环取代喹啉羧酸/酯类似物的合成及其抗分枝杆菌活性。第1部分。

Synthesis and antimycobacterial activities of ring-substituted quinolinecarboxylic acid/ester analogues. Part 1.

作者信息

Vaitilingam Balasubramanian, Nayyar Amit, Palde Prakash B, Monga Vikramdeep, Jain Rahul, Kaur Sukhraj, Singh Prati Pal

机构信息

Department of Medicinal Chemistry, National Institute of Pharmaceutical Education and Research, Sector 67, SAS Nagar, Punjab 160 062, India.

出版信息

Bioorg Med Chem. 2004 Aug 1;12(15):4179-88. doi: 10.1016/j.bmc.2004.05.018.

DOI:10.1016/j.bmc.2004.05.018

PMID:15246094

Abstract

Structural optimization of recently discovered new chemical entity, 2,8-dicyclopentyl-4-methylquinoline (DCMQ; MIC= 6.25 microg/mL, M. tuberculosis H37Rv) resulted in the synthesis of four new series of ring-substituted quinolinecarboxylic acids/esters constituting 45 analogues. All new derivatives were evaluated for in vitro antimycobacterial activities against M. tuberculosis H37Rv. Certain ring-substituted-2-quinolinecarboxylic acid ester and ring-substituted-2-quinoline acetic acid ester analogues described herein showed moderate to good inhibitory activity. In particular, three analogues methyl 4,5-dicyclopentyl-2-quinolinecarboxylate (3b), methyl 4,8-dicyclopentyl-2-quinolinecarboxylate (3c) and ethyl 2-(2,8-dicyclopentyl-4-quinolyl)acetate (14g) exhibited excellent MIC values of 1.00, 2.00 and 4.00microg/mL, respectively. Results obtained indicate that substitution of the quinoline ring with dicyclopentyl substituent presumably enhances the antimycobacterial activities in the quinoline analogues described herein.

摘要

对最近发现的新化学实体2,8 - 二环戊基 - 4 - 甲基喹啉（DCMQ；对结核分枝杆菌H37Rv的最低抑菌浓度（MIC）= 6.25微克/毫升）进行结构优化，合成了四个新系列的环取代喹啉羧酸/酯，共45个类似物。对所有新衍生物进行了针对结核分枝杆菌H37Rv的体外抗分枝杆菌活性评估。本文所述的某些环取代 - 2 - 喹啉羧酸酯和环取代 - 2 - 喹啉乙酸酯类似物表现出中度至良好的抑制活性。特别是，三个类似物4,5 - 二环戊基 - 2 - 喹啉羧酸甲酯（3b）、4,8 - 二环戊基 - 2 - 喹啉羧酸甲酯（3c）和2 - (2,8 - 二环戊基 - 4 - 喹啉基)乙酸乙酯（14g）分别表现出优异的最低抑菌浓度值，为1.00、2.00和4.00微克/毫升。所得结果表明，用二环戊基取代基取代喹啉环可能会增强本文所述喹啉类似物的抗分枝杆菌活性。

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环取代喹啉羧酸/酯类似物的合成及其抗分枝杆菌活性。第1部分。

Synthesis and antimycobacterial activities of ring-substituted quinolinecarboxylic acid/ester analogues. Part 1.

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