Author:
Fuchs Serge Y.,Adler Victor,Buschmann Thomas,Yin Zhimin,Wu Xiangwei,Jones Stephen N.,Ronai Ze’ev
Abstract
In this study we elucidated the role of nonactive JNK in regulating p53 stability. The amount of p53–JNK complex was inversely correlated with p53 level. A peptide corresponding to the JNK binding site on p53 efficiently blocked ubiquitination of p53. Similarly, p53 lacking the JNK binding site exhibits a longer half-life than p53wt. Outcompeting JNK association with p53 increased the level of p53, whereas overexpression of a phosphorylation mutant form of JNK inhibited p53 accumulation. JNK–p53 and Mdm2–p53 complexes were preferentially found in G0/G1and S/G2M phases of the cell cycle, respectively. Altogether, these data indicate that JNK is an Mdm2-independent regulator of p53 stability in nonstressed cells.
Publisher
Cold Spring Harbor Laboratory
Subject
Developmental Biology,Genetics