分子特征表明,在新城疫病毒感染的DF1细胞中,副病毒蛋白W的表达受到动力学调节。

Q2 Medicine VirusDisease Pub Date : 2023-06-01 Epub Date: 2023-05-02 DOI:10.1007/s13337-023-00813-2
B Nagaraj Nayak, Kalaimagal Rajagopal, Revathi Shunmugasundaram, Pachineella Lakshmana Rao, Saraswathy Vaidyanathan, Madhuri Subbiah
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引用次数: 0

摘要

病毒采用策略来有效利用其紧凑的基因组。副粘病毒科的成员表现出共转录RNA编辑机制,其中聚合酶口吃从磷蛋白(P)基因产生辅助蛋白。新城疫病毒(NDV)是一种鸟类副粘病毒,通过RNA编辑表达V和W两种辅助蛋白。虽然P和V蛋白已经得到了很好的研究,但对W蛋白知之甚少。最近的研究证实了W蛋白在新冠病毒中的表达以及强毒和弱毒新冠病毒W蛋白的独特亚细胞定位。我们对NDV科马罗夫株的W蛋白进行了鉴定。科马罗夫是一株中等毒力的疫苗株。W mRNA的表达范围在总P基因转录物的7%至9%之间,类似于强毒NDV。然而,在DF1细胞中,可在6小时检测到的W蛋白表达在感染后24小时达到峰值,并在48小时下降,这表明病毒在动力学上调节了表达。W蛋白定位在细胞核中,通过突变,在W蛋白的C末端区域鉴定出强烈的细胞核定位信号。病毒生长动力学研究表明,无论是补充W蛋白还是补充W蛋白的亚细胞定位模式,都不会影响病毒在体外的复制,类似于在无毒NDV中发现的情况。一种定位于细胞质中的W蛋白细胞质突变体,不同于速度原性NDV菌株SG10中记录的特异性线粒体共定位,表明W蛋白可能在决定病毒致病性中发挥作用。本研究首次描述了中等毒力新冠病毒W蛋白的独特特征。补充信息:在线版本包含补充材料,可访问10.1007/s13337-023-00813-2。
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Molecular characterization suggests kinetic modulation of expression of accessory viral protein, W, in Newcastle disease virus infected DF1 cells.

Viruses adopt strategies to efficiently utilize their compact genome. Members of the family Paramyxoviridae, exhibit a cotranscriptional RNA editing mechanism wherein polymerase stuttering generates accessory proteins from Phosphoprotein (P) gene. Newcastle disease virus (NDV), an avian paramyxovirus, expresses two accessory proteins, V and W, by RNA editing. While P and V proteins are well studied, very little is known about W protein. Recent studies confirmed W protein expression in NDV and the unique subcellular localization of W proteins of virulent and avirulent NDV. We characterized the W protein of NDV strain Komarov, a moderately virulent vaccine strain. W mRNA expression ranged between 7 and 9% of total P gene transcripts similar to virulent NDV. However, W protein expression, detectable by 6 h, peaked at 24 h and dropped by 48 h post infection in DF1 cells indicating a kinetically regulated expression by the virus. The W protein localized in the nucleus and by mutations, a strong nuclear localization signal was identified in the C-terminal region of W protein. The viral growth kinetics study suggested neither supplementation of W protein nor subcellular localization pattern of the supplemented W protein influenced viral replication in vitro similar to that noticed in avirulent NDV. A cytoplasmic mutant of W protein localized in cytoplasm unlike specific mitochondrial colocalization as recorded in velogenic NDV strain SG10 indicating a possible role of W protein in determining the viral pathogenicity. This study describes for the first time, the distinct features of W protein of moderately virulent NDV.

Supplementary information: The online version contains supplementary material available at 10.1007/s13337-023-00813-2.

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来源期刊
VirusDisease
VirusDisease Medicine-Infectious Diseases
CiteScore
7.00
自引率
0.00%
发文量
46
期刊介绍: VirusDisease, formerly known as ''Indian Journal of Virology'', publishes original research on all aspects of viruses infecting animal, human, plant, fish and other living organisms.
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