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基于片段的溴结构域抑制剂发现 第 1 部分:抑制剂结合模式及其对先导化合物发现的意义。

Fragment-based discovery of bromodomain inhibitors part 1: inhibitor binding modes and implications for lead discovery.

机构信息

Computational & Structural Chemistry, Molecular Discovery Research, GlaxoSmithKline R&D, Medicines Research Centre, Gunnels Wood Road, Stevenage, Hertfordshire SG1 2NY, UK.

出版信息

J Med Chem. 2012 Jan 26;55(2):576-86. doi: 10.1021/jm201320w. Epub 2012 Jan 11.

Abstract

Bromodomain-containing proteins are key epigenetic regulators of gene transcription and readers of the histone code. However, the therapeutic benefits of modulating this target class are largely unexplored due to the lack of suitable chemical probes. This article describes the generation of lead molecules for the BET bromodomains through screening a fragment set chosen using structural insights and computational approaches. Analysis of 40 BRD2/fragment X-ray complexes highlights both shared and disparate interaction features that may be exploited for affinity and selectivity. Six representative crystal structures are then exemplified in detail. Two of the fragments are completely new bromodomain chemotypes, and three have never before been crystallized in a bromodomain, so our results significantly extend the limited public knowledge-base of crystallographic small molecule/bromodomain interactions. Certain fragments (including paracetamol) bind in a consistent mode to different bromodomains such as CREBBP, suggesting their potential to act as generic bromodomain templates. An important implication is that the bromodomains are not only a phylogenetic family but also a system in which chemical and structural knowledge of one bromodomain gives insights transferrable to others.

摘要

溴结构域蛋白是基因转录的关键表观遗传调节剂和组蛋白密码的读取器。然而,由于缺乏合适的化学探针,该靶类别的治疗益处在很大程度上仍未得到探索。本文通过筛选使用结构见解和计算方法选择的片段集,描述了用于 BET 溴结构域的先导分子的产生。对 40 个 BRD2/片段 X 射线复合物的分析突出了共享和不同的相互作用特征,这些特征可用于亲和力和选择性。然后详细举例说明了六个代表性的晶体结构。其中两个片段是完全新颖的溴结构域化学型,三个片段以前从未在溴结构域中结晶,因此我们的结果大大扩展了有限的公开晶体小分子/溴结构域相互作用知识库。某些片段(包括对乙酰氨基酚)以一致的模式与不同的溴结构域(如 CREBBP)结合,这表明它们有可能作为通用的溴结构域模板。一个重要的含义是,溴结构域不仅是一个系统发育家族,而且是一个化学和结构知识在一个溴结构域中可以转移到其他溴结构域的系统。

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