首页> 美国卫生研究院文献>Veterinary Research >Comparison of the pathogenesis of the highly passaged MCMV Smith strain with that of the low passaged MCMV HaNa1 isolate in BALB/c mice upon oronasal inoculation
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Comparison of the pathogenesis of the highly passaged MCMV Smith strain with that of the low passaged MCMV HaNa1 isolate in BALB/c mice upon oronasal inoculation

机译:经口鼻接种后BALB / c小鼠中高传代MCMV Smith菌株与低传代MCMV HaNa1分离株的发病机理比较

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摘要

Murine cytomegalovirus (MCMV) Smith strain is widely used in mouse models to study HCMV infections. Due to high serial passages, MCMV Smith has acquired genetic and biological changes. Therefore, a low passaged strain would be more relevant to develop mouse models. Here, the pathogenesis of an infection with MCMV Smith was compared with that of an infection with a low passaged Belgian MCMV isolate HaNa1 in BALB/c adult mice following oronasal inoculation with either a low (104 TCID50/mouse) or high (106 TCID50/mouse) inoculation dose. Both strains were mainly replicating in nasal mucosa and submandibular glands for one to two months. In nasal mucosa, MCMV was detected earlier and longer (1–49 days post inoculation (dpi)) and reached higher titers with the high inoculation dose compared to the low inoculation dose (14–35 dpi). In submandibular glands, a similar finding was observed (high dose: 7–49 dpi; low dose: 14–42 dpi). In lungs, both strains showed a restricted replication. In spleen, liver and kidneys, only the Smith strain established a productive infection. The infected cells were identified as olfactory neurons and sustentacular cells in olfactory epithelium, macrophages and dendritic cells in NALT, acinar cells in submandibular glands, and macrophages and epithelial cells in lungs for both strains. Antibody analysis demonstrated for both strains that IgG2a was the main detectable antibody subclass. Overall, our results show that significant phenotypic differences exist between the two strains. MCMV HaNa1 has been shown to be interesting for use in mouse models in order to get better insights for HCMV infections in immunocompetent humans.
机译:鼠巨细胞病毒(MCMV)Smith株广泛用于小鼠模型中,以研究HCMV感染。由于高水平的连续通过,MCMV Smith获得了遗传和生物学的改变。因此,低传代菌株将与开发小鼠模型更相关。在这里,比较了经口鼻接种低剂量(10 4 TCID50 /小鼠)或高(10 6 TCID50 /小鼠)接种剂量。两种菌株主要在鼻粘膜和颌下腺中复制一到两个月。在鼻粘膜中,MCMV的检测时间更早(接种后1–49天(dpi)),高接种剂量的滴度更高,而低接种剂量(14–35 dpi)更高。在下颌下腺中,观察到了类似的发现(高剂量:7–49 dpi;低剂量:14–42 dpi)。在肺中,两种菌株均显示出复制受限。在脾脏,肝脏和肾脏中,只有史密斯毒株才产生生产性感染。对于这两种菌株,感染的细胞被鉴定为嗅觉上皮细胞中的嗅觉神经元和Sustentacular细胞,NALT中的巨噬细胞和树突状细胞,下颌下腺的腺泡细胞以及肺中的巨噬细胞和上皮细胞。两种菌株的抗体分析均表明,IgG2a是可检测的主要抗体亚类。总体而言,我们的结果表明,两种菌株之间存在显着的表型差异。 MCMV HaNa1已被证明可用于小鼠模型,以便更好地了解具有免疫能力的人的HCMV感染。

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