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Structural insights into the potency and selectivity of covalent pan-FGFR inhibitors.

Lingzhi QuXiaojuan ChenHudie WeiMing GuoShuyan DaiLongying JiangJun LiSitong YueZhuchu ChenYongheng Chen
Published in: Communications chemistry (2022)
FIIN-2, TAS-120 (Futibatinib) and PRN1371 are highly potent pan-FGFR covalent inhibitors targeting the p-loop cysteine of FGFR proteins, of which TAS-120 and PRN1371 are currently in clinical trials. It is critical to analyze their target selectivity and their abilities to overcome gatekeeper mutations. In this study, we demonstrate that FIIN-2 and TAS-120 form covalent adducts with SRC, while PRN1371 does not. FIIN-2 and TAS-120 inhibit SRC and YES activities, while PRN1371 does not. Moreover, FIIN-2, TAS-120 and PRN1371 exhibit different potencies against different FGFR gatekeeper mutants. In addition, the co-crystal structures of SRC/FIIN-2, SRC/TAS-120 and FGFR4/PRN1371 complexes reveal structural basis for kinase targeting and gatekeeper mutations. Taken together, our study not only provides insight into the potency and selectivity of covalent pan-FGFR inhibitors, but also sheds light on the development of next-generation FGFR covalent inhibitors with high potency, high selectivity, and stronger ability to overcome gatekeeper mutations.
Keyphrases
  • structural basis
  • tyrosine kinase
  • clinical trial
  • cancer therapy
  • gene expression
  • randomized controlled trial
  • genome wide
  • open label
  • anti inflammatory
  • protein kinase
  • phase ii
  • double blind