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February, the 9th 2007 COMBINATORX SPEED DATING FOR MOLECULES BATIQUE Laura, MARICOURT Aurélie & PALADINI Bénédicte Safe Harbor This is an independent study performed by students from the Faculté des Sciences Pharmaceutiques de Lille The opinions expressed are our own and not necessarily those of Combinatorx SUMMARY Idea Organization chart Finance Research & development: cHTS Patent Pipeline Communication to stockholders conclusion IDEA History summer 1999: group of young researchers: Brent Stockwell Mike Foley Alexy Borisy Curtis Keith « Curious Liquid café » disease: multifactorial process No magic bullet Multiple pathways « networked systems » Multiple pathways: Traditional combinations : « art antérieur » i.e. HIV & cancer treatment Screening for combinations: active small molecules Look for syncretic drug & synergistic drug through different pathways To create a novel, strong & unexpected therapeutic effect « Logistical nightmare »: - library of 100 000 compounds 100 billion paired combinations screening them: $10 billion/50 000 years!!! Focus exclusively on FDA-approved drugs with expired patents 2 000 compounds 2 million paired combinations How? HIGH THROUGHPUT SCREENING (cHTS™) Interests: Pre-approved Compounds Bypassing time-consuming synthesis stage Available data: - pharmacology/toxicology - dosing - formulation - safety and kinetic studies Lessen development time, cost and risks Higher degree of success Risks Why low doses of therapeutics that have nothing to do with a disease have an effect on the disease process? metabolism issue? Why doctors wouldn’t prescribe 2 drugs independently, instead of the combined cocktail? Adjust formulation Regulatory risks: negative synergistic effects? FOUNDERS Founders a group of young researchers Alexis BORISY (Harvard University, independant industry consultant) Mike FOLEY(Harvard University, researching the interface of chemistry and biology) Brent STOCKWELL (Harvard University, assistant professor at Columbia University) Curtis KEITH (Harvard University, McGill University) MANAGEMENT TEAM Management Team Alexis BORISY President Robert FORRESTER Chief Financial Officer Jan LESSEM Lynn BAIRD Daniel GRAU Chief Medical Officer Quality & Clinical operations Commercial Operations Jason COLE General Counsel Curtis KEITH Senior vice president, Research Scientific Advisors Mike FOLEY Brent STOCKWELL Gary BORISY (professor of cell and molecular biology at Northwertern University Medical School) Peter ELLIOTT ( B.S. at London University, Cambridge University ) Todd GOLUD (expert in medecine, cancer biology and pharmacogenomics , Harvard, University of Chicago) Joanna HOROBIN ( over 20 years of industry experience) Josh LEDERBERG (Nobel Laureate, 82) Scientific/Technical Backgrounds CombinatoRx Research group: - 45 employees in Research: approximately one third hold advanced degrees - Matrix organizational structure - Discovery Biology, In vivo Pharmacology, Formulations… Valuable Expertise: - Cell based assay development - High Throughput screening - Commercial insight BOARD OF DIRECTORS Board of Directors Alexis BORISY President & CEO Richard ALDRICH Managing Director Barbara DEPTULA Richard POPS CEO Alkernes Patrick FORTUNE Executive VP, Shire Pharmaceuticals Boston Millenia Partners Franck HAYDU Michael KAUFFMANN Director, Chaiman of the Audit Committee President and CEO EPIX Pharmaceuticals FINANCE Raising Funds 1990s: Beginning of High Throughput screening Founded in March 2000 Business Angel Investor: Jacob Goldfield: $ 2,5million Raised a total of $ 180 million, since 2000: $ 90 million: - Boston Millenia Partners - Canaan Ventures Partners - Flagship Ventures $ 44,3 million: IPO (november 2005) $ 48 million: private placement (march 2006) New Partnerships Leverage the business with partners : gains 50-90% rights to next product candidates retains 