Analysis of Fc-Receptor IIA and IIIA Polymorphisms- .ppt
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1、Analysis of FcReceptor IIA and IIIA Polymorphisms: Correlation with Outcome in Trastuzumab-Treated Her2/neu Amplified Early and Metastatic Breast Cancer Patients POSITIVE DISCLOSURES,Dr. Hurvitz received research/grant support from Genentech/Roche Dr. Stern is an employee of Genentech and stockholde
2、r in Roche Jeremy Stinson is an employee of Genentech and stockholder in Roche Dr. Seshagiri is an employee of Genentech and stockholder in Roche Dr. Robert receives research/grant support from Genentech and is on the Roche Speakers Bureau Dr. Valero receives research/grant support from Genentech/Ro
3、che and is on the Roche Speakers Bureau Dr. Crown receives research/grant support from Roche and is on the Roche Speakers Bureau Dr. Slamon is on the speakers bureau for Genentech,Analysis of Fc Receptor IIa and IIIa Polymorphisms: Correlation with Outcome in Trastuzumab-Treated Her2/neu Amplified E
4、arly and Metastatic Breast Cancer Patients,Sara A. Hurvitz, David Betting, Howard M. Stern, Emmanuel Quinaux, Jeremy Stinson, Somasekar Seshagiri, Ying Zhao, Marc Buyse, John Mackey, Nicholas J. Robert, Vicente Valero, John Crown, Adrian Driga, Valerie Bee, Dennis J. Slamon, John M. Timmerman,Abstra
5、ct 64,1. Growth Factor Receptor Blockade Inactivation of AKT signaling Decreased Cell Proliferation Induction of Apoptosis,Tumor Cell,Trastuzumab: Her2-Monoclonal IgG1 Antibody Postulated Mechanisms of Action,Preclinical evidence for role of ADCC: Efficacy of trastuzumab against breast cancer xenogr
6、afts was largely dependent on FcR binding Clynes et al. Nature Med. 2000;6:443-446,Human FcRIIIa (CD16) polymorphisms,Wu et al, J. Clin. Invest.100:1059, 1997. Lehrnbecher, Blood, 1999;94;4220-4232.,FcRIIIa is expressed on both NK cells and macrophages; ADCC effectors in vivoGene dimorphism encoding
7、 FcRIIIa: phenylalanine (F) or a valine (V) at position 158This residue interacts with IgG1 FcHuman IgG1 binds more strongly to homozygous V/V NK cells than to othersFrequency of genotype in population: 158 V/V 13%, V/F 47%, F/F 40%,Human FcRIIa (CD32) polymorphisms,Wu et al, J. Clin. Invest.100:105
8、9, 1997. Lehrnbecher, Blood, 1999;94;4220-4232.,Gene dimorphism encoding FcRIIa: histidine (H) or arginine (R) at position 131Human IgG1 binds more strongly to homozygous FcRIIa-131 H/H immune cells than to H/R or R/RFrequency in general population: 131 H/H 21%, H/R 58%, R/R 21%,FcR Genotype: Outcom
9、e with Monoclonal Ab Therapy,Rituximab anti-CD20-antibody for non-Hodgkins lymphoma: FcRIIIa-158V/V and FcRIIa-131H/H genotypes associated with improved response rates and PFS. Question: Does FcR genotype play a role in the response to trastuzumab?Such an association would: provide evidence that the
10、 immune system plays a role in the anti-tumor activity of trastuzumab support the development of engineered monoclonal antibodies with an increased affinity for FcR to improve drug efficacy,Cartron, Blood 2002;99:754-758. Weng, W-Ki, et al. JCO 2003,Previous studies of FcR genotypes in trastuzumab-t
11、reated breast cancer: Discordant Results,Foster, et al1: No association between FcRIIIa genotype and response in retrospective analysis of trial evaluating trastuzumab monotherapy in relapsed MBC (N=63) Musolino et al, 20082: Assessed role of FcR genotypes in predicting efficacy of trastuzumab in 54
12、 Her2+ MBC receiving trastuzumab + taxane.,1. Foster, Ostland, Mass, et al. Proceedings ASCO, 2002. 21(Abstract No: 227) 2. Musolino et al. J Clin. Oncol. 2008: 26,Purpose,Determine whether FcRIIIa 158 V/F and/or FcRIIa 131 H/R genotypes are associated with disease free survival (DFS) in large cohor
13、t of patients with Her2/neu-amplified early stage breast cancer treated with trastuzumab.In a separate cohort of Her2+ metastatic breast cancer patients treated with trastuzumab, determine whether FcRIIIa158 V/F and/or FcRIIa131 H/R genotypes are associated with time to progression (TTP).,Methods,Se
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