Adenovirus 2 E1B‐55K protein relieves p53‐mediated transcriptional repression of the survivin and MAP4 promoters

Akusjauml; rvi Gouml; ran; Punga Tanel

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Adenovirus 2 E1B‐55K protein relieves p53‐mediated transcriptional repression of the survivin and MAP4 promoters

机译：腺病毒2 E1B-55K蛋白可缓解Survivin和MAP4启动子的p53介导的转录抑制

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>It is well established that adenovirus E1B-55K protein functions as an inhibitor of the tumor suppressor protein p53 by binding and inactivating p53 as a transcriptional activator protein. Here we show that the adenovirus 2 E1B-55K protein also blocks p53 as a transcriptional repressor protein of the survivin and the MAP4 promoters. The repression is dependent on the ability of E1B-55K to bind to p53 and is enhanced by coexpression of the adenovirus E4orf6 protein. Overexpression of the transcriptional corepressor protein Sin3A partially relieves the inhibitory effect of E1B-55K, suggesting that E1B-55K blocks p53 functions by interfering with the Sin3 complex.

机译：众所周知，腺病毒E1B-55K蛋白通过结合和失活作为转录激活蛋白的p53而起到抑癌蛋白p53的抑制剂的作用。在这里，我们显示腺病毒2 E1B-55K蛋白也将p53阻断为survivin和MAP4启动子的转录阻遏蛋白。该抑制取决于E1B-55K结合p53的能力，并通过腺病毒E4orf6蛋白的共表达而增强。转录共抑制蛋白Sin3A的过表达部分缓解了E1B-55K的抑制作用，表明E1B-55K通过干扰Sin3复合体来阻断p53功能。

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《FEBS Letters》 |2003年第3期|共页
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Akusjauml; rvi Gouml; ran; Punga Tanel;
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1. Two domains of p53 interact with the TATA-binding protein, and the adenovirus 13S E1A protein disrupts the association, relieving p53-mediated transcriptional repression. [J] . N Horikoshi, A Usheva, J Chen, Molecular and Cellular Biology . 1995,第1期

机译：p53的两个结构域与TATA结合蛋白相互作用，腺病毒13S E1A蛋白破坏了这种结合，从而减轻了p53介导的转录抑制。
2. The adenovirus‐2 E1B‐55K protein interacts with a mSin3A/histone deacetylase 1 complex [J] . Akusjauml, rvi Gouml, ran, FEBS Letters . 2000,第3期

机译：腺病毒2 E1B 55K蛋白与mSin3A /组蛋白脱乙酰基酶1复合物相互作用
3. TACC3 mediates the association of MBD2 with histone acetyltransferases and relieves transcriptional repression of methylated promoters [J] . Alfredo Fusco, Carmelo B. Bruni, Francesca Lembo, Nucleic acids research . 2014,第2期

机译：TACC3介导MBD2与组蛋白乙酰转移酶的缔合，并减轻甲基化启动子的转录抑制
4. HCV CORE FRAME SHIFT PROTEIN, F PROTEIN, SHARES THE REPRESSION OF P21 PROMOTER ACTIVITY WITH CORE PROTEIN [C] . Kong Jing, Deng Xiaozhao, Zhang Yun, The 6'th International Forum on Post-genome Technologies(6'IFPT)（第六届国际后基因组生命科学技术学术论坛） . 2009

机译：HCV核心框架转移蛋白F蛋白与核心蛋白共同抑制P21启动子活性
5. Investigating proteins that stimulate transcription from the adenovirus major late promoter. [D] . Ali, Humayra B. 2009

机译：研究刺激腺病毒主要晚期启动子转录的蛋白质。
6. Two domains of p53 interact with the TATA-binding protein and the adenovirus 13S E1A protein disrupts the association relieving p53-mediated transcriptional repression. [O] . N Horikoshi, A Usheva, J Chen, 1995

机译：p53的两个结构域与TATA结合蛋白相互作用腺病毒13S E1A蛋白破坏了这种结合从而减轻了p53介导的转录抑制。
7. Adenovirus 2 E1B-55K protein relieves p53-mediated transcriptional repression of the survivin and MAP4 promoters [O] . Punga Tanel, Akusjärvi Göran 2003

机译：腺病毒2 E1B-55K蛋白缓解p53介导的survivin和MAP4启动子的转录抑制

Adenovirus 2 E1B‐55K protein relieves p53‐mediated transcriptional repression of the survivin and MAP4 promoters

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