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p300/CBP及其相关因子PCAF与转录调控 总被引:1,自引:0,他引:1
p300/CBP及相关因子PCAF具有乙酰转移酶活性,能通过乙酰化组蛋白和非组蛋白的方式参与基因的转录调控.同时,它们能在转录因子和基本转录复合物之间起到桥梁作用,而且也能为整合多种转录因子提供支架,是一种典型的转录辅激活子. p300/CBP与细胞周期调控、细胞凋亡以及癌症的发生等过程之间有着直接的联系。本文概括了p300/CBP与PCAF的基本特性,并简要介绍它们与其他蛋白之间的相互作用,特别是E1A的最新研究进展。 相似文献
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《Molecular cell》2022,82(19):3580-3597.e9
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p300/CBP/p53 interaction and regulation of the p53 response. 总被引:10,自引:0,他引:10
S R Grossman 《European journal of biochemistry》2001,268(10):2773-2778
Substantial evidence points to a critical role for the p300/CREB binding protein (CBP) coactivators in p53 responses to DNA damage. p300/CBP and the associated protein P/CAF bind to and acetylate p53 during the DNA damage response, and are needed for full p53 transactivation as well as downstream p53 effects of growth arrest and/or apoptosis. Beyond this simplistic model, p300/CBP appear to be complex integrators of signals that regulate p53, and biochemically, the multipartite p53/p300/CBP interaction is equally complex. Through physical interaction with p53, p300/CBP can both positively and negatively regulate p53 transactivation, as well as p53 protein turnover depending on cellular context and environmental stimuli, such as DNA damage. 相似文献
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Regulation of FoxO activity by CBP/p300-mediated acetylation 总被引:9,自引:0,他引:9
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WTX encodes a tumor suppressor, frequently inactivated in Wilms tumor, with both plasma membrane and nuclear localization. WTX has been implicated in β-catenin turnover, but its effect on nuclear proteins is unknown. We report an interaction between WTX and p53, derived from the unexpected observation of WTX, p53, and E1B 55K colocalization within the characteristic cytoplasmic body of adenovirus-transformed kidney cells. In other cells without adenovirus expression, the C-terminal domain of WTX binds to the DNA-binding domain of p53, enhances its binding to CBP, and increases CBP/p300-mediated acetylation of p53 at Lys 373/382. WTX knockdown accelerates CBP/p300 protein turnover and attenuates this modification of p53. In p53-reconstitution experiments, cell-cycle arrest, apoptosis, and p53 target-gene expression are suppressed by depletion of WTX. Together, these results suggest that WTX modulates p53 function, in part through regulation of its activator CBP/p300. 相似文献
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Antonello Mai Dante Rotili Domenico Tarantino Angela Nebbioso Sabrina Castellano Gianluca Sbardella Marc Tini Lucia Altucci 《Bioorganic & medicinal chemistry letters》2009,19(4):1132-1135
We identified a series of 4-hydroxyquinolines bearing a C1 to C15 alkyl chain at the C2 position and a carbethoxy/carboxy group at the C3 position of the quinoline nucleus (MC compounds), endowed with selective inhibitory activity against the p300/CBP HAT enzymes. Enzyme inhibition was investigated using in vitro HAT assays and by western blot analysis of cellular lysates to examine the acetylation levels of histone H3 and α-tubulin. When tested in U937 cells, some compounds displayed pro-apoptotic or cytodifferentiating properties. 相似文献
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Takeo Narita Shinsuke Ito Yoshiki Higashijima Wai Kit Chu Katrin Neumann Jonas Walter Shankha Satpathy Tim Liebner William B. Hamilton Elina Maskey Gabriela Prus Marika Shibata Vytautas Iesmantavicius Joshua M. Brickman Konstantinos Anastassiadis Haruhiko Koseki Chunaram Choudhary 《Molecular cell》2021,81(10):2166-2182.e6
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