靶向结核分枝杆菌胸苷单磷酸激酶的取代苄基嘧啶：合成及体外抗分枝杆菌活性

Substituted benzyl-pyrimidines targeting thymidine monophosphate kinase of Mycobacterium tuberculosis: synthesis and in vitro anti-mycobacterial activity.

作者信息

Gasse Cécile, Douguet Dominique, Huteau Valérie, Marchal Gilles, Munier-Lehmann Hélène, Pochet Sylvie

机构信息

Unité de Chimie Organique, CNRS, URA2128, Département Biologie Structurale et Chimie, Institut Pasteur, 28, rue du Dr Roux, 75724 Paris cedex 15, France.

出版信息

Bioorg Med Chem. 2008 Jun 1;16(11):6075-85. doi: 10.1016/j.bmc.2008.04.045. Epub 2008 Apr 25.

DOI:10.1016/j.bmc.2008.04.045

PMID:18467107

Abstract

A series of N(1)-(4-substituted-benzyl)-pyrimidines were synthesized as potential inhibitors of thymidine monophosphate kinase of Mycobacterium tuberculosis (TMPKmt). Key SAR parameters included the chain length substitution in para position of the benzyl ring, the functional group terminating the alkyl chain, and the substituent on the C-5 pyrimidine ring. Synthesized molecules were assayed against both recombinant enzyme and mycobacteria cultures. The most potent compounds have K(i) values in the micromolar range and an MIC(50) of 50microg/mL against Mycobacterium bovis. These results will guide the design of a new generation of lead compounds.

摘要

合成了一系列N(1)-(4-取代苄基)-嘧啶，作为结核分枝杆菌胸苷单磷酸激酶(TMPKmt)的潜在抑制剂。关键的构效关系参数包括苄基环对位的链长取代基、烷基链末端的官能团以及C-5嘧啶环上的取代基。对合成的分子进行了重组酶和分枝杆菌培养物的检测。最有效的化合物的K(i)值在微摩尔范围内，对牛分枝杆菌的MIC(50)为50μg/mL。这些结果将指导新一代先导化合物的设计。

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靶向结核分枝杆菌胸苷单磷酸激酶的取代苄基嘧啶：合成及体外抗分枝杆菌活性

Substituted benzyl-pyrimidines targeting thymidine monophosphate kinase of Mycobacterium tuberculosis: synthesis and in vitro anti-mycobacterial activity.

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