| Literature DB >> 33915015 |
Guangyan Du1,2, Jie Jiang1,2, Qibiao Wu3,4, Nathaniel J Henning1,2, Katherine A Donovan1,2, Hong Yue1,2, Jianwei Che1,2, Wenchao Lu1,2, Eric S Fischer1,2, Nabeel Bardeesy3,4, Tinghu Zhang5, Nathanael S Gray5.
Abstract
Aberrant activation of FGFR signaling occurs in many cancers, and ATP-competitive FGFR inhibitors have received regulatory approval. Despite demonstrating clinical efficacy, these inhibitors exhibit dose-limiting toxicity, potentially due to a lack of selectivity amongst the FGFR family and are poorly tolerated. Here, we report the discovery and characterization of DGY-09-192, a bivalent degrader that couples the pan-FGFR inhibitor BGJ398 to a CRL2VHL E3 ligase recruiting ligand, which preferentially induces FGFR1&2 degradation while largely sparing FGFR3&4. DGY-09-192 exhibited two-digit nanomolar DC50 s for both wildtype FGFR2 and several FGFR2-fusions, resulting in degradation-dependent antiproliferative activity in representative gastric cancer and cholangiocarcinoma cells. Importantly, DGY-09-192 induced degradation of a clinically relevant FGFR2 fusion protein in a xenograft model. Taken together, we demonstrate that DGY-09-192 has potential as a prototype FGFR degrader.Entities:
Keywords: FGFR1; FGFR2; cholangiocarcinoma; degrader; protein degradation
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Year: 2021 PMID: 33915015 PMCID: PMC8324087 DOI: 10.1002/anie.202101328
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 16.823