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Distinctive Effects of the Epstein-Barr Virus Family of Repeats on Viral Latent Gene Promoter Activity and B-Lymphocyte Transformation

机译:EB病毒家族重复序列对病毒潜伏基因启动子活性和B淋巴细胞转化的显着影响

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摘要

The Epstein-Barr virus (EBV), a human B-lymphotropic gamma herpesvirus, contains multiple repetitive sequences within its genome. A group of repetitive sequences, known as the family of repeats (FR), contains multiple binding sites for the viral trans-acting protein EBNA-1. The FR sequences are important for viral genome maintenance and for the regulation of the promoter involved in viral latent gene expression. It has been reported that a palindromic sequence with a putative secondary structure exists at the 3′ end of the FR in the genome of the EBV B95-8 strain and that this palindromic sequence has been deleted from the FR of the commonly used EBV miniplasmids. For the first time, we cloned an EBV B95-8 DNA fragment containing the full-length FR, which enabled us to examine the functional difference between full-length and deleted FRs. The full-length FR, like the deleted FR, functioned as a transcriptional enhancer of the viral latent gene promoter, but that transactivation was significantly attenuated in the case of the full-length FR. No significant enhancement of replication was observed when the deleted FR was replaced with the full-length FR in an EBV miniplasmid. By contrast, when the same set of FR sequences were tested in the context of the complete EBV genome, the full-length FR resulted in more-efficient B-cell transformation than the deleted FR. We propose that the presence of the full-length FR contributes to the precise regulation of the viral latent promoter and increases the efficiency of B-cell transformation.
机译:爱泼斯坦-巴尔病毒(EBV)是一种人类B淋巴性伽马疱疹病毒,在其基因组内包含多个重复序列。一组重复序列(称为重复家族(FR))包含病毒反式作用蛋白EBNA-1的多个结合位点。 FR序列对于维持病毒基因组和调节参与病毒潜基因表达的启动子很重要。据报道,在EBV B95-8菌株的基因组的FR的3'末端存在具有假定的二级结构的回文序列,并且该回文序列已经从常用EBV小质粒的FR中缺失。我们首次克隆了包含全长FR的EBV B95-8 DNA片段,这使我们能够检查全长FR和缺失的FR之间的功能差异。全长FR与缺失的FR一样,起病毒潜在基因启动子的转录增强子的作用,但是在全长FR的情况下,反式激活明显减弱。当在EBV小质粒中用全长FR替换缺失的FR时,没有观察到复制的明显增强。相比之下,当在完整EBV基因组的背景下测试同一组FR序列时,全长FR导致比缺失FR更有效的B细胞转化。我们建议全长FR的存在有助于病毒潜伏启动子的精确调节,并增加B细胞转化的效率。

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