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A posttranslational modification cascade involving p38, Tip60, and PRAK mediates oncogene-induced senescence.


ABSTRACT: Oncogene-induced senescence is an important tumor-suppressing defense mechanism. However, relatively little is known about the signaling pathway mediating the senescence response. Here, we demonstrate that a multifunctional acetyltransferase, Tip60, plays an essential role in oncogenic ras-induced senescence. Further investigation reveals a cascade of posttranslational modifications involving p38, Tip60, and PRAK, three proteins that are essential for ras-induced senescence. Upon activation by ras, p38 induces the acetyltransferase activity of Tip60 through phosphorylation of Thr158; activated Tip60 in turn directly interacts with and induces the protein kinase activity of PRAK through acetylation of K364 in a manner that depends on phosphorylation of both Tip60 and PRAK by p38. These posttranslational modifications are critical for the prosenescent function of Tip60 and PRAK, respectively. These results have defined a signaling pathway that mediates oncogene-induced senescence, and identified posttranslational modifications that regulate the enzymatic activity and biological functions of Tip60 and PRAK.

SUBMITTER: Zheng H 

PROVIDER: S-EPMC3679363 | biostudies-literature | 2013 Jun

REPOSITORIES: biostudies-literature

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A posttranslational modification cascade involving p38, Tip60, and PRAK mediates oncogene-induced senescence.

Zheng Hui H   Seit-Nebi Alim A   Han Xuemei X   Aslanian Aaron A   Tat John J   Liao Rong R   Yates John R JR   Sun Peiqing P  

Molecular cell 20130516 5


Oncogene-induced senescence is an important tumor-suppressing defense mechanism. However, relatively little is known about the signaling pathway mediating the senescence response. Here, we demonstrate that a multifunctional acetyltransferase, Tip60, plays an essential role in oncogenic ras-induced senescence. Further investigation reveals a cascade of posttranslational modifications involving p38, Tip60, and PRAK, three proteins that are essential for ras-induced senescence. Upon activation by r  ...[more]

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