100% rigthts to existing clinical programs CombinatorX_investors_presentation_2006.pdf 2004 September 2005 December Spinal Muscular Atrophy Foundation (SMA) potential milestones payment Accelerate Brain Cancer Cure (ABC²) for Glioblastoma Multiforme (GBM) Novartis: screening work: $500 000 April July National Institute of Allergy and Infectious Disease (NIAID) $4,4million grant block the adverse effects of anthrax toxin Henkan Pharmaceutical: (taiwan) $500 000 upfront potential $23million milestones payments CRX-026 (exclusive & territorial license) IPO 2006 Private placement November August October CHDI (Neurodegener ative Disease Foundation) Huntington’s disease Bio*One Capital: $2,5 million grant $17,5 million milestones payments Infectious disease Angiotech Pharmaceutical: $27million upfront $15million equity investment & potential milestones payments medical devices and interventional medicines March January April June AdipoGenix: obesity Fovea Pharmaceutical: $20 million in potential milestones payments Ophtalmic disease Cystic Fibrosis Foundation Therapeutics (CFFT):potenti al $ 13,8 million in Research Cystic fibrosis (CF) ANALYSE BOURSIERE Identity card of compagny Name : combinatoRx, Incorporated Symbol : CRXX CEO : Alexis Borisy Description : a biopharmaceutical compagny focused on developing new medecines built from synergistic combinations of approved drugs Information industry : drugs - biotechnology Les échos L’action Entrée en bourse le 9 novembre 2005 Capitalisation boursière = 250 millions $ Cash position = 150 millions $ Yahoo finance Comparaison avec l’indice des biotech Private placement Angiotech Adipogenix Fovéa IPO : 9/11/05 CFFT Yahoo finance RESEARCH & DEVELOPMENT COMBINATORX DISCOVERY PROCESS Major Milestones for Development Cell-based phenotypic assay Multi-target drug discovery Action on multiple pathways The only solution: screening of the whole cell Much more complex than biochemical screening « disease-modifying targets » Cells preserve the essential elements of the disease network Empiric multi-target discovery: Phenotypic cellular models i.e. Screening for inflammatory responses: 1) Stimulation of PBMC with LPS production of TNF by several cell types 2) Monitoring production of TNF screening in 384-well format: combinations of compounds that inhibit inflammatory response 3) Potential candidates therapeutics treatment: psoriasis, RA, asthma… Multicomponent therapeutics for networked systems; Curtis T. Keith, Alexis A. Borisy and Brent Stockwell; Nature reviews, drug discovery, january 2005 High Throughput Screening: cHTS Screening pairwise combinations Demand informatic tools (automated robotic screening) & Laboratory Information Management System (LIMS) Partition: active compounds: tested through dose-ratio interaction surfaces inactive compounds: tested in synergistic pairs at a single high concentration Each point = combination activity Gathering of compounds by pharmacological target Perfect symetry? A549, HCT 116, MRC 9 Tumoral cell lines CombinatorX_investors_presentation_2006.pdf High density signal: pathways interaction Potential synergy (red) (blue: no synergy) Potential « hit »? CombinatorX_investors_presentation_2006.pdf Dose-response Matrix 6 concentrations (including 0) for each compound 36 different wells of a microtiter plate Aim: identification of « hits » Interaction surface measured for each pair of compounds 3D inhibition surface Multiple combinations of # ratio of doses Comparison/reference model interaction surface Standard mathematic model of additivity (Loewe, Bliss…) to identify a synergy, an antagonism or a simple additivity Model excess surface score Overall shape of the interaction surface: information: how the compounds act on pathways how the targets for the compounds are related to each other (network connectivity) Analyzing a collection of scores synergy scores « synergy profile » of each agent to emphasize relationships between pathways grid: axes sorted by molecular mechanism for each agent, grouped by pathway Multi-target therapeutics: when the whole is greater than the sum of the parts; Grant R. Zimmermann, Joseph Léhar and Curtis T. Keith; elsevier, drug discovery today, january 2007 Prioritizing & Optimizing Combinations Evaluation: chemical compatibility compatibility: ADMET Determination: Combination Structure-Activity Relationship (CSAR): Combination Mechanism-Activity relationship (CMAR): Examples Inhibition of C.albicans proliferation 384-well plates « cellular viability assay »: Alamar blue fluorescence symetry selection: 30 compounds 2 antifungal agents No antifungal agent 1 antifungal agent Systematic discovery of multicomponent therapeutics; Alexis A. Borisy, Joseph Léhar, E. Royden Price, Grant R. Zimmermann, Michael A. Foley, Brent R. Stockwell, and Curtis T. Keith; PNAS; june 2003 i.e: pentamidine-phenazopyridine : Dose-response matrix pentamidine = 0,03µM phenazopyridine = 4,2µM Systematic discovery of multicomponent therapeutics; Alexis A. Borisy, Joseph Léhar, E. Royden Price, Grant R. Zimmermann, Michael A. Foley, Brent R. Stockwell, and Curtis T. Keith; PNAS; june 2003 Anthrax Antitoxin Program NIAID: $4,4million grant Biodefense Therapeutic goals: Block toxic effects of exposure to anthrax (Bacillus anthracis and its toxin) status: preclinical CombinatorX_investors_presentation_2006.pdf PATENT USPTO PATENT IDEA DEVELOPPEMENT ET MISE AU POINT D’UN PROCEDE cHTS Besoin de lever des fonds Secret Ex: formule du coca cola Communications Méthode dévoilée Protection de la Méthode Revendication: Screening de 2 molécules Synergique Robotisation Associations Conséquences: Nouvelle Innovante Application industrielle BREVET Publication de demande de brevet en 2002 DRUG’S PATENTS Revendications: Description du mécanisme d’action Description des cibles Résultats: Combinaisons inattendues Applicables industriellement Non prévisible pour l’homme de l’art Brevets délivrés: 6 brevets délivrés Ex: Pentamidine + Chlorpromazine ex: Amoxapine+Prednisolone Principes et mécanismes des maladies inflammatoires Inhibition imp de TNF Pas activité aux concentrations Utilisation pour inh/réduire inflammation Composition: Amoxapine de 1-600mg Prednisolone de 0.05 à 200 mg Formulation: IV,IM,VO,VV,VR,Vinh PIPELINE Introduction CRx-026: rescue CRx-102: success CRx-140: failure Introduction Disease areas: Immuno-inflammatory Oncology Metabolic disease Neurodegenerative disease Infectious disease Portfolio: 8 product candidates (phase 2 clinical trials) multiple preclinical candidates in metabolic disease CombinatoRx Pipeline: 2007 Product Strategy Target product profile: single pill/ synergistic/ New medical benefit/ Novel & non obvious patterns of activity/ customized, synergy-based formulation: Non substituable CombinatoRx Advantage: Discovery to Phase 2: Focusing on rapidly building a product pipeline and drug development risk CRx-026 HTS result In vitro, 100 000 combinations tested 600 interesting drugs 13 synergistic combinations identified and confirmed One of these combinations contains: Anti psychosis agent: Chlorpromazine Anti protozoal agent: Pentamidine Birth CRx-026 CRx-026 Chlorpromazine Antipsychotic, anxiolytic Pentamidine Antimicrobial, antiprotozoal (pneumocystosis, leshmaniasis, trypanosoma) •Neither demontrates substancial activity at concentration •Neither is currently used as an Anticancer drug Studies (1) Test in vitro: Percent inhibition of A 549 proliferation Excess over Bliss additivism Excess over HSA (highest single agent) Systematic discovery of multicomponent therapeutics; Alexis A. Borisy, Joseph Léhar, E. Royden Price, Grant R. Zimmermann, Michael A. Foley, Brent R. Stockwell, and Curtis T. Keith; PNAS; june 2003 Studies (2) Effect of chlorpromazine + pentamidine on the growth of A 549 in mice