BS69 is involved in cellular senescence through the p53-p21Cip1 pathway.

BS69 is involved in cellular senescence through the p53-p21Cip1 pathway. Research Abstract Details 

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BS69 is involved in cellular senescence through the p53-p21Cip1 pathway. Abstract Text:

Wei Zhang,Ho Man Chan,Yan Gao,Randy Poon,Zhenguo Wu,

The multidomain-containing cellular protein BS69 interacts with adenovirus E1A and several other viral and cellular factors, and acts as a transcription repressor. Here, we show that BS69 is involved in the p53-p21Cip1-mediated senescence pathway. Knockdown of BS69 by RNA interference in human primary fibroblasts results in elevated levels of p21Cip1 and the appearance of several senescent markers, including enhanced senescence-associated beta-galactosidase activity and formation of senescence-associated heterochromatin foci. Importantly, knockdown of either p53 or p21Cip1, but not p16(INK4a) or Rb, allows cells to bypass premature senescence that is induced by BS69 knockdown. Furthermore, we show that BS69 forms complexes with both p53 and p400, and that BS69 associates with the p21Cip1 promoter through p53. Together, our data indicate that BS69 is involved in cellular senescence mainly through the p53-p21Cip1 pathway.

BS69 is involved in cellular senescence through the p53-p21Cip1 pathway. Publishing Authors By Initials

W Zhang,HM Chan,Y Gao,R Poon,Z Wu,

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BS69 is involved in cellular senescence through the p53-p21Cip1 pathway. Journal Published:

PUBLICATION TYPE: Research Support, Non-U.S. Gov

Journal: EMBO reports

VOLUME: 8

Page Numbers: 952-8

Journal Abbreviation: EMBO Rep.

ISSN: 1469-221X

DAY: 24

MONTH: 08

YEAR: 2007

BS69 is involved in cellular senescence through the p53-p21Cip1 pathway. Information

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LANGUAGE: eng

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Grant and Affiliation Information for BS69 is involved in cellular senescence through the p53-p21Cip1 pathway.

AFFILIATION: Department of Biochemistry, Hong Kong University of Science and Technology, Clear Water Bay, Kowloon, Hong Kong.

Country: England

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MEDLINETA: EMBO Rep

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