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水泡性口炎病毒基质蛋白抑制小鼠L929细胞中的核因子κB激活。

The vesicular stomatitis virus matrix protein inhibits NF-κB activation in mouse L929 cells.

作者信息

Varble Andrew J, Ried Christopher D, Hammond Warren J, Marquis Kaitlin A, Woodruff Matthew C, Ferran Maureen C

机构信息

Thomas Gosnell School of Life Sciences, Rochester Institute of Technology, Rochester, New York, USA.

Thomas Gosnell School of Life Sciences, Rochester Institute of Technology, Rochester, New York, USA.

出版信息

Virology. 2016 Dec;499:99-104. doi: 10.1016/j.virol.2016.09.009. Epub 2016 Sep 17.

DOI:10.1016/j.virol.2016.09.009
PMID:27643886
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5102766/
Abstract

A previous study found that NF-κB activation is delayed in L929 cells infected with wild-type (wt) strains of VSV, while activation occurred earlier in cells infected with mutant strain T1026R1 (R1) that encodes a mutation in the cytotoxic matrix (M) protein. The integrity of the other R1 proteins is unknown; therefore our goal was to identify the viral component responsible for preventing NF-κB activation in L929 cells. We found that the M protein inhibits viral-mediated activation of NF-κB in the context of viral infection and when expressed alone via transfection, and that the M51R mutation in M abrogates this function. Addition of an IκB kinase (IKK) inhibitor blocked NF-κB activation and interferon-β mRNA expression in cells infected with viruses encoding the M51R mutation in M. These results indicate that the VSV M protein inhibits activation of NF-κB by targeting an event upstream of IKK in the canonical pathway.

摘要

先前的一项研究发现,感染野生型(wt)水疱性口炎病毒(VSV)毒株的L929细胞中NF-κB的激活会延迟,而感染编码细胞毒性基质(M)蛋白突变的突变株T1026R1(R1)的细胞中激活则更早发生。其他R1蛋白的完整性未知;因此,我们的目标是确定负责阻止L929细胞中NF-κB激活的病毒成分。我们发现,M蛋白在病毒感染的情况下以及通过转染单独表达时均能抑制病毒介导的NF-κB激活,并且M中的M51R突变消除了该功能。添加IκB激酶(IKK)抑制剂可阻断感染编码M中M51R突变的病毒的细胞中的NF-κB激活和干扰素-β mRNA表达。这些结果表明,VSV M蛋白通过靶向经典途径中IKK上游的事件来抑制NF-κB的激活。

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