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上皮细胞瘤中EB病毒核抗原EBNA1的结构改变

Alterations in the structure of the EBV nuclear antigen, EBNA1, in epithelial cell tumours.

作者信息

Snudden D K, Smith P R, Lai D, Ng M H, Griffin B E

机构信息

Department of Virology, Royal Postgraduate Medical School, London, UK.

出版信息

Oncogene. 1995 Apr 20;10(8):1545-52.

PMID:7731709
Abstract

The EBV nuclear antigen, EBNA1, is the only viral protein consistently expressed in all virus-infected cells. It is required in trans for viral replication, maintenance of EBV extrachromosomal episomes, and transcriptional transactivation in latently-infected B-cells. It binds RNA suggestive of a regulatory role in post-transcriptional events and in transgenic mice, it is tumorigenic. In RNase protection studies relating to the EBV-associated tumour, nasopharyngeal carcinoma (NPC), we show that a C-terminal EBNA1 RNA probe from the prototype B95-8 marmoset strain can protect its own mRNA from enzymatic digestion, but does not fully protect EBNA1 mRNA from NPC cells. This finding is consistent with changes in the coding region for the antigen. We thus determined the sequences of EBNA1 genes derived from an NPC xenograft and numerous patient biopsies and identified a number of mutations in the gene in these human cells, relative to B95-8. Many of the nucleotide changes would lead to non-conservative amino acid alterations in apparently functionally significant regions of the protein. We show that although some of the mutations lie in regions designated as critical to DNA binding, they have negligible effect on this property of EBNA1. The basic regions in EBNA1 that may bind to RNA, at least in vitro, are exempt from mutation. Thus, unless the alterations are 'silent', which for such a critical viral function seems unlikely, they may relate to as yet unmapped viral activities, such as a role in tumorigenesis and the ability of EBNA1 to evade the cellular immune system, or be associated with the ability of the antigen to regulate gene transcription.

摘要

EB病毒核抗原EBNA1是唯一在所有病毒感染细胞中持续表达的病毒蛋白。它在反式作用中对病毒复制、EBV染色体外游离基因的维持以及潜伏感染B细胞中的转录反式激活是必需的。它与RNA结合,提示在转录后事件中起调节作用,并且在转基因小鼠中具有致瘤性。在与EBV相关肿瘤鼻咽癌(NPC)有关的核糖核酸酶保护研究中,我们发现来自原型B95 - 8狨猴株的C末端EBNA1 RNA探针可以保护其自身的mRNA不被酶消化,但不能完全保护NPC细胞中的EBNA1 mRNA。这一发现与该抗原编码区的变化一致。因此,我们确定了来自NPC异种移植瘤和众多患者活检组织的EBNA1基因序列,并相对于B95 - 8鉴定出这些人类细胞中该基因的一些突变。许多核苷酸变化会导致该蛋白明显功能重要区域的非保守氨基酸改变。我们表明,尽管一些突变位于被指定对DNA结合至关重要的区域,但它们对EBNA1的这一特性影响可忽略不计。EBNA1中可能与RNA结合的碱性区域,至少在体外,未发生突变。因此,除非这些改变是“沉默”的,而对于这样一个关键的病毒功能来说这似乎不太可能,否则它们可能与尚未明确的病毒活性有关,比如在肿瘤发生中的作用以及EBNA1逃避细胞免疫系统的能力,或者与该抗原调节基因转录的能力有关。

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