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A Novel Cardiotropic Murine Adenovirus Representing a Distinct Species of Mastadenoviruses

机译:代表不同种类的乳腺腺病毒的新型心型鼠腺病毒。

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摘要

During cell culture isolation experiments to recover Dobrava hantavirus from a suspension of liver from a striped field mouse (Apodemus agrarius), an unknown virus was coisolated. Atypically for hantaviruses, it had extensive cytopathic effects. Using a random PCR approach, it was identified as a novel murine adenovirus, MAdV-3 (for MAdV type 3). A plaque-purified virus clone was prepared and further characterized. The complete genome sequence of MAdV-3 was determined to be 30,570 bp in length. Sequence comparisons to other adenovirus species revealed highest similarity to MAdV-1, the representative of the murine adenovirus A species. However, substantial differences were found in the E1, E3, and E4 genomic regions. The phylogenetic distance of MAdV-3 amino acid sequences for pVIII, protease, polymerase, and hexon from MAdV-1 is markedly higher than 0.1 exchange per position, and, based on our cross-neutralization experiments, MAdV-3 and MAdV-1 can be regarded as different serotypes. Therefore, we propose to classify MAdV-3 as the first isolate of a novel adenovirus species, designated murine adenovirus C (MAdV-C). The novel MAdV-3 virus is not only genetically and serologically distinct from MAdV-1 but also shows a unique organ tropism in infected mice. In contrast to MAdV-1, the virus was not detectable in brain but predominantly infected heart tissue. Thus, infection of mice with cardiotropic MAdV-3 might be an interesting animal model of adenovirus-induced myocarditis.
机译:在进行细胞培养分离实验以从条纹田鼠(Apodemus agrarius)的肝脏悬液中回收Dobrava汉坦病毒时,未知病毒被共分离出来。非典型地对于汉坦病毒,它具有广泛的细胞病变作用。使用随机PCR方法,将其鉴定为新型鼠腺病毒MAdV-3(针对MAdV 3型)。制备噬斑纯化的病毒克隆并进一步表征。确定MAdV-3的完整基因组序列长度为30,570 bp。与其他腺病毒物种的序列比较显示,与鼠腺病毒A物种的代表MAdV-1的相似性最高。但是,在E1,E3和E4基因组区域发现了实质性差异。从MAdV-1到pVIII,蛋白酶,聚合酶和六邻体的MAdV-3氨基酸序列的系统发生距离明显高于每个位置0.1个交换,并且,根据我们的交叉中和实验,MAdV-3和MAdV-1可以被视为不同的血清型。因此,我们建议将MAdV-3分类为新型腺病毒物种的第一个分离株,命名为鼠腺病毒C(MAdV-C)。新型MAdV-3病毒不仅在基因和血清学上不同于MAdV-1,而且在受感染的小鼠中显示出独特的器官嗜性。与MAdV-1相反,该病毒在脑部无法检测到,但主要是感染的心脏组织。因此,心肌病MAdV-3感染小鼠可能是腺病毒诱导的心肌炎的有趣动物模型。

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