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通过反式互补分析剖析人类免疫缺陷病毒整合酶N端结构域的作用。

Dissecting the role of the N-terminal domain of human immunodeficiency virus integrase by trans-complementation analysis.

作者信息

van den Ent F M, Vos A, Plasterk R H

机构信息

Division of Molecular Biology, The Netherlands Cancer Institute, 1066 CX Amsterdam, The Netherlands.

出版信息

J Virol. 1999 Apr;73(4):3176-83. doi: 10.1128/JVI.73.4.3176-3183.1999.

Abstract

The human immunodeficiency virus (HIV) integrase protein (IN) catalyzes two reactions required to integrate HIV DNA into the human genome: 3' processing of the viral DNA ends and integration. IN has three domains, the N-terminal zinc-binding domain, the catalytic core, and the C-terminal SH3 domain. Previously, it was shown that IN proteins mutated in different domains could complement each other. We now report that this does not require any overlap between the two complementing proteins; an N-terminal domain, provided in trans, can restore IN activity of a mutant lacking this domain. Only the zinc-coordinating form of the N-terminal domain can efficiently restore IN activity of an N-terminal deletion mutant. This suggests that interaction between different domains of IN is needed for functional multimerization. We find that the N-terminal domain of feline immunodeficiency virus IN can support IN activity of an N-terminal deletion mutant of HIV type 2 IN. These cross-complementation experiments indicate that the N-terminal domain contributes to the recognition of specific viral DNA ends.

摘要

人类免疫缺陷病毒(HIV)整合酶蛋白(IN)催化将HIV DNA整合到人类基因组中所需的两个反应:病毒DNA末端的3'加工和整合。IN有三个结构域,即N端锌结合结构域、催化核心和C端SH3结构域。此前研究表明,在不同结构域发生突变的IN蛋白可以相互互补。我们现在报告,这并不要求两个互补蛋白之间有任何重叠;以反式提供的N端结构域可以恢复缺乏该结构域的突变体的IN活性。只有N端结构域的锌配位形式才能有效地恢复N端缺失突变体的IN活性。这表明IN不同结构域之间的相互作用对于功能性多聚化是必需的。我们发现猫免疫缺陷病毒IN的N端结构域可以支持2型HIV IN的N端缺失突变体的IN活性。这些交叉互补实验表明,N端结构域有助于识别特定的病毒DNA末端。

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HIV integrase: a target for drug discovery.HIV整合酶:药物研发的靶点。
Genes Funct. 1997 Dec;1(5-6):289-307. doi: 10.1046/j.1365-4624.1997.00026.x.
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