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Is targeted therapy the future of personalized cancer care? Vibeke Kruse MD PhD Medical Oncologist Clinical Pharmacologist Department of Medical Oncology UZ Gent 22 November 2016 Outline 1) Introduction 2) Systemic therapy in oncology • Chemotherapy • Targeted Therapy • Immunotherapy 3) Conclusions Vibeke Kruse 2016 Outline 1) Introduction 2) Systemic therapy in oncology • Chemotherapy • Targeted Therapy • Immunotherapy 3) Conclusions Vibeke Kruse 2016 Personalized medicine Breast Cancer – an example: Breast cancer is NOT one disease Vibeke Kruse 2016 Personalized medicine Diagnosis of breast cancer: Primary tumor Lymph node involvement Metastatic disease TNM classification – stage I-IV Breast cancer is NOT one disease Vibeke Kruse 2016 Personalized medicine Diagnosis of breast cancer: Primary tumor Lymph node involvement Metastatic disease Surgery possible? Systemic treatment ? Chemotherapy ? Targeted therapy ? Radiotherapy ? TNM classification – stage I-IV Breast cancer is NOT one disease Vibeke Kruse 2016 Personalized medicine Treatment of breast cancer: Surgery Radiotherapy Systemic treatment Chemotherapy Targeted therapy - Hormonal Treatment - anti-HER2 treatment - anti-VEGF treatment Vibeke Kruse 2016 Personalized medicine Treatment of breast cancer: Pathology report • Size • Differentiation • Ki67% Surgery possible? • Estrogen receptors Systemic treatment ? • Progesteron receptor Chemotherapy ? Targeted therapy ? Radiotherapy ? • HER2 Staging (metastases ?) Patient • Age • Medical history • Personal Whishes • … Reimbursement Vibeke Kruse 2016 Vibeke Kruse 2016 Outline 1) Introduction 2) Systemic therapy in oncology • Chemotherapy • Targeted Therapy • Immunotherapy 3) Conclusions Vibeke Kruse 2016 Systemic therapy Chemotherapy Targeted therapy Immunotherapy Vibeke Kruse 2016 Systemic therapy Chemotherapy Targeted therapy Immunotherapy Vibeke Kruse 2016 Chemotherapy Mechanism of action Not tumour specific Inhibits cell division by targeting different phases of the cell cycle Can’t differentiate between healthy and cancer cells Attacks all rapidly dividing cells -Bone marrow -Digestive tract -Hair follicles -... Chemotherapy Vibeke Kruse 2016 Chemotherapy Side effects: Chemotherapy Nausea Changed taste Aloplecia Myelosuppression Stomatitis Increased risk for infection Hand foot syndrome …. Vibeke Kruse 2016 Chemotherapy Treatment of side effects: Vibeke Kruse 2016 Systemic therapy Chemotherapy Targeted therapy Immunotherapy Vibeke Kruse 2016 Targeted therapy Vibeke Kruse 2016 Targeted therapy We need: target + (available) treatment Vibeke Kruse 2016 Targeted therapy Same target – different organ Vibeke Kruse 2016 Targeted therapy Same target – different organ HER2 10-15% 15-20% Vibeke Kruse 2016 Targeted therapy Same target – different organ HER2 Vibeke Kruse 2016 Targeted therapy Same target – different organ Vibeke Kruse 2016 Targeted therapy Same target – different organ BRAFmutation 50% 5-10% Vibeke Kruse 2016 Targeted therapy BRAF mutation melanoma Flaherty NEJM 2010 Vibeke Kruse 2016 Targeted therapy BRAF mutation Coloncarcinoma Kopetz S et al. JCO.2015. Vibeke Kruse 2016 Targeted therapy The value of a target depends on the localisation of the tumor Vibeke Kruse 2016 Targeted therapy Side effects: Vibeke Kruse 2016 Systemic therapy Chemotherapy Targeted therapy Immunotherapy Vibeke Kruse 2016 Systemic therapy Vibeke Kruse 2016 Checkpoint Blockade and Cancer • CTLA-4–blocking antibodies release an immune checkpoint at the activation step of an immune response to cancer • PD-1–blocking antibodies release an immune checkpoint at the effector step of an immune response to cancer • Pembrolizumab is a PD-1–blocking antibody with robust efficacy and manageable toxicity in patients with advanced melanoma1-5 Reprinted with permission from Ribas A. N Engl J Med 2012;366:2517-9. Copyright © 2012 Massachusetts Medical Society. Human IgG4 KD: ~29 pM PD-L1 IC50: ~0.1-0.3 nM PD-L2 IC50: ~0.5-0.9 nM 1. Hamid O et al. N Engl J Med. 2013;392:134-144; 2. Robert C et al. Lancet. 