HIV integrase: a target for drug discovery

Genes and function Pub Date : 2008-06-28 DOI:10.1046/j.1365-4624.1997.00026.x

Ramon Puras Lutzke, Ronald Plasterk

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引用次数: 10

Abstract

Current antiviral strategies against HIV rely on structure–function analysis of HIV reverse transcriptase (RT) and protease (PR). The third viral pol gene product, HIV integrase (IN), is also a good target for drug discovery, since IN is essential for retroviral replication and, moreover, it has no obvious functional analogue in the host. IN forms a ternary complex with metal ions and DNA and has a mechanism of catalysis common with other polynucleotidyl transferases. Although there is no structural information for full-length IN available, structures of all three functional IN domains have been determined by X-ray crystallography and NMR spectroscopy. The N-terminal domain has a novel zinc-binding fold, the catalytic domain shares a common structural motif with other polynucleotidyl transferases, and the C-terminal DNA-binding domain has a Src-homology-3-like fold. This structural information provides the basis for drug development. In turn, increasing numbers of IN inhibitors identified so far may serve structure–function analysis of IN. The final goal is the development of new classes of anti-HIV drugs, which can be added to the repertoire of anti-RT and anti-PR drugs.

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HIV整合酶:药物发现的靶标

目前针对HIV的抗病毒策略依赖于HIV逆转录酶(RT)和蛋白酶(PR)的结构-功能分析。第三个病毒pol基因产物HIV整合酶(IN)也是一个很好的药物发现靶点，因为IN是逆转录病毒复制所必需的，而且在宿主中没有明显的功能类似物。IN与金属离子和DNA形成三元配合物，具有与其他多核苷酸转移酶相同的催化机制。虽然没有完整的IN结构信息，但所有三个功能IN域的结构已经通过x射线晶体学和核磁共振光谱确定。n端结构域具有新颖的锌结合折叠，催化结构域与其他多核苷酸转移酶具有共同的结构基序，c端dna结合结构域具有src - homology3 -like折叠。这种结构信息为药物开发提供了基础。反过来，到目前为止发现的越来越多的In抑制剂可能用于In的结构-功能分析。最终目标是开发新的抗hiv药物，这些药物可以添加到抗rt和抗pr药物的库中。

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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Genes and function

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