Primary Focus Lead, Targeted Protein Degradation 坂田 千夏 Head of Engineered Small Molecules 早川 昌彦 Head of Oncology Development Ahsan Arozullah チーフコミュニケーションズ&IRオフィサー 池田 博光 再生リスト 最初から再生 TARGETED PROTEIN DEGRADATION TARGETED PROTEIN DEGRADATION Cautionary statement regarding forward-looking information Contents INTRODUCTION Targeted protein degraders have the potential to overcome limitations of traditional small molecules and tackle “undruggable” targets TARGETED PROTEIN DEGRADATION STRATEGY We aspire to evolve TPD into a key capability for Astellas and a major driver of our pipeline expansion Mutated KRAS is a historically “undruggable” target and KRAS G12D is the most common KRAS driver mutation There is high unmet need in cancers expressing KRAS G12D mutations - take PDAC as an example PROGRESS ON ASP3082 Our lead program, ASP3082, is the first protein degrader for mutated KRAS G12D to enter the clinic Phase 1 study design of ASP3082 Our Phase 1 study population primarily had advanced pancreatic, colorectal and non-small cell lung cancer ASP3082 safety profile in doses up to 600mg ASP3082 exceeded target exposure in the body >300mg QW and KRAS G12D was degraded in a dose-dependent manner Antitumor activity was observed in patients with PDAC and NSCLC receiving doses between 300-600mg Responses to ASP3082 over time in patients with PDAC and NSCLC The results and safety profile of ASP3082 support further clinical investigation PIPELINE UPDATE Robust early research pipeline leveraging advantages of protein degraders Our portfolio consists of targeted protein degraders-addressing historical “undruggables” Our in-house expertise further advances this complex modality Collaboration with external partners - acquiring novel POI/E3 binders to develop innovative targeted protein degraders @ Questions Questions 1 Questions 2 Questions 3 Questions 4 Questions 5 Questions 6 Questions 7 Questions 8 前へ 次へ