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通过免疫组织化学检测心肌炎或扩张型心肌病病例心肌中的肠道病毒衣壳蛋白VP1:肠道病毒在心肌细胞中持续存在的进一步证据。

Detection of enterovirus capsid protein VP1 in myocardium from cases of myocarditis or dilated cardiomyopathy by immunohistochemistry: further evidence of enterovirus persistence in myocytes.

作者信息

Zhang Hongyi, Li Yanwen, McClean Dougal R, Richardson Peter J, Florio Richard, Sheppard Mary, Morrison Karen, Latif Najma, Dunn Michael J, Archard Leonard C

机构信息

Cell and Molecular Biology Section, Division of Biomedical Sciences, Faculty of Medicine, Imperial College, London, UK.

出版信息

Med Microbiol Immunol. 2004 May;193(2-3):109-14. doi: 10.1007/s00430-003-0208-8. Epub 2003 Nov 22.

Abstract

The association of enteroviruses with myocardial disease has been investigated extensively by molecular biological techniques to detect viral RNA, but remains controversial. This retrospective study investigated the involvement of enterovirus in myocarditis or dilated cardiomyopathy (DCM) by detection of viral antigens in myocardial samples from a new patient series using an optimized immunohistochemical technique. Formalin-fixed, paraffin-embedded biopsy, autopsy or explanted myocardial tissue samples were obtained from 136 subjects. These comprised histologically proven cases of acute fatal myocarditis (n=10), DCM (n=89, including 10 patients with healing/borderline myocarditis) and a comparison group of samples from 37 unused donor hearts and cases with other conditions. A monoclonal antibody 5-D8/1 directed against a conserved, non-conformational epitope in capsid protein VP1 was employed for broad detection of different enterovirus serotypes. Investigations were performed blindly. Histological sections from 7 of 10 fatal myocarditis cases, 47 of 89 patients (52.8%) with DCM were positive for the viral capsid protein VP1 by immunohistochemical staining. Consecutive sections of positive samples were negative when the antibody was omitted or replaced with subclass- and concentration-matched normal mouse IgG. In contrast, only 3 of 37 samples (8.1%) in the comparison group were positive (Yates corrected chi(2)=19.99, P<0.001: odds ratio =12.68). VP1 staining was distributed in individual or grouped myofibers and localized in the cytoplasm of myocytes. In some cases, VP1 was detected in only a few myofibers within an entire section. These results provide further evidence of enterovirus involvement in a high proportion of DCM cases and demonstrate that VP1 is present in disease stages from acute myocarditis, healing myocarditis to end-stage DCM requiring cardiac transplantation, indicating translation of viral protein during persistent enterovirus infection.

摘要

肠道病毒与心肌病之间的关联已通过分子生物学技术广泛研究以检测病毒RNA,但仍存在争议。这项回顾性研究通过使用优化的免疫组织化学技术检测新患者系列心肌样本中的病毒抗原,来调查肠道病毒在心肌炎或扩张型心肌病(DCM)中的作用。从136名受试者获取了福尔马林固定、石蜡包埋的活检、尸检或切除的心肌组织样本。这些样本包括组织学确诊的急性致命性心肌炎病例(n = 10)、DCM病例(n = 89,包括10例愈合/临界心肌炎患者)以及来自37个未使用的供体心脏和其他病症病例的样本组成的对照组。使用针对衣壳蛋白VP1中保守的、非构象表位的单克隆抗体5-D8/1来广泛检测不同肠道病毒血清型。研究是盲法进行的。通过免疫组织化学染色,10例致命性心肌炎病例中的7例、89例DCM患者中的47例(52.8%)的组织学切片中病毒衣壳蛋白VP1呈阳性。当省略抗体或用亚类和浓度匹配的正常小鼠IgG替代时,阳性样本的连续切片为阴性。相比之下,对照组的37个样本中只有3个(8.1%)呈阳性(Yates校正χ² = 19.99,P < 0.001:优势比 = 12.68)。VP1染色分布于单个或成群的肌纤维中,并定位于心肌细胞的细胞质中。在某些情况下,在整个切片中仅在少数肌纤维中检测到VP1。这些结果为肠道病毒累及高比例的DCM病例提供了进一步证据,并表明VP1存在于从急性心肌炎、愈合期心肌炎到需要心脏移植的终末期DCM的疾病阶段,表明在持续性肠道病毒感染期间病毒蛋白的翻译。

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