Immune regulation in Epstein-Barr virus-associated diseases.

R Khanna, S R Burrows, D J Moss
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引用次数: 22

Abstract

Epstein-Barr virus (EBV) is a member of the human herpesvirus family and, like many other herpesviruses, maintains a lifelong latent association with B lymphocytes and a permissive association with stratified epithelium in the oropharynx. Clinical manifestations of primary EBV infection range from acute infectious mononucleosis to an asymptomatic persistent infection. EBV is also associated with a number of malignancies in humans. This review discusses features of the biology of the virus, both in cell culture systems and in the natural host, before turning to the role of the immune system in controlling EBV infection in healthy individuals and in individuals with EBV-associated diseases. Cytotoxic T cells that recognize virally determined epitopes on infected cells make up the major effector arm and control the persistent infection. In contrast, the options for immune control of EBV-associated malignancies are more restricted. Not only is antigen expression restricted to a single nuclear antigen, EBNA1, but also these tumor cells are unable to process EBV latent antigens, presumably because of a transcriptional defect in antigen-processing genes (such as TAP1 and TAP2). The likelihood of producing a vaccine capable of controlling the acute viral infection and EBV-associated malignancies is also discussed.

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eb病毒相关疾病的免疫调节
eb病毒(EBV)是人类疱疹病毒家族的一员,与许多其他疱疹病毒一样,与B淋巴细胞保持终身潜伏关联,并与口咽部分层上皮保持许可关联。原发性EBV感染的临床表现从急性传染性单核细胞增多症到无症状的持续性感染不等。EBV还与人类的许多恶性肿瘤有关。这篇综述讨论了病毒在细胞培养系统和自然宿主中的生物学特征,然后转向免疫系统在控制健康个体和EBV相关疾病个体中的EBV感染中的作用。识别受感染细胞上病毒决定的表位的细胞毒性T细胞构成了主要的效应臂并控制持续感染。相比之下,ebv相关恶性肿瘤的免疫控制选择更为有限。不仅抗原表达局限于单一核抗原EBNA1,而且这些肿瘤细胞也无法加工EBV潜伏抗原,可能是因为抗原加工基因(如TAP1和TAP2)的转录缺陷。还讨论了生产一种能够控制急性病毒感染和ebv相关恶性肿瘤的疫苗的可能性。
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