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活性中心金属置换诱导的活性抑制和晶体多态性。

Activity inhibition and crystal polymorphism induced by active-site metal swapping.

机构信息

CNRS, AFMB UMR 7257, 13288 Marseille, France.

出版信息

Acta Crystallogr D Struct Biol. 2017 Aug 1;73(Pt 8):641-649. doi: 10.1107/S205979831700866X. Epub 2017 Jul 28.

Abstract

The Arenaviridae family is one of the two RNA viral families that encode a 3'-5' exonuclease in their genome. An exonuclease domain is found in the Arenaviridae nucleoprotein and targets dsRNA specifically. This domain is directly involved in suppression of innate immunity in the host cell. Like most phosphate-processing enzymes, it requires a divalent metal ion such as Mg (or Mn) as a cofactor to catalyse nucleotide-cleavage and nucleotide-transfer reactions. On the other hand, calcium (Ca) inhibits this enzymatic activity, in spite of the fact that Mg and Ca present comparable binding affinities and biological availabilities. Here, the molecular and structural effects of the replacement of magnesium by calcium and its inhibition mechanism for phosphodiester cleavage, an essential reaction in the viral process of innate immunity suppression, are studied. Biochemical data and high-resolution structures of the Mopeia virus exonuclease domain complexed with each ion are reported for the first time. The consequences of the ion swap for the stability of the protein, the catalytic site and the functional role of a specific metal ion in enabling the catalytic cleavage of a dsRNA substrate are outlined.

摘要

沙粒病毒科是编码基因组中 3′-5′外切核酸酶的两种 RNA 病毒家族之一。外切核酸酶结构域存在于沙粒病毒科核蛋白中,可特异性靶向 dsRNA。该结构域直接参与宿主细胞中先天免疫的抑制。与大多数磷酸处理酶一样,它需要二价金属离子(如 Mg(或 Mn))作为辅助因子来催化核苷酸切割和核苷酸转移反应。另一方面,尽管镁和钙具有相当的结合亲和力和生物利用度,但钙抑制了这种酶活性。在这里,研究了钙取代镁及其抑制机制对磷酸二酯键裂解的影响,磷酸二酯键裂解是先天免疫抑制病毒过程中的一个基本反应。首次报道了与每种离子结合的 Mopeia 病毒外切核酸酶结构域的生化数据和高分辨率结构。概述了离子交换对蛋白质稳定性、催化位点以及特定金属离子在使 dsRNA 底物发生催化裂解中的功能作用的影响。

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