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爱泼斯坦-巴尔病毒核抗原(EBNA-1)与质粒维持区域中簇状位点的序列特异性DNA结合。

Sequence-specific DNA binding of the Epstein-Barr virus nuclear antigen (EBNA-1) to clustered sites in the plasmid maintenance region.

作者信息

Rawlins D R, Milman G, Hayward S D, Hayward G S

出版信息

Cell. 1985 Oct;42(3):859-68. doi: 10.1016/0092-8674(85)90282-x.

Abstract

Latently infected B lymphocytes continuously express an Epstein-Barr Virus nuclear antigen (EBNA-1) required in trans for maintenance of the plasmid state of the EBV genome. Filter binding assays and DNAase I footprinting analyses revealed that the carboxy-terminal domain of EBNA-1 protects binding sites at three different loci in the 172,000 bp EBV genome. Two of these loci correspond to essential elements within an 1800 bp segment defined as the minimal region required for plasmid maintenance (ori-P). Binding to each of 20 X 30 bp tandem repeats in the "sink" locus protects 25 bp centered over a 12 bp palindromic consensus sequence TAGCATATGCTA. The nearby dyad symmetry "origin" locus contains two 46 bp protected regions each encompassing two paired core binding sites. The demonstration of sequence-specific binding at multiple loci suggests that EBNA-1 has pleiotropic functions, which may include control of copy number and segregation of the EBV plasmids as well as initiation of replication.

摘要

潜伏感染的B淋巴细胞持续表达一种EB病毒核抗原(EBNA-1),该抗原对于维持EBV基因组的质粒状态是反式作用所必需的。滤膜结合试验和DNA酶I足迹分析表明,EBNA-1的羧基末端结构域保护EBV基因组172,000 bp中三个不同位点的结合位点。其中两个位点对应于一个1800 bp片段内的必需元件,该片段被定义为质粒维持所需的最小区域(ori-P)。与“汇”位点中20个X 30 bp串联重复序列中的每一个结合,可保护以12 bp回文共有序列TAGCATATGCTA为中心的25 bp。附近的二元对称“起源”位点包含两个46 bp的受保护区域,每个区域包含两个配对的核心结合位点。在多个位点上序列特异性结合的证明表明,EBNA-1具有多效性功能,这可能包括控制EBV质粒的拷贝数和分离以及复制起始。

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