) Heidelberg, are setting up a pipeline for rationally designed clinical trials in pancreatic cancer. Biomarker research constitutes a pivotal aspect of this rational design, both with respect to patient stratification and evaluation of therapy efficacy. Our studies with agonist immunostimulatory antibodies will involve neo-adjuvant studies in patients with primary resectable or locally advanced disease, because this setting features a sufficiently long time window for these drugs to mobilize the patient’s endogenous immune response. Moreover, this allows analysis of treatment impact in the tumor microenvironment. These studies will be performed in the context of the EU-funded network program IACT (Immunostimulatory Agonist antibodies for Cancer Treatment) coordinated by our division. The trials involving T-cell infusion will be staged in patients with recurrent disease after primary tumor resection, because at this stage a faster acting, ready-to-go army of immune cells will be required to effectively combat the tumor. ESSENTIAL PUBLICATIONS: (1.) Oliveira C.C. et al. (2010). The nonpolymorphic MHC Qa-1b mediates CD8+ T cell surveillance of antigen-processing defects. J Exp Med, 207, 207–221. (2.) Offringa R. (2009). Antigen choice in adoptive Tcell therapy of cancer. Curr Opin Immunol, 21, 190–199. (3.) Bos R. et al. (2008). Balancing between antitumor efficacy and autoimmune pathology in T-cell-mediated targeting of carcinoembryonic antigen. Cancer Res, 68, 8446–8455. (4.) van Hall T et al. (2006). Selective cytotoxic T-lymphocyte targeting of tumor immune escape variants. Nat Med, 12, 417–424. 132 Research Program T-cells Tumor fragment Tumor–infiltrating lymphocytes (TILs) are a good source of tumor-reactive T-cells. Although their activity is restrained by the tumor microenvironment, these T-cells can be effectively re-activated and expanded in vitro, also in the case of pancreatic ductal adenocarcinoma (see microscopic image; I. Poschke & J. Hermes). This offers a promising perspective for the development of adoptive Research at DKFZ 2014T-cell therapy for this disease (see inset). 133 Translational Cancer Research Neurooncology Clinical Cooperation Unit Head: Prof. Dr. Wolfgang Wick Neurooncology (G370) Department of Neurooncology Heidelberg University Hospital and National Center for Tumor Diseases Heidelberg Im Neuenheimer Feld 400 69120 Heidelberg Phone: +49 6221 56 7075 Fax: +49 6221 56 7554 [email protected] The clinically oriented research focusses on the development of diagnostic, prognostic and predictive biomarkers in anaplastic glioma and glioblastoma. This research is done in collaboration with the Epigenetics group at the DKFZ, funded by the Federal Ministry of Education and Research (BMBF) and building on two larger randomized trials, which have been coordinated from the clinical neurooncology unit. A second focus is on unravelling the molecular mechanisms of several targeted therapies in glioblastoma, like the protein kinase C beta inhibitor, enzastaurin, the mammalian target of rapamycin inhibitor, temsirolimus and the soluble CD95, APG101 plus the understanding of the interaction between these therapies and radiation. In an ongoing effort, the group is aiming at developing normal hematopoietic stem cells into therapeutic vehicles. The challenges and interactions here are the molecular mechanisms of specific lesions-tropisms as well as the implementation of a safe, clinically useful lentiviral transduction system. With a specific focus on vascular endothelial growth factor receptor 2 and regulator of G protein signaling 4, the group seeks to understand the fundamental principles of evasive resistance against the classical anti-angiogenic agents and, with modification, in radiation therapy. Ultimately, the research in the Clinical Cooperation Unit (CCU) Neurooncology should focus on problems derived from the clinical Neurooncology Program, with the clear