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Qβ噬菌体和MS2噬菌体的结构组织对氧化剂次氯酸和过氧亚硝酸盐引起的衣壳蛋白修饰的影响。

Structural Organizations of Qβ and MS2 Phages Affect Capsid Protein Modifications by Oxidants Hypochlorous Acid and Peroxynitrite.

作者信息

Bastin Guillaume, Loison Pauline, Vernex-Loset Lionel, Dupire François, Challant Julie, Majou Didier, Boudaud Nicolas, Krier Gabriel, Gantzer Christophe

机构信息

Université de Lorraine, CNRS, LCPME, Nancy, France.

ACTALIA, Food Safety Department, Saint-Lô, France.

出版信息

Front Microbiol. 2020 Jun 3;11:1157. doi: 10.3389/fmicb.2020.01157. eCollection 2020.

DOI:10.3389/fmicb.2020.01157
PMID:32582098
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7283501/
Abstract

Pathogenic enteric viruses and bacteriophages such as Qβ and MS2 are transmitted through the fecal-oral route. However, oxidants such as peroxynitrite (ONOOH) and hypochlorous acid (HClO) can prevent new infection by inactivating infectious viruses. Their virucidal effect is well recognized, and yet predicting the effects of oxidants on viruses is currently impossible because the detailed mechanisms of viral inactivation remain unclear. Our data show that ONOOH and HClO cross-linked the capsid proteins and RNA genomes of Qβ and MS2 phages. Consistently, the capsids appeared intact by transmission electron microscopy (TEM) even when 99% of the phages were inactivated by oxidation. Moreover, a precise molecular study of the capsid proteins shows that ONOOH and HClO preferentially targeted capsid protein regions containing the oxidant-sensitive amino acid C, Y, or W. Interestingly, the interaction of these amino acids was a crucial parameter defining whether they would be modified by the addition of O, Cl, or NO or whether it induced the loss of the protein region detected by mass spectrometry, together suggesting potential sites for cross-link formation. Together, these data show that HClO and ONOOH consistently target oxidant-sensitive amino acids regardless of the structural organization of Qβ and MS2, even though the phenotypes change as a function of the interaction with adjacent proteins/RNA. These data also indicate a potential novel mechanism of viral inactivation in which cross-linking may impair infectivity.

摘要

致病性肠道病毒和噬菌体,如Qβ和MS2,通过粪-口途径传播。然而,过氧亚硝酸盐(ONOOH)和次氯酸(HClO)等氧化剂可通过使感染性病毒失活来预防新的感染。它们的杀病毒作用已得到充分认识,但目前无法预测氧化剂对病毒的影响,因为病毒失活的详细机制仍不清楚。我们的数据表明,ONOOH和HClO使Qβ和MS2噬菌体的衣壳蛋白和RNA基因组发生交联。一致的是,即使99%的噬菌体因氧化而失活,通过透射电子显微镜(TEM)观察到的衣壳看起来仍然完整。此外,对衣壳蛋白的精确分子研究表明,ONOOH和HClO优先靶向含有对氧化剂敏感的氨基酸C、Y或W的衣壳蛋白区域。有趣的是,这些氨基酸之间的相互作用是一个关键参数,决定了它们是否会因添加O、Cl或NO而被修饰,或者是否会导致质谱检测到的蛋白质区域缺失,这共同表明了交联形成的潜在位点。总之,这些数据表明,HClO和ONOOH始终靶向对氧化剂敏感的氨基酸,而与Qβ和MS2的结构组织无关,尽管表型会随着与相邻蛋白质/RNA的相互作用而变化。这些数据还表明了一种潜在的病毒失活新机制——交联可能会损害感染性。

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