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由鼠冠状病毒JHM株在BALB/cHeA和STS/A小鼠之间的一系列重组近交系中诱发的急性和晚期疾病。

Acute and late disease induced by murine coronavirus, strain JHM, in a series of recombinant inbred strains between BALB/cHeA and STS/A mice.

作者信息

Kyuwa S, Yamaguchi K, Toyoda Y, Fujiwara K, Hilgers J

机构信息

Department of Animal Pathology, University of Tokyo, Japan.

出版信息

Microb Pathog. 1992 Feb;12(2):95-104. doi: 10.1016/0882-4010(92)90112-2.

Abstract

To examine the genetic control of acute and late disease induced by a murine coronavirus, strain JHM (JHMV), BALB/cHeA, STS/A, F1 hybrids and 13 recombinant inbred (RI) strains between BALB/cHeA and STS/A mouse strains were inoculated intracerebrally with 100 pfu of JHMV. All the BALB/cHeA mice died within 2 weeks from acute encephalitis. In contrast, STS/A mice were shown to be partially resistant, with a mortality rate of 30%, longer survival times and lower rates of viral production. The mortality rates, survival times and viral titers of F1 hybrids and the RI strains varied, suggesting involvement of multiple genes. STS/A, F1 hybrid and RI mice surviving the acute infection occasionally developed severe paraparesis about 1 month post-infection. In these mice, vacuolar degeneration, astrocytosis, the absence of perivascular cuffing and minimal demyelination were found in the central nervous system. No infectious virus could be recovered from these mice. Although the paralysis of delayed onset was limited to STS/A, F1 hybrid and eight of the 13 RI strains, the incidence varied significantly among the RI strains. These results may suggest that JHMV-induced late disease is also under multifactorial control. The pathogenesis of JHMV infection is discussed.

摘要

为研究鼠冠状病毒JHM株(JHMV)诱导的急性和迟发性疾病的遗传控制,将100个噬斑形成单位(pfu)的JHMV脑内接种到BALB/cHeA、STS/A、F1杂种小鼠以及BALB/cHeA和STS/A小鼠品系之间的13个重组近交(RI)品系小鼠中。所有BALB/cHeA小鼠在2周内死于急性脑炎。相比之下,STS/A小鼠表现出部分抗性,死亡率为30%,存活时间更长,病毒产生率更低。F1杂种小鼠和RI品系小鼠的死亡率、存活时间和病毒滴度各不相同,表明有多个基因参与其中。在急性感染中存活下来的STS/A、F1杂种和RI小鼠偶尔会在感染后约1个月出现严重的轻瘫。在这些小鼠的中枢神经系统中发现有空泡变性、星形细胞增生、血管周围套袖现象缺失以及轻微脱髓鞘。从这些小鼠中无法分离出感染性病毒。虽然迟发性麻痹仅限于STS/A、F1杂种和13个RI品系中的8个,但RI品系之间的发病率差异显著。这些结果可能表明JHMV诱导的迟发性疾病也受多因素控制。本文还讨论了JHMV感染的发病机制。

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