通过基于结构的虚拟筛选方法发现新型苯-1,3-二甲酸对细菌MurD和MurE连接酶的抑制剂

Discovery of novel benzene 1,3-dicarboxylic acid inhibitors of bacterial MurD and MurE ligases by structure-based virtual screening approach.

作者信息

Perdih Andrej, Kovac Andreja, Wolber Gerhard, Blanot Didier, Gobec Stanislav, Solmajer Tom

机构信息

National Institute of Chemistry, Hajdrihova, Ljubljana, Slovenia.

出版信息

Bioorg Med Chem Lett. 2009 May 15;19(10):2668-73. doi: 10.1016/j.bmcl.2009.03.141. Epub 2009 Apr 1.

DOI:10.1016/j.bmcl.2009.03.141

PMID:19369074

Abstract

The peptidoglycan biosynthetic pathway provides an array of potential targets for antibacterial drug design, attractive especially with respect to selective toxicity. Within this pathway, the members of the Mur ligase family are considered as promising emerging targets for novel antibacterial drug design. Based on the available MurD crystal structures co-crystallised with N-sulfonyl glutamic acid inhibitors, a virtual screening campaign was performed, combining three-dimensional structure-based pharmacophores and molecular docking calculations. A novel class of glutamic acid surrogates-benzene 1,3-dicarboxylic acid derivatives-were identified and compounds 14 and 16 found to possess dual MurD and MurE inhibitory activity.

摘要

肽聚糖生物合成途径为抗菌药物设计提供了一系列潜在靶点，特别是在选择性毒性方面具有吸引力。在该途径中，Mur连接酶家族成员被认为是新型抗菌药物设计中很有前景的新兴靶点。基于与N-磺酰谷氨酸抑制剂共结晶的现有MurD晶体结构，开展了一项虚拟筛选活动，结合基于三维结构的药效团和分子对接计算。鉴定出了一类新型谷氨酸替代物——苯-1,3-二羧酸衍生物，发现化合物14和16具有双重MurD和MurE抑制活性。

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通过基于结构的虚拟筛选方法发现新型苯-1,3-二甲酸对细菌MurD和MurE连接酶的抑制剂

Discovery of novel benzene 1,3-dicarboxylic acid inhibitors of bacterial MurD and MurE ligases by structure-based virtual screening approach.

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