小鼠品系对中枢神经系统（CNS）单纯疱疹病毒 1 型（HSV-1）感染的影响。

Herpesviridae Pub Date : 2012-03-26 DOI:10.1186/2042-4280-3-4

Lorne F Kastrukoff, Allen S Lau, Eva E Thomas

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引用次数: 0

摘要

背景：小鼠感染 HSV-1 后会出现致死性脑炎或病毒诱导的中枢神经系统脱髓鞘。影响结果的因素有多种，包括感染途径、病毒和小鼠品系。当通过口腔粘膜感染亚致死剂量的 HSV-1 2 株时，易感的 SJL/J、A/J 和 PL/J 小鼠整个大脑都会出现脱髓鞘病变。相比之下，中度抗性 BALB/c 小鼠的病变仅限于脑干（BST），而抗性 BL/6 小鼠的病变则不存在。造成这种品系差异的原因尚不清楚：在这项研究中，我们结合组织学、免疫组化和原位杂交技术，研究了病毒与不同品系小鼠脱髓鞘早期（PI < 24 天）病变发展之间的关系：最初，病毒 DNA 和抗原阳性细胞依次出现在 BALB/c、SJL/J、A/J 和 PL/J 小鼠大脑的非连续区域，但仅限于 BL/6 小鼠的 BST 区域。在 SJL/J、A/J 和 PL/J 小鼠中，病毒感染神经元和非神经元细胞的 "病灶 "区域随后出现在整个大脑中。病灶 "区域按照等级顺序排列，并与正在发展的脱髓鞘病变共定位。当抗原被清除后，脱髓鞘区域仍会保留 DNA 阳性的病毒细胞；这与潜伏感染一致。与此相反，"病灶 "区域仅限于 BALB/c 小鼠的 BST，而不会出现在 BL/6 小鼠中：本研究结果表明，经口腔粘膜感染 HSV-1 的易感小鼠品系在最初 24 天内会出现中枢神经系统脱髓鞘，并分为几个阶段。这些阶段包括：病毒在整个大脑非连续区域的初始传播和细胞感染、病毒感染神经元和非神经元细胞的 "病灶 "区域的形成、"病灶 "区域与正在形成的脱髓鞘病变的共定位以及一些病变的潜伏感染。与此相反，BALB/c 小鼠发生的脱髓鞘病变有限，而 BL/6 小鼠则没有脱髓鞘病变，这与这两个品系的神经元和非神经元细胞受病毒感染的 "病灶 "区域有限或缺乏有关。

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The effect of mouse strain on herpes simplex virus type 1 (HSV-1) infection of the central nervous system (CNS).

Background: Mice infected with HSV-1 can develop lethal encephalitis or virus induced CNS demyelination. Multiple factors affect outcome including route of infection, virus and mouse strain. When infected with a sub-lethal dose of HSV-1 strain 2 via the oral mucosa, susceptible SJL/J, A/J, and PL/J mice develop demyelinating lesions throughout the brain. In contrast, lesions are restricted to the brainstem (BST) in moderately resistant BALB/c mice and are absent in resistant BL/6 mice. The reasons for the strain differences are unknown.

Methods: In this study, we combine histology, immunohistochemistry, and in-situ hybridization to investigate the relationship between virus and the development of lesions during the early stage (< 24 days PI) of demyelination in different strains of mice.

Results: Initially, viral DNA and antigen positive cells appear sequentially in non-contiguous areas throughout the brains of BALB/c, SJL/J, A/J, and PL/J mice but are restricted to an area of the BST of BL/6 mice. In SJL/J, A/J, and PL/J mice, this is followed by the development of 'focal' areas of virus infected neuronal and non-neuronal cells throughout the brain. The 'focal' areas follow a hierarchical order and co-localize with developing demyelinating lesions. When antigen is cleared, viral DNA positive cells can remain in areas of demyelination; consistent with a latent infection. In contrast, 'focal' areas are restricted to the BST of BALB/c mice and do not occur in BL/6 mice.

Conclusions: The results of this study indicate that susceptible mouse strains, infected with HSV-1 via the oral mucosa, develop CNS demyelination during the first 24 days PI in several stages. These include: the initial spread of virus and infection of cells in non-contiguous areas throughout the brain, the development of 'focal' areas of virus infected neuronal and non-neuronal cells, the co-localization of 'focal' areas with developing demyelinating lesions, and latent infection in a number of the lesions. In contrast, the limited demyelination that develops in BALB/c and the lack of demyelination in BL/6 mice correlates with the limited or lack of 'focal' areas of virus infected neuronal and non-neuronal cells in these two strains.

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Herpesviridae

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