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Genetic Determinants of Virulence between Two Foot-and-Mouth Disease Virus Isolates Which Caused Outbreaks of Differing Severity

机译:导致不同严重程度暴发的两种口蹄疫病毒分离株之间毒力的遗传决定因素

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Individual foot-and-mouth disease virus (FMDV) strains reveal different degrees of infectivity and pathogenicity in host animals. The differences in severity among outbreaks might be ascribable to these differences in infectivity among FMDV strains. To investigate the molecular mechanisms underlying these differences, we estimated the infectivity of O/JPN/2000 and O/JPN/2010, which caused outbreaks of markedly different scales, in cell lines, Holstein cattle, and suckling mice. Viral growth of the two strains in cells was not remarkably different; however, O/JPN/2000 showed apparently low transmissibility in cattle. Mortality rates of suckling mice inoculated intraperitoneally with a 50% tissue culture infective dose (TCIDsub50/sub) of 10 for O/JPN/2000 and O/JPN/2010 also differed, at 0% and 100%, respectively. To identify genes responsible for this difference in infectivity, genetic regions of the full-length cDNA of O/JPN/2010 were replaced with corresponding fragments of O/JPN/2000. A total of eight recombinant viruses were successfully recovered, and suckling mice were intraperitoneally inoculated. Strikingly, recombinants having either VP1 or 3D derived from O/JPN/2000 showed 0% mortality in suckling mice, whereas other recombinants showed 100% mortality. This finding indicates that VP1, the outermost component of the virus particle, and 3D, an RNA-dependent RNA polymerase, are individually involved in the virulence of O/JPN/2010. Three-dimensional structural analysis of VP1 confirmed that amino acid differences between the two strains were located mainly at the domain interacting with the cellular receptor. On the other hand, measurement of their mutation frequencies demonstrated that O/JPN/2000 had higher replication fidelity than O/JPN/2010. IMPORTANCE Efforts to understand the universal mechanism of foot-and-mouth disease virus (FMDV) infection may be aided by knowledge of the molecular mechanisms which underlie differences in virulence beyond multiple topotypes and serotypes of FMDV. Here, we demonstrated independent genetic determinants of two FMDV isolates which have different transmissibility in cattle, namely, VP1 and 3D protein. Findings suggested that the selectivity of VP1 for host cell receptors and replication fidelity during replication were important individual factors in the induction of differences in virulence in the host as well as in the severity of outbreaks in the field. These findings will aid the development of safe live vaccines and antivirals which obstruct viral infection in natural hosts.
机译:个别口蹄疫病毒(FMDV)株在宿主动物中显示出不同程度的感染性和致病性。暴发之间严重程度的差异可能归因于FMDV菌株之间的传染性差异。为了研究导致这些差异的分子机制,我们估算了O / JPN / 2000和O / JPN / 2010的感染性,它们在细胞系,荷斯坦牛和乳鼠中引起了明显不同的规模爆发。两种菌株在细胞中的病毒生长没有显着差异。但是,O / JPN / 2000在牛中显示出明显的低透射率。对于O / JPN / 2000和O / JPN / 2010,腹膜内接种50%组织培养感染剂量(TCID 50 )为10的乳鼠死亡率也有所不同,分别为0%和100%,分别。为了鉴定造成这种传染性差异的基因,将O / JPN / 2010全长cDNA的遗传区域替换为O / JPN / 2000的相应片段。总共成功地回收了八种重组病毒,并腹膜内接种了乳鼠。引人注目的是,具有O / JPN / 2000的VP1或3D的重组体在乳鼠中的死亡率为0%,而其他重组体的死亡率为100%。该发现表明,VP1是病毒颗粒的最外层组件,而3D是RNA依赖性RNA聚合酶,分别与O / JPN / 2010的毒力有关。 VP1的三维结构分析证实,两个菌株之间的氨基酸差异主要位于与细胞受体相互作用的域。另一方面,对它们的突变频率的测量表明,O / JPN / 2000比O / JPN / 2010具有更高的复制保真度。重要信息了解口蹄疫病毒(FMDV)感染的普遍机制的努力,可能是通过了解FMDV多种表型和血清型之外的毒力差异的分子机制来进行的。在这里,我们展示了两种FMDV分离株的独立遗传决定因素,它们在牛中具有不同的传播能力,即VP1和3D蛋白。研究结果表明,VP1对宿主细胞受体的选择性和复制过程中的复制保真度是诱导宿主中毒力差异以及现场暴发严重程度的重要因素。这些发现将有助于开发安全的活疫苗和抗病毒药物,这些疫苗和抗病毒药物会阻碍自然宿主中的病毒感染。

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