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HIV-1整合酶催化结构域游离状态及其与金属辅因子结合状态的晶体结构:活性位点与其他病毒整合酶高度相似。

Crystal structures of the catalytic domain of HIV-1 integrase free and complexed with its metal cofactor: high level of similarity of the active site with other viral integrases.

作者信息

Maignan S, Guilloteau J P, Zhou-Liu Q, Clément-Mella C, Mikol V

机构信息

Rhône-Poulenc Rorer, 13, Quai J. Guesde, Vitry/Seine, F-94403, France.

出版信息

J Mol Biol. 1998 Sep 18;282(2):359-68. doi: 10.1006/jmbi.1998.2002.

DOI:10.1006/jmbi.1998.2002
PMID:9735293
Abstract

Human immunodeficiency virus (HIV) integrase is the enzyme responsible for insertion of a DNA copy of the viral genome into host DNA, an essential step in the replication cycle of HIV. HIV-1 integrase comprises three functional and structural domains: an N-terminal zinc-binding domain, a catalytic core domain and a C-terminal DNA-binding domain. The catalytic core domain with the F185H mutation has been crystallized without sodium cacodylate in a new crystal form, free and complexed with the catalytic metal Mg2+. The structures have been determined and refined to about 2.2 A. Unlike the previously reported structures, the three active-site carboxylate residues (D,D-35-E motif) are well ordered and both aspartate residues delineate a proper metal-binding site. Comparison of the active binding site of this domain with that of other members from the polynucleotidyl transferases superfamily shows a high level of similarity, providing a confident template for the design of antiviral agents.

摘要

人类免疫缺陷病毒(HIV)整合酶是负责将病毒基因组的DNA拷贝插入宿主DNA的酶,这是HIV复制周期中的关键步骤。HIV-1整合酶由三个功能和结构域组成:N端锌结合结构域、催化核心结构域和C端DNA结合结构域。具有F185H突变的催化核心结构域已以一种新的晶体形式在没有二甲胂酸钠的情况下结晶,分别以游离形式以及与催化金属Mg2+结合的形式存在。这些结构已被确定并精修至约2.2埃。与之前报道的结构不同,三个活性位点羧酸盐残基(D、D-35-E基序)排列良好,且两个天冬氨酸残基勾勒出一个合适的金属结合位点。将该结构域的活性结合位点与多核苷酸转移酶超家族的其他成员进行比较,显示出高度的相似性,为抗病毒药物的设计提供了可靠的模板。

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