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柯萨奇病毒B4诱导的胰腺病中的宿主因素。

Host factors in Coxsackievirus B4-induced pancreopathy.

作者信息

Cook S H, Loria R M, Madge G E

出版信息

Lab Invest. 1982 Apr;46(4):377-82.

PMID:6279960
Abstract

The diabetogenic potential of the human isolate, Coxsackievirus B4 (CB4) (Edwards) was studied in three inbred mice strains, SWR/J, DBA/2, and C57BL/6. The mice were infected with this agent and evaluated for mortality, pancreatic histopathology, and glucose tolerance. Results showed that the mortality induced by CB4 in these inbred strains differed considerably. There was no evidence of a correlation between virus-induced mortality and virus-induced pancreopathy. Although CB4 (Edwards) was most lethal to C57BL/6 mice, based on the infecting 50 per cent lethal dose (LD50), this mouse strain developed no pancreatic pathology. The most severe pancreopathy, i.e., acinar necrosis with acute interstitial inflammation and islet atrophy, was observed in SWR/J mice, which had an intermediate susceptibility to virus-induced mortality. DBA/2 mice, which displayed the lowest susceptibility to virus-induced lethality, showed less pancreatic pathology (i.e., acute and chronic interstitial inflammation) than SWR/J mice. IN SWR/J mice, virus-mediated alteration in glucose homeostasis was expressed by an increase in glucose tolerance 7 and 21 days after infection. In contrast, C57BL/6 mice showed a tendency toward chemical diabetes at 21 days postinfection. This study suggests that CB4-induced mortality and pancreatic pathology are independent parameters and do not necessarily determine the glucose tolerance of a given host genotype.

摘要

在三种近交系小鼠SWR/J、DBA/2和C57BL/6中研究了人分离株柯萨奇病毒B4(CB4)(爱德华兹株)的致糖尿病潜力。将这些小鼠感染该病原体,并评估其死亡率、胰腺组织病理学和葡萄糖耐量。结果显示,CB4在这些近交系中诱导的死亡率差异很大。没有证据表明病毒诱导的死亡率与病毒诱导的胰腺病变之间存在相关性。尽管基于感染性50%致死剂量(LD50),CB4(爱德华兹株)对C57BL/6小鼠的致死性最强,但该小鼠品系未出现胰腺病理变化。在对病毒诱导的死亡率具有中等易感性的SWR/J小鼠中,观察到最严重的胰腺病变,即腺泡坏死伴急性间质炎症和胰岛萎缩。对病毒诱导的致死性敏感性最低的DBA/2小鼠,其胰腺病变(即急性和慢性间质炎症)比SWR/J小鼠少。在SWR/J小鼠中,感染后7天和21天葡萄糖耐量增加表明病毒介导的葡萄糖稳态改变。相比之下,C57BL/6小鼠在感染后21天表现出化学性糖尿病的倾向。这项研究表明,CB4诱导的死亡率和胰腺病变是独立的参数,不一定决定给定宿主基因型的葡萄糖耐量。

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