Design, synthesis, and biological evaluation of largazole derivatives: alteration of the zinc-binding domain

Article ID	Journal	Published Year	Pages	File Type
5216546	Tetrahedron	2014	7 Pages	PDF

Abstract

A new series of largazole analogues in which the side chain was replaced with disulfide groups were synthesized, and their biological activities were evaluated. Compound 8 bearing an octyl moiety showed much better selectivity for HDAC1 over HDAC7 than largazole (320-fold). Structure-activity relationships suggested that the length in the disulfide chain of largazole is important for the selectivity toward HDAC1 over HDAC7.

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Keywords

largazole HDAC inhibitor Macrocycles Disulfide bridge Peptides

Related Topics

Physical Sciences and Engineering Chemistry Organic Chemistry

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Design, synthesis, and biological evaluation of largazole derivatives: alteration of the zinc-binding domain

Authors

Jinyue Su, Yatao Qiu, Kun Ma, Yiwu Yao, Zhen Wang, Xianling Li, Dayong Zhang, Zhengchao Tu, Sheng Jiang,