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The conserved domain CR2 of Epstein-Barr virus nuclear antigen leaderprotein is responsible not only for nuclear matrix association but alsofor nuclear localization

机译:爱泼斯坦-巴尔病毒核抗原前导蛋白的保守结构域CR2不仅负责核基质的缔合,而且还负责核的定位

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There is a growing body of evidence for the importance of the nuclear matrix in various nuclear events including gene expression and DNA replication. Epstein-Barr virus (EBV) nuclear antigen leader protein (EBNA-LP) is a nuclear matrix-associated protein that has been suggested to play an important role in EBV-induced transformation. To define the biological significance of the association of EBNA-LP with the nuclear matrix, we mapped the domain of EBNA-LP responsible for nuclear matrix association and investigated the functions of the EBNA-LP mutant mutagenized by substitution of alanines for the cluster of arginine residues in the mapped region. The results of the present study were as follows. (i) Transiently expressed EBNA-LP in COS-7 or BOSC23 cells was associated with the nuclear matrix, similarly to that in EBV-infected B cells. (ii) Mutational analysis of EBNA-LP revealed that a 10-amino acid segment of EBNA-LP is critical for nuclear matrix association of the protein. Interestingly, the identified region overlapped with the region CR2 of EBNA-LP conserved among a subset of primate gammaherpesviruses. The identified segment is referred to as EBNA-LP NMTS (nuclear matrix targeting signal). (iii) The EBNA-LP mutant with the arginine to alanine substitutions in NMTS was no longer localized not only to the nuclear matrix but also to the nucleus. (iv) The EBNA-LP mutant lacked its ability to coactivate EBNA-2-dependent transactivation. These results indicated that EBNA-LP needs to be localized in the nucleus and/or associated with the nuclear matrix through CR2 to elicit its function such as the coactivation of the EBNA-2-dependent transcriptional activation.
机译:越来越多的证据表明核基质在包括基因表达和DNA复制在内的各种核事件中的重要性。爱泼斯坦巴尔病毒(EBV)核抗原前导蛋白(EBNA-LP)是一种与核基质相关的蛋白,已被证明在EBV诱导的转化中起重要作用。为了定义EBNA-LP与核基质结合的生物学意义,我们绘制了负责核基质结合的EBNA-LP结构域,并研究了通过丙氨酸替代精氨酸簇而诱变的EBNA-LP突变体的功能。映射区域中的残基。本研究的结果如下。 (i)在COS-7或BOSC23细胞中瞬时表达的EBNA-LP与核基质相关,类似于在EBV感染的B细胞中。 (ii)EBNA-LP的突变分析表明,EBNA-LP的10个氨基酸段对蛋白质的核基质缔合至关重要。有趣的是,所鉴定的区域与灵长类γ疱疹病毒子集之间保守的EBNA-LP的CR2区域重叠。识别出的片段称为EBNA-LP NMTS(核基质靶向信号)。 (iii)在NMTS中具有精氨酸至丙氨酸取代的EBNA-LP突变体不仅不再局限于核基质,而且也不再局限于核。 (iv)EBNA-LP突变体缺乏共激活EBNA-2依赖性反式激活的能力。这些结果表明,EBNA-LP需要定位在细胞核中和/或通过CR2与核基质缔合,以引发其功能,例如EBNA-2依赖性转录激活的共激活。

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