Proline, glutamic acid and leucine-rich protein-1 is essential for optimal p53-mediated DNA damage response

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作者
B C Nair
S R Krishnan
G R Sareddy
M Mann
B Xu
M Natarajan
P Hasty
D Brann
R R Tekmal
R K Vadlamudi
机构
[1] University of Texas Health Science Center,
[2] and Cancer Therapy and Research Center,undefined
[3] Molecular Radiation Biology Laboratory,undefined
[4] Research Institute,undefined
[5] Institute of Molecular Medicine and Genetics,undefined
[6] Georgia Reagents University,undefined
来源
Cell Death & Differentiation | 2014年 / 21卷
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摘要
Proline-, glutamic acid- and leucine-rich protein-1 (PELP1) is a scaffolding oncogenic protein that functions as a coregulator for a number of nuclear receptors. p53 is an important transcription factor and tumor suppressor that has a critical role in DNA damage response (DDR) including cell cycle arrest, repair or apoptosis. In this study, we found an unexpected role for PELP1 in modulating p53-mediated DDR. PELP1 is phosphorylated at Serine1033 by various DDR kinases like ataxia-telangiectasia mutated, ataxia telangiectasia and Rad3-related or DNAPKc and this phosphorylation of PELP1 is important for p53 coactivation functions. PELP1-depleted p53 (wild-type) breast cancer cells were less sensitive to various genotoxic agents including etoposide, camptothecin or γ-radiation. PELP1 interacts with p53, functions as p53-coactivator and is required for optimal activation of p53 target genes under genomic stress. Overall, these studies established a new role of PELP1 in DDRs and these findings will have future implications in our understanding of PELP1’s role in cancer progression.
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页码:1409 / 1418
页数:9
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