Design, synthesis, molecular dynamics studies and biological evaluations of 4-hydroxy-5-pyrrolinone-3-carbohydrazides as HIV-1 integrase inhibitors

European Journal of Medicinal Chemistry Reports Pub Date : 2024-08-20 DOI:10.1016/j.ejmcr.2024.100208

Nafiseh Karimi , Amirreza Dowlati Beirami , Rouhollah Vahabpour Roudsari , Zahra Hajimahdi , Afshin Zarghi

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引用次数: 0

Abstract

Acquired immune deficiency syndrome (AIDS) diseases despite the efficacy of anti-HIV therapy, remain one of the human's most serious problems. Hence, the introduction of novel anti-HIV agents as first-line therapy is still required. HIV integrase lacking human enzyme homologous is an interesting target for developing new anti-HIV drugs. Following our attempts to describe active integrase inhibitor structures, here a series of novel 4-Hydroxy-5-pyrrolinone-3-carbohydrazides as HIV integrase inhibitor agents were identified. Biological results showed that all compounds could inhibit integrase strand transfer reaction and also exhibited anti-HIV activity in a cell-based assay. The interaction between integrase and designed compounds was investigated using molecular docking and molecular dynamics simulations.

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作为 HIV-1 整合酶抑制剂的 4-hydroxy-5-pyrrolinone-3-carbohydraides 的设计、合成、分子动力学研究和生物学评价

尽管抗艾滋病毒疗法很有效，但获得性免疫缺陷综合征（艾滋病）疾病仍然是人类最严重的问题之一。因此，仍然需要引入新型抗艾滋病毒药物作为一线疗法。缺乏人类同源酶的艾滋病毒整合酶是开发新型抗艾滋病毒药物的一个有趣靶点。继我们尝试描述活性整合酶抑制剂结构之后，这里又发现了一系列新型 4-羟基-5-吡咯烷酮-3-甲酰肼作为 HIV 整合酶抑制剂。生物学结果表明，所有化合物都能抑制整合酶链转移反应，并在基于细胞的试验中表现出抗艾滋病毒活性。利用分子对接和分子动力学模拟研究了整合酶与所设计化合物之间的相互作用。

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来源期刊

European Journal of Medicinal Chemistry Reports

CiteScore

4.50

自引率

0.00%

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