aim to translate the results back into the clinic. tumors. Currently, one such predictive marker for anaplastic glioma is under research. Using a similar approach, a study cohort of elderly patients with malignant glioma will be characterized for differential methylation patterns compared to the standard malignant glioma in middle-aged patients aiding the understanding of the comparatively worse prognosis. From this and other research on targeted therapies, new molecules and ultimately, points for intervention are to be developed. Here, the focus is on small molecule screens and compound development. With the establishment of a new group on multiphoton-microscopy in the CCU, the core field of angiogenesis and brain metastases will be strengthened. The focus of this group is to understand the mode of action of anti-angiogenic therapies in the brain and to elucidate the specific properties of cancer cells that successfully establish brain metastases. As with other projects, the group is strongly linked to the CCU Neuropathology and the experimental imaging departments at both the Head Clinic and the DKFZ. This will be of utmost importance for the transfer of research results to the clinic. ESSENTIAL PUBLICATIONS: (1.) Wick W. et al. (2009). NOA-04 Randomized Phase III Trial of Sequential Radiochemotherapy of Anaplastic Glioma With PCV or Temozolomide. J. Clin. Oncol., 27, 5874–5880. (2.) Wick W. et al. (2012). Temozolomide chemotherapy alone versus radiotherapy alone for malignant astrocytoma in the elderly: the NOA-08 randomised, phase Future Outlook: Given a new biomarker, which optimally would be sufficient to guide therapy decisions, this will be characterized, developed and explored for its potential in diseases other than brain 3 trial. Lancet Oncol. 13, 707–715. (3.) Berger B. et al. (2010) Defective p53 antiangiogenic signaling in glioblastoma. Neuro-Oncol, 12, 894– 907. (4.) Wick A. et al. (2011) Bevacizumab does not increase the risk of remote relapse in malignant glioma. Ann Neurol, 69, 586–592. Blood vessel morphology and function imaged by in vivo MPLSM. 134 Research Program Translational Cancer Research Neuropathology Clinical Cooperation Unit Head: Prof. Dr. Andreas von Deimling The Clinical Cooperation Unit Neuropathology was founded in 2007. Our research focuses on molecular genetics of pediatric and adult tumors of the central nervous system, the function of neurofibromin, and the molecular reference analysis for brain tumor studies. Prof. A. Korshunov examines pediatric brain tumors in close cooperation with other groups from the DKFZ, with a focus on medulloblastomas, pilocytic astrocytomas and ependymomas. We are participating in the International Cancer Genome Consortium (ICGC). For adult gliomas our main interest is in diffuse astroand oligodendroglial tumors characterized by IDH1 mutations. Dr. D. Capper and F. Sahm are characterizing this and other mutations and are developing diagnostic tools for routine applications. Dr. S. Pusch and Dr. J. Balss are conducting research on the function of mutated IDH1. The tumor syndrome neurofibromatosis type 1 is caused by mutations of the NF1 gene which encodes neurofibromin. Many biological features of neurofibromin are mediated by its RasGAP activity. However, additional functions have been suggested. A group headed by Dr. D. Reuss is uncovering alternative pathways of neurofibromin to inhibit tumor cell growth. Our molecular diagnostic program is headed by Prof. C. Hartmann and serves multiple clinical studies by providing data such as mutational status of tumor suppressor genes or oncogenes. Our clinical partners compare these data with clinical parameters. Future Outlook: We will contribute to genomic analyses of medulloblastoma and pilocytic astrocytoma within the ICGC: Acquisition of high-quality tumor and matched germline samples according to ICGC guidelines; histopathological assessment; acquisition of