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A field strain of minute virus of mice (MVMm) exhibits age- and strain-specific pathogenesis

机译:小鼠微小病毒野毒株(MVMm)表现出年龄和毒株特异性发病机理

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摘要

The influence of mouse strain, immune competence and age on the pathogenesis of a field strain of minute virus of mice (MVMm) was examined in BALB/c, C3H, C57BL/6 and SCID mice experimentally infected as neonates, weanlings and adults. Sera, bodily excretions and tissues were harvested at 7, 14, 28 and 56 days after inoculation and evaluated by serology, quantitative PCR and histopathology. Seroconversion to recombinant viral capsid protein 2 was consistently observed in all immunocompetent strains of mice, regardless of the age at which they were inoculated, while seroconversion to the viral nonstructural protein 1 was only consistently detected in neonate inoculates. Viral DNA was detected by quantitative PCR in multiple tissues of immunocompetent mice at each time point after inoculation, with the highest levels being observed in neonate inoculates at 7 days after inoculation. In contrast, viral DNA levels in tissues and bodily excretions increased consistently over time in immunodeficient SCID mice, regardless of the age at which they were inoculated, with mortality being observed in neonatal inoculates between 28 and 56 days after inoculation. Overall, productive infection was observed more frequently in immunocompetent mice inoculated as neonates as compared to those inoculated as weanlings or adults, and immunodeficient SCID mice developed persistent, progressive infection, with mortality being observed in mice inoculated as neonates. Importantly, the clinical syndrome observed in experimentally infected SCID neonatal mice recapitulates the clinical presentation reported for the naturally infected immunodeficient NOD µ-chain knockout mice from which MVMm was initially isolated.
机译:在实验感染新生儿,断奶和成年的BALB / c,C3H,C57BL / 6和SCID小鼠中,研究了小鼠品系,免疫能力和年龄对微小病毒田间株(MVMm)发病机理的影响。接种后第7、14、28和56天收集血清,身体排泄物和组织,并通过血清学,定量PCR和组织病理学进行评估。在所有具有免疫能力的小鼠品系中,始终观察到血清向重组病毒衣壳蛋白2的血清转化,无论它们接种的年龄如何,而仅在新生儿接种物中始终检测到向病毒非结构蛋白1的血清素转化。在接种后的每个时间点通过免疫反应小鼠的多个组织中的定量PCR检测病毒DNA,在接种后7天时观察到最高水平的新生儿接种。相比之下,免疫缺陷SCID小鼠的组织和身体排泄物中的病毒DNA水平随着时间的推移持续增加,而与接种年龄无关,在接种后28至56天之间观察到新生儿接种时的死亡率。总体而言,与作为断奶或成年疫苗接种的免疫能力强的小鼠相比,在具有免疫能力的小鼠中更频繁地观察到生产性感染,并且免疫缺陷的SCID小鼠发展为持续性进行性感染,在作为新生小鼠的小鼠中观察到死亡率。重要的是,在实验感染的SCID新生小鼠中观察到的临床综合征概括了最初从中分离出MVMm的自然感染的免疫缺陷NOD µ链敲除小鼠的临床表现。

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