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甲型肝炎病毒在高静水压下行为的分子基础

Molecular basis of the behavior of hepatitis a virus exposed to high hydrostatic pressure.

作者信息

D'Andrea Lucía, Pérez-Rodríguez Francisco J, Costafreda M Isabel, Beguiristain Nerea, Fuentes Cristina, Aymerich Teresa, Guix Susana, Bosch Albert, Pintó Rosa M

机构信息

Enteric Virus Laboratory, Department of Microbiology, School of Biology, University of Barcelona, Barcelona, Spain Enteric Virus Laboratory, Institute of Nutrition and Food Safety, Campus Torribera, University of Barcelona, Santa Coloma de Gramenet, Spain.

CENTA, IRTA, Monells, Spain.

出版信息

Appl Environ Microbiol. 2014 Oct;80(20):6499-505. doi: 10.1128/AEM.01693-14. Epub 2014 Aug 8.

Abstract

Food-borne hepatitis A outbreaks may be prevented by subjecting foods at risk of virus contamination to moderate treatments of high hydrostatic pressure (HHP). A pretreatment promoting hepatitis A virus (HAV) capsid-folding changes enhances the virucidal effect of HHP, indicating that its efficacy depends on capsid conformation. HAV populations enriched in immature capsids (125S provirions) are more resistant to HHP, suggesting that mature capsids (150S virions) are more susceptible to this treatment. In addition, the monoclonal antibody (MAb) K24F2 epitope contained in the immunodominant site is a key factor for the resistance to HHP. Changes in capsid folding inducing a loss of recognition by MAb K24F2 render more susceptible conformations independently of the origin of such changes. Accordingly, codon usage-associated folding changes and changes stimulated by pH-dependent breathings, provided they confer a loss of recognition by MAb K24F2, induce a higher susceptibility to HHP. In conclusion, the resistance of HAV to HHP treatments may be explained by a low proportion of 150S particles combined with a good accessibility of the epitope contained in the immunodominant site close to the 5-fold axis.

摘要

通过对有病毒污染风险的食品进行适度的高静水压(HHP)处理,可以预防食源性甲型肝炎暴发。促进甲型肝炎病毒(HAV)衣壳折叠变化的预处理可增强HHP的杀病毒效果,这表明其效果取决于衣壳构象。富含未成熟衣壳(125S前病毒体)的HAV群体对HHP更具抗性,这表明成熟衣壳(150S病毒体)对这种处理更敏感。此外,免疫显性位点中包含的单克隆抗体(MAb)K24F2表位是对HHP抗性的关键因素。衣壳折叠的变化导致MAb K24F2识别丧失,从而产生更敏感的构象,而与这种变化的起源无关。因此,密码子使用相关的折叠变化以及pH依赖性呼吸刺激引起且导致MAb K24F2识别丧失的变化,会使病毒对HHP更敏感。总之,HAV对HHP处理的抗性可能是由于150S颗粒比例较低,以及靠近5重轴的免疫显性位点中所含表位具有良好的可及性。

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