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EB病毒编码的EBNA-5在核仁外包涵体中与P14ARF结合,并延长表达P14ARF的细胞的存活时间。

EBV-encoded EBNA-5 associates with P14ARF in extranucleolar inclusions and prolongs the survival of P14ARF-expressing cells.

作者信息

Kashuba Elena, Mattsson Karin, Pokrovskaja Katja, Kiss Csaba, Protopopova Marina, Ehlin-Henriksson Barbro, Klein George, Szekely Laszlo

机构信息

Microbiology and Tumor Biology Center (MTC), Karolinska Institute, Nobels vag 16, Box 280, S-171 77 Stockholm, Sweden.

出版信息

Int J Cancer. 2003 Jul 10;105(5):644-53. doi: 10.1002/ijc.11124.

Abstract

Epstein-Barr virus (EBV) carrying lymphoblastoid cells of normal origin express the full program of all 9 virus-encoded, growth transformation associated proteins. They have an intact p53 pathway as a rule. This raises the question of whether any of the viral proteins impair the pathway functionally. Using a yeast 2-hybrid system, we have shown that EBNA-5 but not the other EBNAs interacts with the p14ARF protein, a regulator of the p53 pathway. The interaction was confirmed in vitro using a GST pull-down assay. Moreover, expression of EBNA-5 increased the survival of p14ARF-transfected cells. EBV infection of resting B cells induced the expression of p14ARF mRNA without increased level of the protein. A fraction of the p14ARF localized to the nucleoli but the bulk of the protein accumulated in nuclear but extranucleolar inclusions. Formation of the extranucleolar inclusions led to complete relocalization of EBNA-5 from nucleoplasm to these structures. The inclusions also contained p53 and HDM2, and were surrounded by PML bodies and proteasomes, which suggests that these inclusions could be targets for proteasome dependent protein degradation.

摘要

携带爱泼斯坦-巴尔病毒(EBV)的正常来源淋巴母细胞表达全部9种病毒编码的、与生长转化相关的蛋白质。通常它们具有完整的p53通路。这就提出了一个问题,即是否有任何病毒蛋白在功能上损害该通路。利用酵母双杂交系统,我们发现EBNA-5而非其他EBNA与p53通路的调节因子p14ARF蛋白相互作用。通过谷胱甘肽S-转移酶(GST)下拉试验在体外证实了这种相互作用。此外,EBNA-5的表达增加了p14ARF转染细胞的存活率。静息B细胞的EBV感染诱导了p14ARF mRNA的表达,但蛋白水平并未升高。一部分p14ARF定位于核仁,但大部分蛋白积聚在核内但核仁外的包涵体中。核仁外包涵体的形成导致EBNA-5从核质完全重新定位到这些结构中。这些包涵体还含有p53和HDM2,并被早幼粒细胞白血病(PML)小体和蛋白酶体包围,这表明这些包涵体可能是蛋白酶体依赖性蛋白质降解的靶点。

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