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来自年龄达 100 岁的健康受试者的血清 IgG 抗体可与 JC 多瘤病毒发生反应。

Serum IgG antibodies from healthy subjects up to 100 years old react to JC polyomavirus.

机构信息

Department of Morphology, Surgery and Experimental Medicine, Section of Pathology, Oncology and Experimental Biology, School of Medicine, University of Ferrara, Ferrara, Italy.

Clinical Laboratory Analysis, University Hospital of Ferrara, Ferrara, Italy.

出版信息

J Cell Physiol. 2018 Aug;233(8):5513-5522. doi: 10.1002/jcp.26457. Epub 2018 Feb 22.

DOI:10.1002/jcp.26457
PMID:29323725
Abstract

JC polyomavirus (JCPyV) was identified in 1971 in the brain tissue of a patient (J.C.) affected by the progressive multifocal leukoencephalopathy (PML). JCPyV encodes for the oncoproteins large T antigen (Tag) and small t-antigen (tag). These oncoproteins are responsible of the cell transformation and tumorigenesis in experimental animals. JCPyV is ubiquitous in human populations. After the primary infection, which is usually asymptomatic, JCPyV remains lifelong in the host in a latent phase. Its reactivation may occur in heathy subjects and immunocompromised patients. Upon reactivation, JCPyV could reach (i) the CNS inducing the PML, (ii) the kidney of transplant patients causing the organ rejection. Association between JCPyV, which is a small DNA tumor virus, and gliomas and colorectal carcinomas has been published. In the present investigation, we report on a new indirect ELISA with two specific synthetic peptides mimicking JCPyV VP1 immunogenic epitopes to detect specific serum IgG antibodies against JCPyV. Serum samples of healthy subjects (n = 355) ranging 2-100 years old, were analyzed by this new indirect ELISA. The linear peptides VP1 K and VP1 N resemble the natural JCPyV VP1 capsidic epitopes constituting a docking site for serum antibodies. Data from this innovative immunologic assay indicate that the overall prevalence of JCPyV-VP1 antibodies in healthy subjects is at 39%. The innovative indirect ELISA with JCPyV VP1 mimotopes seems to be a useful method to detect specific IgG antibodies against this virus, without cross-reactivity with the closely related SV40 and BKPyV polyomaviruses.

摘要

JC 多瘤病毒(JCPyV)于 1971 年在患有进行性多灶性白质脑病(PML)的患者(J.C.)的脑组织中被发现。JCPyV 编码致癌蛋白大 T 抗原(Tag)和小 t 抗原(tag)。这些致癌蛋白负责实验动物的细胞转化和肿瘤发生。JCPyV 在人类中普遍存在。初次感染后(通常无症状),JCPyV 在宿主中处于潜伏状态,终身存在。其再激活可能发生在健康受试者和免疫功能低下的患者中。再激活后,JCPyV 可能会(i)进入中枢神经系统引起 PML,(ii)进入移植患者的肾脏导致器官排斥。JCPyV 是一种小型 DNA 肿瘤病毒,与神经胶质瘤和结直肠癌之间的关联已被发表。在本研究中,我们报告了一种新的间接 ELISA,该方法使用两种模拟 JCPyV VP1 免疫原性表位的特异性合成肽来检测针对 JCPyV 的特异性血清 IgG 抗体。我们用这种新的间接 ELISA 分析了 355 名年龄在 2-100 岁之间的健康受试者的血清样本。线性肽 VP1K 和 VP1N 类似于天然 JCPyV VP1 衣壳表位,构成血清抗体的对接位点。来自该创新免疫测定法的数据表明,健康受试者中 JCPyV-VP1 抗体的总体流行率为 39%。该新型间接 ELISA 用 JCPyV VP1 模拟表位似乎是一种有用的方法,可检测针对该病毒的特异性 IgG 抗体,而与密切相关的 SV40 和 BKPyV 多瘤病毒无交叉反应性。

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