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猪繁殖与呼吸综合征病毒病毒卵巢肿瘤结构域蛋白酶对泛素和干扰素刺激基因产物15的特异性研究

Insights into the Porcine Reproductive and Respiratory Syndrome Virus Viral Ovarian Tumor Domain Protease Specificity for Ubiquitin and Interferon Stimulated Gene Product 15.

作者信息

Bester Stephanie M, Daczkowski Courtney M, Faaberg Kay S, Pegan Scott D

机构信息

Department of Pharmaceutical and Biomedical Sciences , University of Georgia , Athens , Georgia 30602 , United States.

Virus and Prion Research Unit , USDA-ARS-National Animal Disease Center , Ames , Iowa 50010 , United States.

出版信息

ACS Infect Dis. 2018 Sep 14;4(9):1316-1326. doi: 10.1021/acsinfecdis.8b00068. Epub 2018 Jun 12.

Abstract

Porcine reproductive and respiratory syndrome (PRRS) is a widespread economically devastating disease caused by PRRS virus (PRRSV). First recognized in the late 1980s, PRRSV is known to undergo somatic mutations and high frequency viral recombination, which leads to many diverse viral strains. This includes differences within viral virulence factors, such as the viral ovarian tumor domain (vOTU) protease, also referred to as the papain-like protease 2. These proteases down-regulate innate immunity by deubiquitinating proteins targeted by the cell for further processing and potentially also acting against interferon-stimulated genes (ISGs). Recently, vOTUs from vaccine derivative Ingelvac PRRS modified live virus (MLV) and the highly pathogenic PRRSV strain JXwn06 were biochemically characterized, revealing a marked difference in activity toward K63 linked polyubiquitin chains and a limited preference for interferon-stimulated gene product 15 (ISG15) substrates. To extend our research, the vOTUs from NADC31 (low virulence) and SDSU73 (moderately virulent) were biochemically characterized using a myriad of ubiquitin and ISG15 related assays. The K63 polyubiquitin cleavage activity profiles of these vOTUs were found to track with the established pathogenesis of MLV, NADC31, SDSU73, and JXwn06 strains. Fascinatingly, NADC31 demonstrated significantly enhanced activity toward ISG15 substrates compared to its counterparts. Utilizing this information and strain-strain differences within the vOTU encoding region, sites were identified that can modulate K63 polyubiquitin and ISG15 cleavage activities. This information represents the basis for new tools to probe the role of vOTUs in the context of PRRSV pathogenesis.

摘要

猪繁殖与呼吸综合征(PRRS)是由猪繁殖与呼吸综合征病毒(PRRSV)引起的一种广泛传播且具有经济破坏性的疾病。PRRSV于20世纪80年代末首次被发现,已知会发生体细胞突变和高频病毒重组,从而产生许多不同的病毒株。这包括病毒毒力因子的差异,如病毒卵巢肿瘤结构域(vOTU)蛋白酶,也称为木瓜样蛋白酶2。这些蛋白酶通过去泛素化细胞靶向的蛋白质以进行进一步加工,并且可能还作用于干扰素刺激基因(ISG),从而下调先天免疫。最近,对疫苗衍生株英特威PRRS修饰活病毒(MLV)和高致病性PRRSV毒株JXwn06的vOTU进行了生化表征,揭示了它们对K63连接的多聚泛素链的活性存在显著差异,并且对干扰素刺激基因产物15(ISG15)底物的偏好有限。为了扩展我们的研究,使用大量与泛素和ISG15相关的测定方法对NADC31(低毒力)和SDSU73(中等毒力)的vOTU进行了生化表征。发现这些vOTU的K63多聚泛素切割活性谱与已确定的MLV、NADC31、SDSU73和JXwn06毒株的发病机制相符。有趣的是,与其他毒株相比,NADC31对ISG15底物表现出显著增强的活性。利用这些信息以及vOTU编码区域内的毒株差异,确定了可以调节K63多聚泛素和ISG15切割活性的位点。这些信息为探索vOTU在PRRSV发病机制中的作用的新工具奠定了基础。

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