2014;384:1109-1117; 3. Daud A et al. Presented at: Society for Melanoma Research 2014 Annual Meeting; November 13-16, 2014; Zurich, Switzerland; 4. Robert C et al. Abstract LBA34. Presented at: ESMO 2014 Congress; September 26-30, 2014; Madrid, Spain; 5. Ribas A et al. Presented at: Society for Melanoma Research 2014 Annual Meeting; November 13-16, 2014; Zurich, Switzerland. Non-Conventional Response and I-O Therapy Apparent progression upon radiographic imaging after initial I-O therapy can actually be a sign of non-conventional response to I-O therapy. This response may occur when T cells infiltrate 1,2 the tumor site and cause tumors to flare or appearance of new lesions upon imaging. I-O therapy Tumor cells T cells infiltrating the tumor site Appearance of new lesions upon imaging I-O, immuno-oncology. 1. Wolchok JD et al. Clin Cancer Res. 2009;15:7412-7420. 2. Ribas A et al. Clin Cancer Res. 2009;15:7116-7118. 31 Immune-Mediated Adverse Reactions Immune-mediated adverse reactions affect certain organ systems1 1. 2. 3. 4. 5. Nervous system2 Eyes1,3 Skin1,2,4 Respiratory system1,2 Liver2,4 Endocrine system2,4 Gastrointestinal tract1-4 Hematopoietic cells5 Amos SM et al. Blood. 2011;118(3):499-509. Chow LQ. Am Soc Clin Oncol Educ Book. 2013:280-285. Robinson MR et al. J Immunother. 2004;27(6):478-479. Phan GQ et al. Proc Natl Acad Sci U S A. 2003;100(14):8372-8377. Lin TS et al. J Clin Oncol. 2010;28(29):4500-4506. 32 irAE – prognostic value? • Is there a link between response to immunotherapy and development of an irAE? • Some data support an association between clinical benefit and the induction of a cutanous irAEs Freeman-Keller et al. Clin Cancer Res; 22(4) February 15, 2016 Vibeke Kruse 2016 Vibeke Kruse 2016 ION | key assets in Ghent growing base of preclinical and translational research activity in cancer immunology Bioscience Engineering Statistics and Bioinformatics VIB Biochemistry Nanobody lab Nuclear receptor lab Cytokine receptor lab Molecular immunology Pharmaceutical Sciences biopharmaceutical technology unit Medicine and Health Sciences Immunology – Hematology Experimental Immunology Dermatology Research Unit Thoracic Tumor Immunology lab Gastroenterology-Hepatology Radiation Oncology Lab of Experimental Cancer Research VIB Inflamm. Research Center Molecular & cellular oncology Molecular signalling and cell death Inflammation and immunity Veterinary Science Laboratory of gene therapy KV Mar 2016 LABS CLINICS patients Bioscience Engineering VIB-UGent biomarker discovery UZ Gent immuno-assays translational research Veterinary Sciences • tumor boards • biobanks IO in clinical trials & routine practice immuno-profiling immuno-monitoring Pharmaceutic al Sciences KV Mar 2016 The ION-Ghent steering group Vibeke Kruse, Medical Oncology Lieve Brochez, Dermatologic Oncology Tessa Kerre, Hematological Oncology & Immunology Katrien De Wolf, Piet Ost, Radiation Oncology Karim Vermaelen, Thoracic Oncol. & Immunology with support from Sofie Bekaert (BIMETRA) Pieter Rondou (CRIG) KV Mar 2016 Outline 1) Introduction 2) Systemic therapy in oncology • Chemotherapy • Targeted Therapy • Immunotherapy 3) Conclusions Vibeke Kruse 2016 Conclusion Is targeted therapy the future of personalized cancer care? Targeted therapy is a cornerstone of cancer care But …. • Personalized cancer care is MORE than targeted therapy alone Not all cancers have a target (so far) We need to define more targets and develop new targeted therapies/making existing therapies available • • • Immunotherapy is of growing importance (target(s): different aspects of the immune system) Chemotherapy still plays an important role High need for biomarkers Vibeke Kruse 2016 Conclusion Is targeted therapy the future of personalized cancer care? Vibeke Kruse 2016 Conclusion Is targeted therapy the future of personalized cancer care? A combination of Chemotherapy Targeted therapy Immunotherapy Surgery Radiotherapy Combinations ….. Vibeke Kruse 2016 THANK YOU FOR YOUR ATTENTION [email protected] Vibeke Kruse 2016