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通过在板上生成和筛选聚焦化合物文库发现志贺毒素 2 型抑制剂。

Discovery of inhibitors of Shiga toxin type 2 by on-plate generation and screening of a focused compound library.

机构信息

Alberta Glycomics Centre, Department of Chemistry, University of Alberta, Edmonton, Alberta T6G 2G2 (Canada) http://www.chem.ualberta.ca/∼glyco/who/index.htm.

出版信息

Angew Chem Int Ed Engl. 2014 Feb 3;53(6):1510-5. doi: 10.1002/anie.201309436. Epub 2014 Jan 22.

Abstract

A new microtiter-plate-based method for the rapid generation and evaluation of focused compound libraries was developed and applied to screening ligand analogues for the E. coli Shiga-like toxin Stx2a. The method is general, it mitigates the masking of intrinsic affinity gains by multivalency and enables the discovery of potential hits when starting from ligands that exhibit extremely low affinity with proteins that depend on multivalency for their function.

摘要

开发了一种新的基于微孔板的快速生成和评估聚焦化合物库的方法,并将其应用于筛选大肠杆菌类志贺毒素 Stx2a 的配体类似物。该方法具有通用性,它可以减轻多价性对固有亲和力增益的掩盖作用,并能够在从与依赖多价性发挥功能的蛋白质亲和力极低的配体开始时发现潜在的命中物。

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