학술행사/세미나 안내 및 신청
Isoform-specific inhibition of FGFR signaling achieved by a de novo-designed mini-protein
연사
박준성 Ph.D
세미나개최일
2023-10-18(수) 11:00
작성자
문성희
작성일
2023-10-12
조회
544
Cellular signaling by fibroblast growth factor receptors (FGFRs) is a highly regulated process mediated by specific interactions between distinct subsets of fibroblast growth factor (FGF) ligands and two FGFR isoforms generated by alternative splicing: an epithelial b- and mesenchymal c-isoforms. Here, the properties of a mini-protein, mb7, developed by an in silico design strategy to bind to the ligand-binding region of FGFR2 are investigated. Structural, biophysical, and cellular analyses demonstrating that mb7 binds with high affinity to the c-isoforms of FGFR, resulting in inhibition of cellular signaling induced by a subset of FGFs that preferentially activate c-isoforms of FGFR are described. Notably, as mb7 blocks interaction between FGFR with Klotho proteins, it functions as an antagonist of the metabolic hormones FGF19 and FGF21, providing mechanistic insights and strategies for the development of therapeutics for diseases driven by aberrantly activated FGFRs.