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HIV整合的分子机制与治疗干预

Molecular mechanisms of HIV integration and therapeutic intervention.

作者信息

Vandegraaff Nick, Engelman Alan

机构信息

Avexa Limited, Richmond, Victoria 3121, Australia.

出版信息

Expert Rev Mol Med. 2007 Feb 26;9(6):1-19. doi: 10.1017/S1462399407000257.

Abstract

Retroviruses, such as human immunodeficiency virus type 1 (HIV-1), are plus-sense RNA viruses that require reverse transcription and then DNA integration to establish a chromosomal provirus as an obligate replication intermediate. The viral enzyme reverse transcriptase synthesises linear double-stranded cDNA, which is the template for the viral enzyme integrase. Integrase catalyses two separate chemical reactions: an initial 3' processing of the nascent cDNA ends, which is followed in the cell nucleus by their covalent attachment to the 5' phosphates of a double-stranded staggered cut in chromosomal DNA. As integrase activity is essential for productive retroviral infection, there is intense interest in developing small-molecule inhibitors of the HIV-1 enzyme to increase the breadth of the antiviral arsenal used to fight HIV/AIDS. Purified integrase protein displays the 3' processing and DNA-strand-transfer activities essential for cDNA integration in integration assays in vitro, but numerous studies indicate that cellular proteins play important roles during integration in infected cells. This review highlights the molecular mechanisms behind HIV-1 integration, focusing on recent insights into functions of human cellular cofactors. The progress towards developing integrase inhibitors for their use in the clinic is also reviewed.

摘要

逆转录病毒,如1型人类免疫缺陷病毒(HIV-1),是正义RNA病毒,它们需要逆转录,然后进行DNA整合,以建立染色体前病毒作为必需的复制中间体。病毒酶逆转录酶合成线性双链cDNA,它是病毒酶整合酶的模板。整合酶催化两个独立的化学反应:新生cDNA末端的初始3'加工,随后在细胞核中它们与染色体DNA双链交错切口的5'磷酸共价连接。由于整合酶活性对于逆转录病毒的有效感染至关重要,因此人们对开发HIV-1酶的小分子抑制剂以增加用于对抗HIV/AIDS的抗病毒武器库的广度有着浓厚的兴趣。纯化的整合酶蛋白在体外整合测定中显示出cDNA整合所必需的3'加工和DNA链转移活性,但大量研究表明细胞蛋白在受感染细胞的整合过程中发挥着重要作用。本综述重点介绍了HIV-1整合背后的分子机制,着重于对人类细胞辅助因子功能的最新见解。还综述了开发整合酶抑制剂用于临床的进展情况。

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