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New Perspectives in Cancer Therapy Óren Smaletz Programa de Oncologia Hospital Israelita Albert Einstein Disclosure of Potential Conflicts of Interest • Honoraria: Pfizer, Merck KGaA • Research Funding: Pfizer • Scientific Funding: Merck KGaA, Roche CFM Resolution nº 1.595/2000 SBOC/SBC oct/2007 A 72-year-old man presented for evaluation of progressive dyspnea and cough McMullan D and Cohen G. N Engl J Med 2006;354:397 Change in the US Death Rates* by Cause, 1950 & 2002 Rate Per 100,000 600 586.8 1950 500 2002 400 300 240.1 200 193.9 180.7 193.4 100 56.0 48.1 22.5 0 Heart Diseases Cerebrovascular Diseases Pneumonia/ Influenza Cancer * Age-adjusted to 2000 US standard population. Sources: 1950 Mortality Data - CDC/NCHS, NVSS, Mortality Revised. 2002 Mortality Data: US Mortality Public Use Data Tape, 2002, NCHS, Centers for Disease Control and Prevention, 2004 Fight Against Cancer • Surgery • Radiotherapy • Chemotherapy • Targeted Therapy Agents FDA Approved New Molecules for Solid Tumor Use per Year 2002 2003 2004 2005 2006 2007 0 1 T argeted T herapy Agent 2 Cy totox ic Agent 3 Schrag, D., New Engl J Med 2004 Hanahan D, Cell 2000 The EGFR (erbB) Family and Ligands EGF TGFa Amphiregulin b-cellulin HB-EGF Epiregulin Heregulins NRG2 NRG3 Heregulins b-cellulin 100 44 36 48 100 82 59 79 100 33 24 28 HER1 EGFR ErbB-1 HER2/neu ErbB-2 HER3 ErbB-3 HER4 ErbB-4 Cysteine-rich domains Tyrosine kinase domain C-terminus Família EGFR (Her) Hudis NEJM 2007 Trastuzumab – mecanismo de ação Hudis NEJM 2007 Trastuzumab in Breast Cancer Trastuzumab – metastatic breast cancer Slamon, NEJM 2001 Trastuzumab – metastatic breast cancer Slamon, NEJM 2001 Trastuzumab – adjuvant treatment Trastuzumab – adjuvant treatment EGFR Signaling Pathways R R R R R R Extracellular Membrane pY pY pY pY K K K K K Intracellular Substract K Substract pY pY pY Cellular effects Signaling Molecules + + + proliferation apoptosis angiogenesis metastasis EGFR Expression in Human Cancer Tumors Overexpression associated with: • • • • • Invasion Metastasis Advanced disease Poor outcome Resistance to chemotherapy, hormonotherapy radiotherapy Expression (%)* NSCLC 50-90 Colorectal 45-80 Gastric 30-60 Pancreatic 30-50 Ovarian 35-60 Prostate 40-70 Breast 14-91 Head and Neck 70-100 Kidney 80-100 *lowest to highest published range of expression Disease-free Survival and EGFR and TGF-a Levels in Head and Neck Cancer EGFR TGFa Proportion Surviving 1.0 low low medium medium 0.8 0.6 0.4 0.2 high high p=.0001 p=.0001 0.0 0 1 2 3 4 Years after surgery 5 6/0 1 2 3 4 Years after surgery Rubin Grandis J et al. JNCI 1998; 90: 824–832. 5 6 EGFR Mab Currently Approved Clinical activity randomized trials Cetuximab FDA ANVISA Dosage Head & Neck Colon/Rectal Y Y Y Y 400 mg/m2 i.v. initial dose followed by 250 mg/m2 weekly Panitumumab Colon/Rectal Y N 6 mg/kg i.v. every 14 days Cetuximab (Erbitux®) • IgG1 (chimerized antibody) • Exclusive for EGFR and its heterodimers • Prevents ligand binding to EGFR • High affinity. Kd = 0.39 nM (M-225 Kd = 1 nM) • 1 log > natural ligand • Stimulates receptor internalization • Blocks receptor dimerization, tyrosine kinase phosphorylation, signal transduction Panitumumab (Vectibix®) • fully human IgG2κ mAb • high affinity (Kd ~ 0.05 nM) • Upon binding, internalized and donwregulates EGFR • Prevents – receptor dimerization – EGFR-tyrosine autophosphorylation – activation of downstream signaling molecules Mechanism of Action of anti-EGFR Monoclonal Antibodies Membrane Cancer Cell X Cell proliferation Apoptosis X Metastasis X Angiogenesis Nucleus X Cetuximab in Colorectal Cancer (“Bond Trial”) • Eligibility criteria Pretreated metastatic colorectal cancer with irinotecan All patients had to be EGF-R positive Primary end-point Tumor response Cetuximab in Colorectal Cancer (“Bond Trial”) Cetuximab and Irinotecan 218 patients Irinotecan pretreated Metastatic CRC EGFR positive Cetuximab 111 patients Cetuximab in Colorectal Cancer (“Bond Trial”) N OR (%) TTP (months) Survival (months) C225 and Irinotecan 218 22.9 4.1 8.6 C225 111 10.8 1.5 6.9 p = 0.007 Cunningham et al., New Engl J Med 2004 Cunningham et al., New Engl J Med 2004 Panitumumab in Colon/Rectal Cancer Panitumumab + BSC 463 EGFR +, M1 Colon/Rectal Cancer, POD on standard chemoRX BSC Primary Endpoint: PFS Minimum f/u 12 months Van Cutsem et al., J Clin Oncol 2007 Panitumumab vs. BSC Van Cutsem st al. J Clin Oncol 2007 Van Cutsem st al. J Clin Oncol 2007 Panitumumab vs. BSC EGFR and K-RAS • K-RAS mutation present in 40-45% patients • When K-ras gene is mutated, K-ras protein (p21 ras) is active independently of EGFR activation Khambata-Ford et al. JCO 2007 K-RAS mutation detection • PCR test for mutation in codons 12 and 13 kras Chen et al. Clin Chem 2004 pre-treated Metastatic CRC (no other option available) Cetuximab + BSC 287 patients BSC 285 patients Karapetis et al. New Engl J Med 2008 Take Home Message • Moleculat Targeted Therapy – showtime • Benefit is evident – as well as costs • Who should receive? – Clinical oncology os meeting science Thank you [email protected]