clinical data and follow-up information and molecular characterization of samples using previously proposed diagnostic and prognostic markers. In cooperation with DKFZ partners, we have designed a conditional knock-in mouse model for the IDH1-R132H mutation. We will attempt to create mutant IDH1 driven mouse brain tumor models. This likely will require combination with other tumorigenic alterations such as TP53 mutations and tissue specific expression at different times of development. Future tasks within the NF1 project are to verify our results from cellular models in animal models and to extend our understanding of potential alternative NF1 pathways. We will use well characterized NF1 mouse models in which mice develop multiple neurofibromas closely resembling human disease. In our molecular diagnostic program we attempt to meet the growing demand from our clinical partners within the DKFZ as well as from multicenter studies. We are prepared to adapt our molecular diagnostic assays to the needs of individual study protocols. Neuropathology (G380) German Cancer Research Center Im Neuenheimer Feld 220 69120 Heidelberg Phone: +49 6221 56 4650 [email protected] ESSENTIAL PUBLICATIONS: (1.) Balss J. et al. (2008). Analysis of the IDH1 codon 132 mutation in brain tumors. Acta Neuropathol., 116, 597–602. (2.) Capper D. et al. (2009). Monoclonal Antibody Specific for IDH1 R132H Mutation. Acta Neuropathol., 118, 599–601. (3.) Korshunov A. (2010). Molecular staging of intracranial ependymoma in children and adults. J. Clin. Oncol., 28, 3182–3190. (4.) Hartmann C. et al. (2010). Patients with IDH1 wild type anaplastic astrocytomas exhibit worse prognosis than IDH1 mutated glioblastomas and IDH1 mutation status accounts for the unfavorable prognostic effect of higher age: implications for classification of gliomas. Acta Neuropathol., 120, 707–718. Research at DKFZ 2014 Example for development of a diagnostic tool. Our antibody H09 specifically binds to IDH1 protein with the R132H mutation. All tumor cells impose in a strong brown color while normal brain tissue is stained blue and grey. 135 Translational Cancer Research Neuroimmunology and Brain Tumor Immunology Clinical Cooperation Unit Head: Prof. Dr. Michael Platten Experimental Neuroimmunology (G160) Department of Neurooncology Heidelberg University Hospital Im Neuenheimer Feld 400 D-69120 Heidelberg Phone: +49 6221 56 7107 Fax: +49 6221 56 5935 [email protected] A paradigmatic autoimmune disease of the central nervous system (CNS) is multiple sclerosis. On the other hand a hallmark of intrinsic CNS tumors is profound systemic and local immunosuppression. The cellular and molecular mechanisms that are involved in the deregulation of CNS immunity in these diseases are incompletely understood, but probably involve pathways common to both: too much immune response in multiple sclerosis and too little immune response in brain tumors. Our group is interested in the metabolic control of CNS immunity and brain tumor development. The long-term goal is to identify crucial metabolic switches that may serve as therapeutic targets. In the past years we have identified key steps in the catabolism of the essential amino acid tryptophan as an endogenous mechanism, restricting unwanted immune responses. These discoveries have led to the identification of novel therapeutic approaches and diagnostic tools that are currently undergoing clinical evaluation. Recently, we have identified a key receptor of tryptophan catabolites that not only mediates tumor-promoting host cell interactions, but also tumor cell intrinsic mechanisms to sustain tumor growth and invasiveness. These recent discoveries open a new view of the role of tryptophan catabolism in cancer and identify novel therapeutic targets. probably other types of cancer, via the aryl hydrocarbon receptor (AHR) raises further questions which will be tackled in the future. This is especially