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细小病毒非结构蛋白 2 与染色质调节细胞蛋白相互作用。

Parvovirus nonstructural protein 2 interacts with chromatin-regulating cellular proteins.

机构信息

Department of Biological and Environmental Science and Nanoscience Center, University of Jyvaskyla, Jyvaskyla, Finland.

Institute of Biotechnology and Helsinki Institute of Life Science (HiLIFE), University of Helsinki, Helsinki, Finland.

出版信息

PLoS Pathog. 2022 Apr 8;18(4):e1010353. doi: 10.1371/journal.ppat.1010353. eCollection 2022 Apr.

Abstract

Autonomous parvoviruses encode at least two nonstructural proteins, NS1 and NS2. While NS1 is linked to important nuclear processes required for viral replication, much less is known about the role of NS2. Specifically, the function of canine parvovirus (CPV) NS2 has remained undefined. Here we have used proximity-dependent biotin identification (BioID) to screen for nuclear proteins that associate with CPV NS2. Many of these associations were seen both in noninfected and infected cells, however, the major type of interacting proteins shifted from nuclear envelope proteins to chromatin-associated proteins in infected cells. BioID interactions revealed a potential role for NS2 in DNA remodeling and damage response. Studies of mutant viral genomes with truncated forms of the NS2 protein suggested a change in host chromatin accessibility. Moreover, further studies with NS2 mutants indicated that NS2 performs functions that affect the quantity and distribution of proteins linked to DNA damage response. Notably, mutation in the splice donor site of the NS2 led to a preferred formation of small viral replication center foci instead of the large coalescent centers seen in wild-type infection. Collectively, our results provide insights into potential roles of CPV NS2 in controlling chromatin remodeling and DNA damage response during parvoviral replication.

摘要

自主细小病毒至少编码两种非结构蛋白,NS1 和 NS2。虽然 NS1 与病毒复制所需的重要核过程有关,但关于 NS2 的作用知之甚少。具体来说,犬细小病毒 (CPV) NS2 的功能仍然未定义。在这里,我们使用邻近依赖性生物素鉴定 (BioID) 来筛选与 CPV NS2 相关的核蛋白。这些关联在未感染和感染的细胞中都可见,但在感染的细胞中,相互作用的主要类型的蛋白质从核膜蛋白转移到染色质相关蛋白。BioID 相互作用揭示了 NS2 在 DNA 重塑和损伤反应中的潜在作用。具有 NS2 蛋白截断形式的突变病毒基因组研究表明宿主染色质可及性发生了变化。此外,对 NS2 突变体的进一步研究表明,NS2 发挥的功能会影响与 DNA 损伤反应相关的蛋白质的数量和分布。值得注意的是,NS2 剪接受体位点的突变导致小病毒复制中心焦点的形成偏好,而不是野生型感染中所见的大融合中心。总的来说,我们的结果提供了关于 CPV NS2 在控制染色质重塑和细小病毒复制过程中的 DNA 损伤反应方面的潜在作用的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/91dc/9020740/5aa26630e532/ppat.1010353.g001.jpg

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