4'-Methyl-4,5'-bithiazole-based correctors of defective delta F508-CFTR cellular processing

4'-甲基-4,5'-联噻唑类校正缺陷的ΔF508-CFTR细胞加工

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Abstract

The synthesis and Delta F508-CFTR corrector activity of a 148-member methylbithiazole-based library are reported. Synthetic routes were devised and optimized to generate methylbithiazole analogs in four steps. Corrector potency and efficacy were assayed using epithelial cells expressing human Delta F508-CFTR. These structure-activity data establish that the bithiazole substructure plays a critical function; eight novel methylbithiazole correctors were identified with low micromolar potencies.

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