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JNK1: a Protein Kinase Stimulated by UV Light and Ha-Ras That Binds and Phosphorylates the C-Jun Activation Domain

Overview
Journal Cell
Publisher Cell Press
Specialty Cell Biology
Date 1994 Mar 25
PMID 8137421
Citations 847
Authors
B Derijard
M Hibi
I H Wu
T Barrett
B Su
T Deng
M Karin
R J Davis
Affiliations
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Abstract

The ultraviolet (UV) response of mammalian cells is characterized by a rapid and selective increase in gene expression mediated by AP-1 and NF-kappa B. The effect on AP-1 transcriptional activity results, in part, from enhanced phosphorylation of the c-Jun NH2-terminal activation domain. Here, we describe the molecular cloning and characterization of JNK1, a distant relative of the MAP kinase group that is activated by dual phosphorylation at Thr and Tyr during the UV response. Significantly, Ha-Ras partially activates JNK1 and potentiates the activation caused by UV. JNK1 binds to the c-Jun transactivation domain and phosphorylates it on Ser-63 and Ser-73. Thus, JNK1 is a component of a novel signal transduction pathway that is activated by oncoproteins and UV irradiation. These properties indicate that JNK1 activation may play an important role in tumor promotion.

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