Identification of Novel Human Immunodeficiency Virus-1 Integrase Inhibitors by Shape-Based Virtual Screening

American medical journal Pub Date : 2010-12-31 DOI:10.3844/AMJSP.2010.151.156

T. Omprakash, A. Selvan, A. Hameed, S. Geetha

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引用次数: 2

Abstract

Abstract: Problem statement: Human Immunodeficiency Virus-1 (HIV-1) is causative agent of the immune system disease, Acquired Immune Deficiency Syndrome (AIDS). Majority of anti-HIV drugs target reverse transcriptase and protease enzymes. Toxicity and development of multidrug resistant HIV-1 virus strains are the reasons for studying new targets in HIV-1 replication process for identifying novel inhibitor with low toxicity and high activity. Approach: In this study, ROCS software was used to identify the novel HIV-1 Integrase (HIV-1 IN) inhibitor by shape-based virtual screening. The currently used drug raltegravir was used as query molecule. Results: Here five novel molecules were identified, among them Rank 5 molecule was shown to have higher structural and electrostatic similarity to query molecule and this molecule was considered as good inhibitor of HIV-1 IN enzyme. Conclusion: ROCS, EON and FRED effectively identified one active inhibitor of HIV-1 IN among five compounds, which was similar to the query molecule and this study showed that ROCS, EON and FRED can play a vital role in drug discovery projects.

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基于形状的虚拟筛选鉴定新型人类免疫缺陷病毒-1整合酶抑制剂

摘要:问题陈述:人类免疫缺陷病毒-1 (HIV-1)是免疫系统疾病获得性免疫缺陷综合征(AIDS)的病原体。大多数抗hiv药物靶向逆转录酶和蛋白酶。HIV-1病毒毒株的毒性和多药耐药的发展是研究HIV-1复制过程中的新靶点，以寻找低毒高活性的新型抑制剂的原因。方法:在本研究中，使用ROCS软件通过基于形状的虚拟筛选来鉴定新型HIV-1整合酶(HIV-1 In)抑制剂。以目前使用的药物雷替格拉韦作为查询分子。结果:共鉴定出5个新分子，其中Rank 5分子与查询分子具有较高的结构和静电相似性，该分子被认为是HIV-1 IN酶的良好抑制剂。结论:ROCS、EON和FRED在5个化合物中有效鉴定出一种HIV-1 IN活性抑制剂，该抑制剂与查询分子相似，本研究表明ROCS、EON和FRED在药物发现项目中发挥重要作用。

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American medical journal

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