Extracellular Signal-Regulated Kinase 2-Dependent Phosphorylation Induces Cytoplasmic Localization and Degradation of p21(Cip1)

Authors
Hwang, Chae YoungLee, CheoljuKwon, Ki-Sun
Issue Date
2009-06-15
Publisher
AMER SOC MICROBIOLOGY
Citation
MOLECULAR AND CELLULAR BIOLOGY, v.29, no.12, pp.3379 - 3389
Abstract
p21(Cip1) is an inhibitor of cell cycle progression that promotes G(1)-phase arrest by direct binding to cycl-independent kinase and proliferating cell nuclear antigen. Here we demonstrate that mitogenic stimuli, such as epidermal growth factor treatment and oncogenic Ras transformation, induce p21(Cip1) downregulation at the posttranslational level. This downregulation requires the sustained activation of extracellular signal-regulated kinase 2 (ERK2), which directly interacts with and phosphorylates p21(Cip1), promoting p21(Cip1) nucleocytoplasmic translocation and ubiquitin-dependent degradation, thereby resulting in cell cycle progression. ERK1 is not likely involved in this process. Phosphopeptide analysis of in vitro ERK2-phosphorylated p21(Cip1) revealed two phosphorylation sites, Thr57 and Ser130. Double mutation of these sites abolished ERK2-mediated p21(Cip1) translocation and degradation, thereby impairing ERK2-dependent cell cycle progression at the G(1)/S transition. These results indicate that ERK2 activation transduces mitogenic signals, at least in part, by downregulating the cell cycle inhibitory protein p21(Cip1).
Keywords
ACTIVATED PROTEIN-KINASE; CYCLIN-DEPENDENT KINASES; CDK INHIBITORS; UV-IRRADIATION; PCNA BINDING; MAP KINASE; S-PHASE; P21; PROTEASOME; P21(WAF1/CIP1); ACTIVATED PROTEIN-KINASE; CYCLIN-DEPENDENT KINASES; CDK INHIBITORS; UV-IRRADIATION; PCNA BINDING; MAP KINASE; S-PHASE; P21; PROTEASOME; P21(WAF1/CIP1)
ISSN
0270-7306
URI
https://pubs.kist.re.kr/handle/201004/132393
DOI
10.1128/MCB.01758-08
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KIST Article > 2009
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