important as tryptophan catabolism has evolved in recent years as a key metabolic pathway in cancer biology and immune regulation, and early clinical trials in cancer patients start to employ pharmacological inhibitors. Besides translational projects aiming at the identification of novel drugs interfering with this pathway, future basic science projects aim at elucidating the immunological consequences of this metabolic pathway in multiple sclerosis and brain tumors at cellular and molecular levels using novel transgenic animal models. In parallel, novel vaccination strategies for gliomas will be developed involving mutated antigens using humanized mouse models. Based on patented work on successful clinical application, a phase I/II clinical trial will be initiated in 2014. The long term goal is to combine therapeutic strategies to alleviate tumor-associated immune suppression with vaccination approaches against novel tumor antigens in brain tumors. The translational projects involve the Department of Neurooncology at University Hospital Heidelberg, the National Center for Tumor Diseases and collaborations with the Clinical Cooperation Units Neurooncology and Neuropathology. Future Outlook: The discovery that TDO-derived tryptophan catabolites (kynurenines) drives brain, and ESSENTIAL PUBLICATIONS: (1.) Opitz C.A. et al. (2009). Toll-like receptor engagement enhances the immunosuppressive properties of human bone marrow-derived mesenchymal stem cells by inducing indoleamine-2,3-dioxygenase-1 via Brain MRI scan of mice with brain tumors that catabolize tryptophan (+ TDO) compared with tumors that do not catabolize tryptophan (- TDO) and do not form large tumors. Activation of the immunosuppressive AHR-program (TiPARP) in an immune cell (LCA) infiltrating a tryptophan catabolizing tumor. 136 Research Program interferon-β and protein kinase R. Stem Cell, 27, 909– 919. (2.) Opitz C.A. et al. (2011). An endogenous tumourpromoting ligand of the human aryl hydrocarbon receptor. Nature, 478, 197–203. (3.) Sahm F. et al. (2013). The endogenous tryptophan metabolite and NAD+ precursor quinolinic acid confers resistance of gliomas to oxidative stress. Cancer Research, 73, 3225–3234. (4.) Lanz T.V. et al. (2013). Protein kinase Cβ as a therapeutic target stabilizing blood-brain barrier disruption in experimental autoimmune encephalomyelitis. PNAS, 110, 14735–14740. Translational Cancer Research Experimental Therapies for Hematologic Malignancies Max-Eder-Junior Research Group Head: Dr. Marc S. Raab Despite recent advances, most cancers of the blood and bone marrow remain incurable. Our group is therefore focused on understanding critical pathophysiological mechanisms of hematologic malignancies to enable the identification of innovative therapeutic targets and treatment strategies. Together with the Clinical Cooperation Unit Molecular Hematology/ Oncology (G330, Prof. A. Krämer), we are currently investigating the clustering of supernumerary centrosomes. This is a well-recognized cellular process on which cancer cell growth is dependent. We are therefore working to decipher the mechanism of centrosomal clustering in hematologic malignancies, with a view to the development of specific inhibitors to exploit this mechanism for therapeutic ends. In our model disease, multiple myeloma, we aim to discover molecular mechanisms of the pivotal transition from its premalignant precursor state to the active malignant stage, as well as on the pathogenesis of refractory disease. Here, we are focusing on the characterization of aberrant cell signaling and identification of corresponding genetic changes. We are also interested in the evaluation of novel agents, which inhibit cellular pathways known to be important in myeloma pathogenesis. This work is done in collaboration with our industry partners who provide promising compounds for assessment in our extensive pre-clinical models. We also participate