compared classical treatment Systematic discovery of multicomponent therapeutics; Alexis A. Borisy, Joseph Léhar, E. Royden Price, Grant R. Zimmermann, Michael A. Foley, Brent R. Stockwell, and Curtis T. Keith; PNAS; june 2003 Mechanism of Action Anti proliferative activity approved In vitro studies pentamidine chlorpromazine Activity on a mitotic kinesin (hsEg5/KSP), tubulin and inhibition of PRL phosphatase Kinesin It is a protein can move when it have ATP Function: Separate DNA when cellular division Inhibition of KSP Blocks proper spindle function during mitosis Mitotic kinesin is a molecular essential for centrosome separation Centrosome Centrosome: Result Figure 3: A. Inhibition of hsEg5/KSP ATPase activity in cell-free enzymatic assay (squares) and inhibition of proliferation of HCT116 colon cancer cell line (triangles). B. Chlorpromazine caused the formation of monopolar spindle during mitosis (A549 cells). C. Chlorpromazine inhibits centrosome separation but spares duplication (HCT116 cells). Green = alpha-tubulin; red =gamma-tubulin ; blue = DNA.. Discovery and clinical development of CRx-026, a syncretic and anti-mitotic agent with significant anti-cancer activity; Peter J. Elliott, Alexis A. Borisy, Curtis T. Keith; march 2004; CombinatoRx.pdf Pre-Clinical Profil (1) Synergy Activity In vivo activity Discovery and clinical development of CRx-026, a syncretic and anti-mitotic agent with significant anti-cancer activity; Peter J. Elliott, Alexis A. Borisy, Curtis T. Keith; march 2004; CombinatoRx.pdf Pre-Clinical Profil (2) Compared classical treatment Discovery and clinical development of CRx-026, a syncretic and anti-mitotic agent with significant anti-cancer activity; Peter J. Elliott, Alexis A. Borisy, Curtis T. Keith; march 2004; CombinatoRx.pdf Conclusion Clinical evaluation: CRx-026 synergy with taxanes & vinca-alkaloids CRx-102 CRx-102: Novel Oral Syncretic Drug Candidate Very low dose of prednisolone (3mg): steroid Cardiovascular agent (inhibitor of PDE): dipyridamole (200 or 400mg) Novel mechanism selectively amplifies steroid’s desirable activities: A combination sciences dissociated agent Dissociated Steroid Concept ? GC therapy is highly effective at reducing inflammation but chronic use leads to undesirable side effects (osteoporosis, glaucoma, diabetes…) A dissociated steroid could: clinical use steroid toxicities Dipyridamole selective « amplifier » ?? CombinatorX_investors_presentation_2006.pdf CRx-102: Mechanism of Action Crx-102 prednisolone dipyridamole GR PD A2A, A2B mRNA stability ATP GR PD PKA +GRE trans-activation GR PD +GRE cis-repression Steroid Side EffectAssociated Genes GR PD Adenosine Reuptake AC cAMP AMP PDEs NFkB NFAT AP-1 CBP CREB HAT HDAC enhanced trans-repression inhibition of inflammation Steroid Immunomodulatory Effects « Transactivation » side effects « Transrepression » anti-inflammatory effects Dipyridamole: Action on «transrepression way » CRx-102 Clinical Results to Date Phase 2A highly positive studies Generally well tolerated Extrait des JP Morgan, le 17/01/07, slide 16 Opportunities The efficacy & safety profile of CRx-102 may result in a viable alternative for NSAIDS/COXIBs Commercial Opportunities Extrait des JP Morgan, le 17/01/07 CRx-140 CRx 140 : a novel oraly available syncretic agent CRx 140 : one of seven product candidates Indication : psoriasis Cyclosporine has more side effects Aim : increase effect of cyclosporine with another drug Testing in phase II clinical trials Psoriasis Maladie chronique et généralement bénigne Lésions érythémato-squameuses Aussi fréquent pour les 2 sexes Évolution par poussées Étiologies inconnues Existe chez les jeunes sujets => psoriasis en goutte Divers traitements Clinical trials Study design : multi-center, blinded, controlled, patients with a severe psoriasis Index : PASI and PGA PASI : Psoriasis Area and Severity Index PGA : Physician Global