亲环素
FKBP公司
亲环素A
双功能
配体(生物化学)
化学
小分子
连接器
细胞生物学
血浆蛋白结合
生物化学
生物
受体
分子生物学
催化作用
操作系统
基因
计算机科学
作者
Ziyang Zhang,Kevan M. Shokat
标识
DOI:10.1002/anie.201910124
摘要
Abstract Here we report the design, synthesis, and characterization of bifunctional chemical ligands that induce the association of Ras with ubiquitously expressed immunophilin proteins such as FKBP12 and cyclophilin A. We show this approach is applicable to two distinct Ras ligand scaffolds, and that both the identity of the immunophilin ligand and the linker chemistry affect compound efficacy in biochemical and cellular contexts. These ligands bind to Ras in an immunophilin‐dependent fashion and mediate the formation of tripartite complexes of Ras, immunophilin, and the ligand. The recruitment of cyclophilin A to GTP‐bound Ras blocks its interaction with B‐Raf in biochemical assays. Our study demonstrates the feasibility of ligand‐induced association of Ras with intracellular proteins and suggests it as a promising therapeutic strategy for Ras‐driven cancers.
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