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副粘病毒V蛋白抑制mda-5的机制。

Mechanism of mda-5 Inhibition by paramyxovirus V proteins.

作者信息

Childs K S, Andrejeva J, Randall R E, Goodbourn S

机构信息

Division of Basic Medical Sciences, St. George's, University of London, London SW17 0RE, United Kingdom.

出版信息

J Virol. 2009 Feb;83(3):1465-73. doi: 10.1128/JVI.01768-08. Epub 2008 Nov 19.

DOI:10.1128/JVI.01768-08
PMID:19019954
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2620892/
Abstract

The RNA helicases encoded by melanoma differentiation-associated gene 5 (mda-5) and retinoic acid-inducible gene I (RIG-I) detect foreign cytoplasmic RNA molecules generated during the course of a virus infection, and their activation leads to induction of type I interferon synthesis. Paramyxoviruses limit the amount of interferon produced by infected cells through the action of their V protein, which binds to and inhibits mda-5. Here we show that activation of both mda-5 and RIG-I by double-stranded RNA (dsRNA) leads to the formation of homo-oligomers through self-association of the helicase domains. We identify a region within the helicase domain of mda-5 that is targeted by all paramyxovirus V proteins and demonstrate that they inhibit activation of mda-5 by blocking dsRNA binding and consequent self-association. In addition to this commonly targeted domain, some paramyxovirus V proteins target additional regions of mda-5. In contrast, V proteins cannot bind to RIG-I and consequently have no effect on the ability of RIG-I to bind dsRNA or to form oligomers.

摘要

黑色素瘤分化相关基因5(mda - 5)和视黄酸诱导基因I(RIG - I)编码的RNA解旋酶可检测病毒感染过程中产生的外来细胞质RNA分子,它们的激活会导致I型干扰素合成的诱导。副粘病毒通过其V蛋白的作用限制受感染细胞产生的干扰素量,V蛋白与mda - 5结合并抑制其活性。在此我们表明,双链RNA(dsRNA)对mda - 5和RIG - I的激活会导致解旋酶结构域通过自我缔合形成同型寡聚体。我们确定了mda - 5解旋酶结构域内一个被所有副粘病毒V蛋白靶向的区域,并证明它们通过阻断dsRNA结合及随后的自我缔合来抑制mda - 5的激活。除了这个常见的靶向结构域,一些副粘病毒V蛋白还靶向mda - 5的其他区域。相比之下,V蛋白不能与RIG - I结合,因此对RIG - I结合dsRNA或形成寡聚体的能力没有影响。

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本文引用的文献

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