Assessments 2 endpoints : Primary : PGA Secondary : PASI Results Side effects Conclusions Phase IIa clinical results did not show statistical significance in prespecified endpoints Development discontinued as an oral product candidate for psoriasis Resources focuses on other product candidates in portfolio COMMUNICATION TO STOCKHOLDERS CombinatoRx Pipeline: 200 Pipeline Pipeline Extrait des JP Morgan, le 17/01/07 2006 Pipeline Failure in phase 2 clinical trials Extrait des JP Morgan, le 17/01/07, slide 7 Goals 2006 2005 = a year of validation : Core Business Strategy Drug discovery approach Continued promise of cHTS technology from you, stockholders 2005 : collaborations Pipeline => oncology and inflammation : CRx-102 : very encouraging CRx-140 : failure Continue to fill our internal pipeline Expect a mix of successes & failures; Look forward to a continued flow of candidates in our pipeline CombinatoRx, « from the president » Real actions New Partnerships : Fovea pharmaceutical AdipoGenix Cystic Fibrosis Foundation Therapeutics Private placement New failure : CRx-119 Developing 3 new molecules Goals 2007 Extrait des JP Morgan, le 17/01/07, slide 9 JP Morgan Présentation attractive pour les investisseurs et les futurs Extrait des JP Morgan, le 17/01/07, slide 7 CONCLUSION Concept original Pipeline étendu Avenir prometteur Attente de résultats cliniques concrets !! Balance Bénéfices/Risques Merci de votre attention BIBLIOGRAPHY CombinatorX_investors_presentation_2006.pdf Multi-target therapeutics: when the whole is greater than the sum of the parts; Grant R. Zimmermann, Joseph Léhar and Curtis T. Keith; elsevier, drug discovery today, january 2007 Speed dating for molecules; Wendy Wolfson; Chemistry & Biology; elsevier; may 2006 Alexis Borisy; Charlie Schmidt, Portland, Maine; Nature biotechnology; may 2006 Screening for drug discovery: the leading question; Adam Smith; Technology Feature, Nature; july 2002 Multicomponent therapeutics for networked systems; Curtis T. Keith, Alexis A. Borisy and Brent Stockwell; Nature reviews, drug discovery, january 2005 Multi-target lead discovery for networked systems; Curtis T. Keith & Grant R. Zimmermann; Current drug discovery, Feature; september 2004 cHTS Systematic discovery of novel combination therapeutics; Grant R. Zimmermann, Margaret S. Lee, Joseph Léhar, Alexis A. Borisy, Curtis T. Keith; CombinatoRx_pdf; 2005 Systematic discovery of multicomponent therapeutics; Alexis A. Borisy, Peter J. Elliott, Nicole W. Hurst, Margaret S. Lee, Joseph Léhar, E. Royden Price, George Serbedzia, Grant R. Zimmermann, Michael A. Foley, Brent R. Stockwell, and Curtis T. Keith; PNAS; june 2003 CombinatoRx_investors_presentation CRx-102_november 2006.pdf Molecular Insights Into Steroid Dissociation of CRx-102, a Clinically Active Immunomodulatory Agent; E. Royden Price, C. Fraser, P. Manivasakam, G. Nolan, B. Smith, J. Léhar, G. R. Zimmermann, C. T. Keith; november 2006; CombinatoRx.pdf A phase II trial of a new anti-inflammatory combination drug, CRx140, in patients with severe psoriasis; Alice Gottlieb, Yanzhen Zhang, Melissa Nichols, CRx-140 group at CombinatoRx, Incorporated and CRx-140 group of investigators UMDNJ & Robert Wood Johnson Med. Ctr., Nexx Brunswick, NJ and CombinatoRx; march 2006; CombinatoRx.pdf Discovery and clinical development of CRx-026, a syncretic and anti-mitotic agent with significant anti-cancer activity; Peter J. Elliott, Margaret S. Lee, Mitchell Keegan, Yanzhen Zhang, M. James Nichols, Alexis A. Borisy, Curtis T. Keith; march 2004; CombinatoRx.pdf CombinatoRx_ Annual Report 2005.pdf CombinatoRx_investors_presentation_april 2006.pdf HBA CombinatoRx presentation; september 2006.pdf JP Morgan, january 2007 www.combinatorx.com : www.combinatorx.com/pipeline/ http://www.combinatorx.com/overview/ http://www.combinatorx.com/discovery/ http://phx.corporate-ir.net/phoenix.zhtml?c=148036&p=irol-news