基于结构的ZipA-FtsZ相互作用的羧基联苯吲哚抑制剂设计。

Structure-based design of carboxybiphenylindole inhibitors of the ZipA-FtsZ interaction.

作者信息

Sutherland Alan G, Alvarez Juan, Ding Weidong, Foreman K W, Kenny Cynthia Hess, Labthavikul Pornpen, Mosyak Lidia, Petersen Peter J, Rush Thomas S, Ruzin Alexey, Tsao Desiree H H, Wheless Karen L

机构信息

Chemical and Screening Sciences, Wyeth Research, Pearl River, NY 10965, USA.

出版信息

Org Biomol Chem. 2003 Dec 7;1(23):4138-40. doi: 10.1039/b312016c. Epub 2003 Oct 29.

DOI:10.1039/b312016c

PMID:14685315

Abstract

Structural features of two weak inhibitors of the ZipA-FtsZ protein-protein interaction which were found to bind to overlapping but different areas of the key binding site were combined in one new series of carboxybiphenyl-indoles with improved inhibitory activity.

摘要

两种ZipA-FtsZ蛋白-蛋白相互作用的弱抑制剂的结构特征被发现可结合到关键结合位点的重叠但不同区域，将这些特征整合到一个新的羧基联苯-吲哚系列中，其抑制活性得到了提高。

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基于结构的ZipA-FtsZ相互作用的羧基联苯吲哚抑制剂设计。

Structure-based design of carboxybiphenylindole inhibitors of the ZipA-FtsZ interaction.

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基于结构的ZipA-FtsZ相互作用的羧基联苯吲哚抑制剂设计。

Structure-based design of carboxybiphenylindole inhibitors of the ZipA-FtsZ interaction.

作者信息

机构信息

出版信息

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