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基于晶体学片段的药物发现:使用针对HIV蛋白酶的溴化片段文库。

Crystallographic fragment-based drug discovery: use of a brominated fragment library targeting HIV protease.

作者信息

Tiefenbrunn Theresa, Forli Stefano, Happer Meaghan, Gonzalez Ana, Tsai Yingssu, Soltis Michael, Elder John H, Olson Arthur J, Stout Charles D

机构信息

Department of Integrative Computational and Structural Biology, TSRI, 10550 N. Torrey Pines Rd., La Jolla, CA, USA.

出版信息

Chem Biol Drug Des. 2014 Feb;83(2):141-8. doi: 10.1111/cbdd.12227. Epub 2013 Oct 30.

Abstract

A library of 68 brominated fragments was screened against a new crystal form of inhibited HIV-1 protease in order to probe surface sites in soaking experiments. Often, fragments are weak binders with partial occupancy, resulting in weak, difficult-to-fit electron density. The use of a brominated fragment library addresses this challenge, as bromine can be located unequivocally via anomalous scattering. Data collection was carried out in an automated fashion using AutoDrug at SSRL. Novel hits were identified in the known surface sites: 3-bromo-2,6-dimethoxybenzoic acid (Br6) in the flap site and 1-bromo-2-naphthoic acid (Br27) in the exosite, expanding the chemistry of known fragments for development of higher affinity potential allosteric inhibitors. At the same time, mapping the binding sites of a number of weaker binding Br-fragments provides further insight into the nature of these surface pockets.

摘要

为了在浸泡实验中探测表面位点,针对一种新晶型的抑制型HIV-1蛋白酶筛选了一个包含68个溴化片段的文库。通常,片段是弱结合剂,占有率较低,导致电子密度弱且难以拟合。使用溴化片段文库解决了这一挑战,因为溴可以通过反常散射明确定位。数据收集在SSRL使用AutoDrug以自动化方式进行。在已知表面位点鉴定出了新的命中片段:在翼片位点的3-溴-2,6-二甲氧基苯甲酸(Br6)和在外位点的1-溴-2-萘甲酸(Br27),扩展了用于开发具有更高亲和力的潜在变构抑制剂的已知片段的化学结构。同时,绘制许多较弱结合的Br-片段的结合位点,可进一步深入了解这些表面口袋的性质。

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