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柯萨奇病毒B3型小鼠心肌炎:基因定义的近交系小鼠心肌炎的病理谱

Coxsackievirus B3 murine myocarditis: a pathologic spectrum of myocarditis in genetically defined inbred strains.

作者信息

Herskowitz A, Wolfgram L J, Rose N R, Beisel K W

出版信息

J Am Coll Cardiol. 1987 Jun;9(6):1311-9. doi: 10.1016/s0735-1097(87)80471-0.

Abstract

Group B coxsackieviruses are the most frequent causative agents in human viral myocarditis. Susceptibility to viral infections varies widely among individuals. In the mouse, coxsackievirus B3 also causes myocarditis. The differential susceptibility of different inbred strains of mice to coxsackie B3-induced myocarditis also appears to be under genetic control. This study details the histopathology of coxsackie B3 myocarditis in six different inbred strains of mice for the first 45 days after coxsackie B3 infection. These strains differ either in the haplotypes of their major histocompatibility complex or in their background genome. During the first 7 days after coxsackie B3 infection, there are dramatic differences among strains with respect to prevalence and severity of myocarditis. Focal zones of myocyte necrosis involving polymorphonuclear leukocytes as well as contraction band injury appear to be the early manifestations of direct viral injury. Four of the six strains, though, continue to show myocardial inflammation after day 9. This late phase myocarditis is characterized by the emergence of mononuclear cells within healing foci of myocyte necrosis as well as a distinctive diffuse interstitial pattern of myocarditis. The strains that develop this late ongoing myocardial inflammation frequently produce heart-specific autoantibodies. Thus the pathologic features of murine coxsackie B3 myocarditis change over the course of the illness, and genetic susceptibility to both early and late phase myocarditis differs markedly among various mouse strains.

摘要

B组柯萨奇病毒是人类病毒性心肌炎最常见的病原体。个体对病毒感染的易感性差异很大。在小鼠中,柯萨奇病毒B3也会引发心肌炎。不同近交系小鼠对柯萨奇B3诱导的心肌炎的易感性差异似乎也受基因控制。本研究详细描述了柯萨奇B3感染后最初45天内,六种不同近交系小鼠的柯萨奇B3心肌炎的组织病理学情况。这些品系在主要组织相容性复合体的单倍型或其背景基因组方面存在差异。在柯萨奇B3感染后的前7天,各品系在心肌炎的患病率和严重程度方面存在显著差异。涉及多形核白细胞的心肌细胞坏死灶以及收缩带损伤似乎是病毒直接损伤的早期表现。然而,六个品系中的四个在第9天后仍继续出现心肌炎症。这种晚期心肌炎的特征是在心肌细胞坏死的愈合灶内出现单核细胞以及一种独特的弥漫性间质性心肌炎模式。发生这种晚期持续性心肌炎症的品系经常产生心脏特异性自身抗体。因此,小鼠柯萨奇B3心肌炎的病理特征在病程中会发生变化,并且不同小鼠品系对早期和晚期心肌炎的遗传易感性存在显著差异。

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