Synthesis and Inhibiting Activity of Some 4-Hydroxycoumarin Derivatives on HIV-1 Protease.

ISRN Pharmaceutics Pub Date : 2011-01-01 Epub Date: 2011-07-26 DOI:10.5402/2011/137637

Stancho Stanchev, Frank Jensen, Anton Hinkov, Vasil Atanasov, Petia Genova-Kalou, Radka Argirova, Ilia Manolov

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引用次数: 12

Abstract

Six novel 4-hydroxycoumarin derivatives were rationally synthesized, verified, and characterized by molecular docking using crystal HIV-1 protease. Molecular docking studies predicted antiprotease activity of (7) and (10). The most significant functional groups, responsible for the interaction with HIV-1 protease by hydrogen bonds formation are pyran oxygen, atom, lactone carbonyl oxygen and one of the hydroxyl groups. The newly synthesized compounds were biologically tested in MT-4 cells for inhibiting HIV-1 replication, exploring the protection of cells from the cytopathic effect of HIV measured by cell survival in MTT test. One derivative -7 showed 76-78% inhibition of virus infectivity with IC(50) = 0.01 nM, much less than the maximal nontoxic concentration (1 mM). Antiprotease activity of 7 in two different concentrations was detected to be 25%. Nevertheless, the results of study of (7) encourage using it as a pharmacophore for further synthesis and evaluation of anti-HIV activity.

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一些4-羟基香豆素衍生物的合成及其对HIV-1蛋白酶的抑制活性

利用晶体HIV-1蛋白酶合理合成了6个新型4-羟基香豆素衍生物，并对其进行了分子对接验证。分子对接研究预测了(7)和(10)的抗蛋白酶活性。通过氢键形成与HIV-1蛋白酶相互作用的最重要的官能团是吡喃氧、原子、内酯羰基氧和一个羟基。新合成的化合物在MT-4细胞中进行了抑制HIV-1复制的生物学测试，探讨了MTT测试中细胞存活率测量的HIV细胞病变效应对细胞的保护作用。其中衍生物-7在IC(50) = 0.01 nM时，对病毒感染的抑制率为76-78%，远低于最大无毒浓度(1 mM)。7在两种不同浓度下的抗蛋白酶活性均为25%。尽管如此，(7)的研究结果鼓励将其作为药效团进一步合成和评价抗hiv活性。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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ISRN Pharmaceutics

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