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在许多没有进行性多灶性白质脑病的患者的人脑样本中都存在JC病毒DNA。

JC virus DNA is present in many human brain samples from patients without progressive multifocal leukoencephalopathy.

作者信息

White F A, Ishaq M, Stoner G L, Frisque R J

机构信息

Department of Molecular and Cell Biology, Pennsylvania State University, University Park 16802.

出版信息

J Virol. 1992 Oct;66(10):5726-34. doi: 10.1128/JVI.66.10.5726-5734.1992.

Abstract

Sections of normal and diseased brain and kidney tissues were screened for the presence of JC virus (JCV) DNA by using the polymerase chain reaction. As expected, all samples obtained from patients with progressive multifocal leukoencephalopathy (PML) tested positive when multiple JCV-specific primer and probe combinations were used. Unexpectedly, more than 50% of non-PML-affected brains were also found to harbor low levels of JCV DNA. To confirm that the positive signals seen in the tissue sections were not the result of contamination, amplified DNA was cloned and sequenced and in some cases was shown to represent strains of JCV not identified previously. Two predominant regulatory region configurations of JCV have been detected in the human host: archetype JCV, which is excreted in the urine of normal and immunocompromised individuals, and "PML-type" JCV found in diseased brains. This latter group of variants appears to derive from archetype JCV by the deletion and duplication of sequences within the promoter-enhancer region. In the present study, the archetype strain of JCV was identified only in normal kidney samples; JCV DNA found in non-PML-affected brain specimens and in kidney tissue from patients with PML resembled that of strains isolated from PML-affected brain tissue. Our findings indicate that JCV reaches the brain more frequently than previously thought and may persist at this site without causing demyelinating disease. A subsequent episode of prolonged immunodeficiency or a direct interaction with an immunocompromising agent (e.g., human immunodeficiency virus type 1) might activate the latent JCV infection and lead to the development of PML.

摘要

通过聚合酶链反应对正常和患病的脑及肾组织切片进行筛查,以检测JC病毒(JCV)DNA的存在。正如预期的那样,当使用多种JCV特异性引物和探针组合时,从进行性多灶性白质脑病(PML)患者获得的所有样本检测均呈阳性。出乎意料的是,还发现超过50%未受PML影响的脑也含有低水平的JCV DNA。为了确认在组织切片中看到的阳性信号不是污染的结果,对扩增的DNA进行了克隆和测序,在某些情况下,结果显示代表了先前未鉴定的JCV毒株。在人类宿主中已检测到JCV的两种主要调控区构型:原型JCV,存在于正常个体和免疫功能低下个体的尿液中;以及在患病脑中发现的“PML型”JCV。后一组变体似乎是通过启动子-增强子区域内序列的缺失和重复从原型JCV衍生而来。在本研究中,仅在正常肾样本中鉴定出JCV的原型毒株;在未受PML影响的脑标本和PML患者的肾组织中发现的JCV DNA与从PML受影响脑组织中分离出的毒株相似。我们的研究结果表明,JCV到达脑部的频率比以前认为的更高,并且可能在该部位持续存在而不引起脱髓鞘疾病。随后的长期免疫缺陷发作或与免疫抑制因子(如1型人类免疫缺陷病毒)的直接相互作用可能会激活潜伏的JCV感染并导致PML的发生。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a915/241447/8d4e1d1a80b1/jvirol00041-0036-a.jpg

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