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疱疹病毒狒狒中爱泼斯坦-巴尔病毒LMP2A同源物的5'编码和调控区序列差异与保守功能

5' Coding and regulatory region sequence divergence with conserved function of the Epstein-Barr virus LMP2A homolog in herpesvirus papio.

作者信息

Franken M, Annis B, Ali A N, Wang F

机构信息

Department of Medicine, Brigham & Women's Hospital, Boston, Massachusetts 02115, USA.

出版信息

J Virol. 1995 Dec;69(12):8011-9. doi: 10.1128/JVI.69.12.8011-8019.1995.

Abstract

B-lymphotropic herpesviruses naturally infecting Old World primates share biologic, epidemiologic, pathogenic, and molecular features with the human pathogen Epstein-Barr virus (EBV). These related gammaherpesviruses have colinear genomes with considerable nucleotide homology. The replicative cycle genes share a high degree of homology across species, whereas the transformation-associated EBV latent genes appear to be much more divergent. For example, the EBV BamHI Nhet fragment, which encodes all or part of the EBV latent infection membrane proteins, cross-hybridizes poorly to DNA from nonhuman primate B-lymphotropic herpesviruses. A viral DNA fragment corresponding to this region of the EBV genome was isolated from the baboon B-lymphotropic herpesvirus, herpesvirus papio, and used to clone a herpesvirus papio cDNA corresponding to EBV LMP2A. At least three tyrosine kinase interaction motifs are conserved despite significant amino acid divergence of the herpesvirus papio LMP2A first exon from the EBV homolog. Functionally, the herpesvirus papio LMP2A is tyrosine phosphorylated and induces tyrosine phosphorylation of cell proteins similar to EBV LMP2A. The 12 hydrophobic LMP2 transmembrane domains are well conserved. Two CBP (Jk) binding sites important for EBNA-2-induced transactivation of the LMP2A promoter are also present in the herpesvirus papio LMP2A promoter, and the simian LMP2A promoter is also responsive to EBV EBNA-2-induced transactivation in human B cells. Thus, transcriptional regulation, splicing, kinase interaction sites, and tyrosine phosphorylation of the LMP2A homologs have been conserved despite significant sequences heterogeneity in the preterminal repeat regions of these human and nonhuman primate EBVs. The conservation of the LMP2 gene, despite its apparent nonessential role for in vitro EBV infection, suggests an important role for LMP2A in vivo. The similarities between these human and simian B-lymphotropic herpesviruses, and the LMP2 genes in particular, suggest that the function of LMP2 in vivo could be addressed by using recombinant LMP2A-mutant simian viruses and experimental infection of Old World primates.

摘要

自然感染旧世界灵长类动物的嗜B淋巴细胞疱疹病毒与人类病原体爱泼斯坦-巴尔病毒(EBV)具有生物学、流行病学、致病性和分子特征。这些相关的γ疱疹病毒具有共线性基因组,核苷酸同源性相当高。复制周期基因在物种间具有高度同源性,而与转化相关的EBV潜伏基因似乎差异更大。例如,编码全部或部分EBV潜伏感染膜蛋白的EBV BamHI Nhet片段与来自非人类灵长类嗜B淋巴细胞疱疹病毒的DNA杂交性很差。从狒狒嗜B淋巴细胞疱疹病毒(疱疹病毒狒狒)中分离出与EBV基因组该区域相对应的病毒DNA片段,并用于克隆与EBV LMP2A相对应的疱疹病毒狒狒cDNA。尽管疱疹病毒狒狒LMP2A第一个外显子与EBV同源物的氨基酸有显著差异,但至少三个酪氨酸激酶相互作用基序是保守的。在功能上,疱疹病毒狒狒LMP2A被酪氨酸磷酸化,并诱导细胞蛋白的酪氨酸磷酸化,类似于EBV LMP2A。12个疏水的LMP2跨膜结构域保存完好。疱疹病毒狒狒LMP2A启动子中也存在两个对EBNA-2诱导的LMP2A启动子反式激活很重要的CBP(Jk)结合位点,并且猿猴LMP2A启动子在人B细胞中也对EBV EBNA-2诱导的反式激活有反应。因此,尽管这些人类和非人类灵长类EBV的末端前重复区域存在显著的序列异质性,但LMP2A同源物的转录调控、剪接、激酶相互作用位点和酪氨酸磷酸化仍得以保留。尽管LMP2对EBV体外感染似乎并非必不可少,但LMP2基因的保守性表明LMP2A在体内具有重要作用。这些人类和猿猴嗜B淋巴细胞疱疹病毒之间的相似性,尤其是LMP2基因,表明可以通过使用重组LMP2A突变猿猴病毒和对旧世界灵长类动物进行实验性感染来研究LMP2在体内的功能。

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