in several national and international clinical trials, including first-in-man applications as well as first-in-class studies. Future Outlook: All our projects are aimed at the discovery of new therapeutic targets, investigating new treatment strategies, and ultimately, improving patient outcome. Our group has three major goals: • Develop novel therapeutic approaches based on centrosomal clustering: We aim to further develop our first lead compound towards clinical application and to screen for novel inhibitors of centrosomal clustering. • Discover key events in myeloma pathogenesis: We specifically focus on refractory disease with the aim to identify novel targets and therapeutic avenues that have not previously been explored, to individualize treatment for this group of patients with the highest unmet medical need. • Translate small molecule therapeutics from bench to clinical trials: This includes the evaluation of novel agents in the preclinical setting and the initiation of early phase clinical trials in hematologic malignancies, with a focus on personalized therapy for multiple myeloma. ESSENTIAL PUBLICATIONS: Experimental Therapies for Hematologic Malignancies (G170) German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg Phone: +49 6221 42 1450 [email protected] (1.) Andrulis M. et al. (2013). Targeting the BRAF V600E mutation in multiple myeloma. Cancer Discovery, 3, 862-869. (2.) Raab M.S. et al. (2012). GF-15, a novel inhibitor of centrosomal clustering, suppresses tumor cell growth in vitro and in vivo. Cancer Research, 72, 5374–5385. (3.) Raab M.S. et al. (2009). Multiple Myeloma. Lancet, 374, 324–339. (4.) Raab M.S. et al. (2009). Targeting PKC: A novel role for beta-catenin in ER stress and apoptotic signaling. Blood. 113, 1513–1521. Multipolar mitosis of a mouse xenograft under treatment with a prototype inhibitor of centrosomal clustering. Research at DKFZ 2014 137 Translational Cancer Research Molecular Mechanisms of Tumor Cell Invasion CHS Junior Research Group (in Cooperation with Heidelberg University) Head: Dr. Björn Tews Molecular Mechanisms of Tumor Cell Invasion (V077) CHS Research Group at CellNetworks Heidelberg University and DKFZ German Cancer Research Center Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 42 1570 [email protected] Glioblastoma is the most aggressive brain tumor with a poor prognosis, reflected by a median patient survival of about 14 months. The invasive nature of glioma cells mainly accounts for their resistance to current treatment modalities, as the diffusely infiltrating tumor cells, which evade surgical resection and survive treatment, inevitably give rise to reoccurring tumors. Substantial evidence has been accumulated to suggest that lysophospholipids are involved in tumorigenesis; they are especially important for therapeutic resistance of tumors by regulating tumor cell invasion. Interestingly, glioma cells use myelin as main trajectory routes, a substrate which normally restricts cell migration due to the presence of inhibitory proteins such as Nogo-A. We therefore investigate lysophospholipid G-protein coupled receptor(GPCR) signaling depending on different extracellular matrix environments. Furthermore, we determine the molecular basis for therapeutic sensitivity of gliomas. Recently, we could identify a key player for increased therapeutic sensitivity, Peroxiredoxin 1 (PRDX1). Loss of PRDX1 expression frequently occurs in 1p/19q-deleted oligodendrogliomas and contributes to chemosensitivity of these tumors. Our methodological repertoire includes modulation of GPCR expression and signaling; different in vitro bioassays to study cell migration and invasion such as organotypic slice cultures; Real-time Cell Analyses (RTCA); time-lapse microscopy; and in vivo mouse tumor models (RCAS/TVA; xenografts) with transgenically labeled tumor cells enabling light sheet microscopy imaging. Real-time Cell Analysis (RTCA) of