基于片段的配体发现中命中生成和结构表征的效率。

Efficiency of hit generation and structural characterization in fragment-based ligand discovery.

机构信息

School of Biological Sciences, Nanyang Technological University, 61 Nanyang Drive, Singapore 639798, Singapore.

出版信息

Curr Opin Chem Biol. 2011 Aug;15(4):482-8. doi: 10.1016/j.cbpa.2011.06.008. Epub 2011 Jul 1.

DOI:10.1016/j.cbpa.2011.06.008

Abstract

Fragment-based ligand discovery constitutes a useful strategy for the generation of high affinity ligands with suitable physico-chemical properties to serve as drug leads. There is an increasing number of generic biophysical screening strategies established with the potential for accelerating the generation of useful fragment hits. Crystal structures of these hits can subsequently be used as starting points for fragment evolution to high affinity ligands. Emerging understanding of the efficiency and operative aspects of hit generation and structural characterization in FBLD suggests that this method should be well suited for academic ligand development of chemical tools and experimental therapeutics.

摘要

基于片段的配体发现是一种有用的策略，可以生成具有合适物理化学性质的高亲和力配体，作为药物先导物。越来越多的通用生物物理筛选策略已经建立起来，具有加速产生有用的片段命中的潜力。这些命中的晶体结构随后可以用作片段进化为高亲和力配体的起点。对 FBLD 中命中生成和结构表征的效率和操作方面的理解表明，该方法应该非常适合化学工具和实验治疗学的学术配体开发。

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基于片段的配体发现中命中生成和结构表征的效率。

Efficiency of hit generation and structural characterization in fragment-based ligand discovery.

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