首页> 外文期刊>The journal of immunology >Severe Focal Sialadenitis and Dacryoadenitis in NZM2328 Mice Induced by MCMV: A Novel Model for Human Sj?gren’s Syndrome
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Severe Focal Sialadenitis and Dacryoadenitis in NZM2328 Mice Induced by MCMV: A Novel Model for Human Sj?gren’s Syndrome

机译:MCMV诱导的NZM2328小鼠中的严重局灶性涎腺炎和泪腺炎:一种人类干燥综合征的新型模型

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The genetic and environmental factors that control the development of Sj?gren’s syndrome, an autoimmune disease mainly involving the salivary and lacrimal glands, are poorly understood. Viruses which infect the glands may act as a trigger for disease. The ability of sialotropic murine CMV (MCMV) to induce acute and chronic glandular disease was characterized in an autoimmune-prone mouse strain, NZM2328. MCMV levels were detectable in the salivary and lacrimal glands 14–28 days after i.p. infection and correlated with acute inflammation in the submandibular gland. After latency, virus was undetectable in the glands by PCR. At this stage, NZM2328 female mice developed severe chronic periductal inflammation in both submandibular and lacrimal glands in contrast to the much milder infiltrates found in female B6- lpr and male NZM2328. The focal infiltrates consisted of CD4+ and B220+ cells as opposed to diffuse CD4+, CD8+, and B220+ cells during acute infection. Salivary gland functional studies revealed a gender-specific progressive loss of secretory function between days 90 and 125 postinfection. Latent MCMV infection did not significantly affect the low incidence of autoantibodies to Ro/SSA and La/SSB Ags in NZM2328 mice. However, reactivities to other salivary and lacrimal gland proteins were readily detected. MCMV infection did not significantly alter the spontaneous onset of kidney disease in NZM2328. Thus, chronic inflammation induced by MCMV with decreased secretory function in NZM2328 mice resembles the disease manifestations of human Sj?gren’s syndrome.
机译:控制Sj?gren综合征(一种主要涉及唾液和泪腺的自身免疫性疾病)发展的遗传和环境因素知之甚少。感染腺体的病毒可能会引发疾病。在易发自身免疫的小鼠品系NZM2328中表征了唾液嗜性小鼠CMV(MCMV)诱发急性和慢性腺体疾病的能力。腹腔镜手术后14-28天,唾液和泪腺中可检测到MCMV水平。感染并与下颌下腺的急性炎症相关。潜伏期后,通过PCR无法在腺体中检测到病毒。在这一阶段,与雌性B6-lpr和雄性NZM2328中发现的温和得多的浸润相比,NZM2328雌性小鼠在颌下和泪腺均出现了严重的慢性导管周围炎症。在急性感染期间,病灶浸润由CD4 +和B220 +细胞组成,与弥漫性CD4 +,CD8 +和B220 +细胞相反。唾液腺功能研究表明,感染后90至125天之间,性别特异性分泌功能逐渐丧失。潜伏的MCMV感染并未显着影响NZM2328小鼠中针对Ro / SSA和La / SSB Ags的自身抗体的低发生率。但是,很容易检测到对其他唾液和泪腺蛋白的反应性。 MCMV感染并未显着改变NZM2328中肾脏疾病的自发发作。因此,由NZM2328小鼠分泌功能降低的MCMV诱发的慢性炎症类似于人类干燥综合征的疾病表现。

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