cells overexpressing a wildtype (wt) or inactive (mut) form of a sphingolipid G-protein coupled receptor which negatively regulates cell adhesion and spreading on a CNS myelin substrate. Cell Index (CI) decribes a relative change in electrical impedance representing the morphological cell status. Data shown are mean values ± SEM. 138 Research Program Future Outlook: Understanding the complex lysophospholipid signaling cascades in glioma subtypes after different treatment regimens will provide important information to design new tailored therapies for patients. ESSENTIAL PUBLICATIONS: (1.)Tews B. et al. (2013). Synthetic microRNA-mediated downregulation of Nogo-A in transgenic rats reveals its role as regulator of synaptic plasticity and cognitive function. Proc Natl Acad Sci, 110, 6583– 6588. (2.) Dittmann L.M. et al. (2011). Downregulation of PRDX1 by promoter hypermethylation is frequent in 1p/19q-deleted oligodendroglial tumours and increases radio- and chemosensitivity of Hs683 glioma cells in vitro. Oncogene, 31, 3409–3418. (3.) Barbus S. et al. (2011). Differential retinoic acid signaling in tumors of long- and short-term glioblastoma survivors. J Natl Cancer Inst, 103, 598– 606. (4.) Tews B. et al. (2007). Hypermethylation and transcriptional downregulation of the CITED4 gene at 1p34.2 in oligodendroglial tumours with allelic losses on 1p and 19q. Oncogene, 26, 5010–5016. This Junior Research Group is generously supported by the Chica-and-Heinz-SchallerFoundation (CHS). Translational Cancer Research Neuropeptides CHS Junior Research Group (in Cooperation with Heidelberg University) Head: Dr. Valery Grinevich Our new laboratory will focus on the dissection of the mechanisms of neuropeptide action in the brain, from molecular – via anatomical – to the whole organism level. We will thus employ genetic, molecular, anatomical, viral, optogenetic and behavioral approaches to study the effects of “addressed” axonal release of various neuropeptides within the distinct brain regions controlling stress and fear responses, maternal and social behaviour. Furthermore, our group will use animal models of psychiatric diseases, including anxiety disorders and autism, to study the possible contribution of neuropeptides to the pathogenesis of the respective human diseases. ESSENTIAL PUBLICATIONS: (1.) Knobloch S. et al. (2012). Evoked axonal oxytocin release in the central amygdala attenuates fear response. Neuron, 73, 553–566. (2.) Liu Y. et al. (2010). Involvement of transducer of regulated cAMP response element-binding protein activity CREB activity on corticotropin releasing hormone transcription. Endocrinology, 151, 109–118. (3.) Grinevich V. et al. (2009). TgArc/Arg3.1-d4EGFP indicator mice: a versatile tool to study brain activity changes in vitro and in vivo. J. Neurosci. Meth. 184, 25–36. (4.) Grinevich V. et al. (2005). Monosynaptic pathway from rat vibrissa motor cortex to facial motor neurons revealed by lentivirus-based axonal tracing. J. Neurosci., 25, 8250–8258. This Junior Research Group is generously supported by the Chica-and-Heinz-SchallerFoundation (CHS). Neuropeptides (V078) German Cancer Research Center CHS Research Group at CellNetworks Heidelberg University and DKFZ Im Neuenheimer Feld 581 69120 Heidelberg Phone: +49 6221 486 174 [email protected] The image depicts virus-mediated cell-type specific fluorescent labeling of hypothalamic oxytocin neurons, as revealed by immunohistochemistry (green: Venus, red and blue: oxytocin and vasopressin-immunoreactivity, respectively), and represents the targets for oxytocin axons originating from the hypothalamic paraventricular nucleus in the rat forebrain. Image illustrated by Julia Kuhl. Research at DKFZ 2014 139 Join us! Index A Abdollahi, Dr. Dr. Amir 108 Allgayer, Prof. Dr. Dr. Heike 131 Angel, Prof. Dr. Peter 36 Arnold, Prof. Dr. Bernd 90 Augustin, Prof. Dr. Hellmut 42 B Beckhove, Prof. Dr. Philipp 88 Boulant, Dr. Steeve 