“无连接子”异羟肟酸作为选择性HDAC8抑制剂的设计与评价

Design and evaluation of 'Linkerless' hydroxamic acids as selective HDAC8 inhibitors.

作者信息

Krennhrubec Keris, Marshall Brett L, Hedglin Mark, Verdin Eric, Ulrich Scott M

机构信息

Department of Chemistry, Ithaca College, Ithaca, NY 14850, USA.

出版信息

Bioorg Med Chem Lett. 2007 May 15;17(10):2874-8. doi: 10.1016/j.bmcl.2007.02.064. Epub 2007 Feb 25.

DOI:10.1016/j.bmcl.2007.02.064

PMID:17346959

Abstract

In this report, we describe new HDAC inhibitors designed to exploit a unique sub-pocket in the HDAC8 active site. These compounds were based on inspection of the available HDAC8 crystal structures bound to various inhibitors, which collectively show that the HDAC8 active site is unusually malleable and can accommodate inhibitor structures that are distinct from the canonical 'zinc binding group-linker-cap group' structures of SAHA, TSA, and similar HDAC inhibitors. Some inhibitors based on this new scaffold are >100-fold selective for HDAC8 over other class I and class II HDACs with IC(50) values <1microM against HDAC8. Furthermore, treatment of human cells with the inhibitors described here shows a unique pattern of hyperacetylated proteins compared with the broad-spectrum HDAC inhibitor TSA.

摘要

在本报告中，我们描述了旨在利用HDAC8活性位点中一个独特亚口袋而设计的新型HDAC抑制剂。这些化合物是基于对与各种抑制剂结合的现有HDAC8晶体结构的研究，这些结构共同表明HDAC8活性位点具有异常的可塑性，能够容纳与SAHA、TSA及类似HDAC抑制剂的典型“锌结合基团-连接子-帽基团”结构不同的抑制剂结构。基于这种新支架的一些抑制剂对HDAC8的选择性比对其他I类和II类HDAC高100倍以上，对HDAC8的IC(50)值<1微摩尔。此外，与广谱HDAC抑制剂TSA相比，用本文所述抑制剂处理人类细胞显示出一种独特的高乙酰化蛋白模式。

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“无连接子”异羟肟酸作为选择性HDAC8抑制剂的设计与评价

Design and evaluation of 'Linkerless' hydroxamic acids as selective HDAC8 inhibitors.

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