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In Vivo Tropism of Attenuated and Pathogenic Measles Virus Expressing Green Fluorescent Protein in Macaques

机译:在猕猴中表达绿色荧光蛋白的减毒和致病性麻疹病毒的体内取向

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摘要

The global increase in measles vaccination has resulted in a significant reduction of measles mortality. The standard route of administration for the live-attenuated measles virus (MV) vaccine is subcutaneous injection, although alternative needle-free routes, including aerosol delivery, are under investigation. In vitro, attenuated MV has a much wider tropism than clinical isolates, as it can use both CD46 and CD150 as cellular receptors. To compare the in vivo tropism of attenuated and pathogenic MV, we infected cynomolgus macaques with pathogenic or attenuated recombinant MV expressing enhanced green fluorescent protein (GFP) (strains IC323 and Edmonston, respectively) via the intratracheal or aerosol route. Surprisingly, viral loads and cellular tropism in the lungs were similar for the two viruses regardless of the route of administration, and CD11c-positive cells were identified as the major target population. However, only the pathogenic MV caused significant viremia, which resulted in massive virus replication in B and T lymphocytes in lymphoid tissues and viral dissemination to the skin and the submucosa of respiratory epithelia. Attenuated MV was rarely detected in lymphoid tissues, and when it was, only in isolated infected cells. Following aerosol inhalation, attenuated MV was detected at early time points in the upper respiratory tract, suggesting local virus replication. This contrasts with pathogenic MV, which invaded the upper respiratory tract only after the onset of viremia. This study shows that despite in vitro differences, attenuated and pathogenic MV show highly similar in vivo tropism in the lungs. However, systemic spread of attenuated MV is restricted.
机译:麻疹疫苗接种的全球增加导致了麻疹死亡率的显着降低。减毒活麻疹病毒(MV)疫苗的标准给药途径是皮下注射,尽管正在研究包括气雾剂输送在内的其他无针途径。在体外,减毒MV具有比临床分离株更广泛的向性,因为它可以同时使用CD46和CD150作为细胞受体。为了比较减毒和致病性MV的体内嗜性,我们通过气管内或气溶胶途径用表达增强型绿色荧光蛋白(GFP)(分别为菌株IC323和Edmonston)的致病性或减毒重组MV感染食蟹猕猴。出乎意料的是,无论给药途径如何,两种病毒的肺部病毒载量和细胞向性相似,并且CD11c阳性细胞被确定为主要目标人群。然而,仅致病性MV引起明显的病毒血症,其导致淋巴组织中的B和T淋巴细胞中大量病毒复制以及病毒扩散至呼吸道上皮的皮肤和粘膜下层。很少在淋巴组织中检测到减毒的MV,而当其出现时,仅在分离的感染细胞中检测到。气雾剂吸入后,在上呼吸道的早期时间点检测到MV降低,表明局部病毒复制。这与致病性MV相反,致病性MV仅在病毒血症发作后才侵入上呼吸道。这项研究表明,尽管在体外存在差异,但减毒和致病性MV在肺中显示出高度相似的体内趋向性。但是,减毒MV的全身扩散受到限制。

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