119 Boutros, Prof. Dr. Michael 70 Brady, Dr. Nathan 74 Brenner, Prof. Dr. Hermann 84 Bukau, Prof. Dr. Bernd 45 Burwinkel, Prof. Dr. Barbara 85 C Cerwenka, PD Dr. Adelheid 93 D Debus, Prof. Dr. Dr. Jürgen 102 Delecluse, Prof. Dr. Dr. Henri-Jacques 116 de Villiers, Prof. Dr. Ethel-Michele 115 Dick, PD Dr. Tobias P. 40 Diederichs, Dr. Sven 73 E Kopka, Prof. Dr. Klaus 100 Kopp-Schneider, Prof. Dr. Annette 83 Krämer, Prof. Dr. Alwin 128 Krammer, Prof. Dr. Peter 89 Kyewski, Prof. Dr. Bruno 91 L Ladd, Prof. Dr. Mark E. 99 Langowski, Prof. Dr. Jörg 62 Lichter, Prof. Dr. Peter 65 Liu, Dr. Hai-Kun 53 Lyko, Prof. Dr. Frank 38 M Maier-Hein, Dr.-Ing. Lena 109 Martin-Villalba, Prof. Dr. Ana 46 Meinzer, Prof. Dr. Hans-Peter 105 Milsom, Dr. Michael 56 Monyer, Prof. Dr. Hannah 44 N Niehrs, Prof. Dr. Christof 35 O Offringa, Prof. Dr. Rienk 132 Oskarsson, Dr. Thordur 58 P Edgar, Prof. Dr. Bruce 43 Eils, Prof. Dr. Roland 68 Essers, Dr. Marieke 55 Pereira, Dr. Gislene 50 Pfister, Prof. Dr. Stefan 66 Plass, Prof. Dr. Christoph 80 Platten, Prof. Dr. Michael 136 F R Feuerer, Dr. Markus 94 Fischer, Dr. Andreas 54 Franke, Prof. Dr. Werner W. 48 Raab, Dr. Marc S. 137 Riemer, PD Dr. Dr. Angelika 117 Rodewald, Prof. Dr. Hans-Reimer 92 Rommelaere, Prof. Dr. Jean 112 Rösli, Dr. Christoph 57 Rösl, Prof. Dr. Frank 114 Roth, Prof. Dr. Wilfried 126 G Gissmann, Prof. Dr. Lutz 113 Grinevich, Dr. Valery 139 Gröne, Prof. Dr. Hermann-Josef 125 Grummt, Prof. Dr. Ingrid 47 H Haberkorn, Prof. Dr. Uwe 104 Hamacher-Brady, Dr. Anne 77 Hansman, Dr. Grant 118 Hell, Prof. Dr. Stefan 106 Hemminki, Prof. Dr. Kari 82 Herzig, Prof. Dr. Stephan 41 Höfer, Prof. Dr. Thomas 69 Hofmann, Dr. Thomas G. 52 Hoheisel, Dr. Jörg D. 67 Hombauer, Dr. Hans 39 Huber, Prof Dr. Dr. Peter 103 J S Schlemmer, Prof. Dr. Heinz-Peter 98 Schütz, Prof. Dr. Günther 49 Stöcklin, Dr. Georg 51 T Teleman, Dr. Aurelio 72 Tews, Dr. Björn 138 Trumpp, Prof. Dr. Andreas 34 U Ulrich, Prof. Dr. Cornelia 124 Utikal, Prof. Dr. Jochen 127 V Jäger, Prof. Dr. Dirk 95 Jahn, Dr. Thomas 76 Jäkel, Prof. Dr. Oliver 101 von Deimling, Prof. Dr. Andreas 135 von Engelhardt, Dr. Jakob 59 von Kalle, Prof. Dr. Christof 122 von Knebel Doeberitz, Prof. Dr. Magnus 123 K W Kaaks, Prof. Dr. Rudolf 81 Klingmüller, PD Dr. Ursula 63 Wick, Prof. Dr. Wolfgang 134 Wiemann, PD Dr. Stefan 64 Witt, Prof. Dr. Olaf 130 142 Imprint Published by German Cancer Research Center in the Helmholtz-Association Edited by German Cancer Research Center Press and Public Relations Im Neuenheimer Feld 280 69120 Heidelberg Germany [email protected] www.dkfz.de Editorial responsibility Dr. Stefanie Seltmann Head of Press and Public Relations Layout Selin Haritounian Tanja Kühnle David Männle Translation Angela Browne Design Concept UNIT Werbeagentur GmbH Print PRINTEC OFFSET > medienhaus >, Kassel Picture Credits Tobias Schwerdt (Pg. 3,6/7, 8 [third picture from above], 9 –11, 12 [Portrait in foreground], 16, 142/143); Nicole Schuster (Pg. 8 [2nd und 4th pictures from above]); Jutta Jung (Pg. 8 [3rd picture from above], 15, 140/141); Brigitte Engelhardt (Pg. 12/13 [background]); DKFZ LifeScience Lab (Pg. 14 [1st and 3rd picture from above]); Nadine Querfurth (Pg. 14 [2nd picture from above]); Dr. Martina Pötschke-Langer (Pg. 17); DKFZ Career Service (Pg. 18), Technology Transfer (Pg. 19), Heidelberg University- Communication and Marketing (Pg. 20 above right), University Hospital Heidelberg (Pg. 21 above left); European Molecular Biology Laboratory Heidelberg (Pg. 21 above middle); Max Planck Institute for Medical Research (Pg. 21 above right); line-of-sight - Fotolia.com (Pg. 20–21 bottom) The images on the individual departmental pages originate from the respective units. © German Cancer Research Center 2014 All rights reserved. 143 German Cancer Research Center Im Neuenheimer Feld 280 69120 Heidelberg, Germany Phone +49 (0) 6221.42-2854 Fax +49 (0) 6221.42-2968 [email protected], www.dkfz.de 50 50 50
