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ID 116316
Title Alternative
Regulation of NR4A nuclear receptors by p38
Author
Sekine, Yusuke The University of Tokyo
Takagahara, Shuichi The University of Tokyo
Hatanaka, Ryo The University of Tokyo
Oguchi, Haruka The University of Tokyo
Noguchi, Takuya The University of Tokyo
Naguro, Isao The University of Tokyo
Kobayashi, Kazuto Fukushima Medical University
Tsunoda, Makoto The University of Tokyo
Funatsu, Takashi The University of Tokyo
Nomura, Hiroshi The University of Tokyo
Toyoda, Takeshi The University of Tokyo
Matsuki, Norio The University of Tokyo
Kuranaga, Erina The University of Tokyo|RIKEN
Miura, Masayuki The University of Tokyo
Takeda, Kohsuke The University of Tokyo
Ichijo, Hidenori The University of Tokyo
Keywords
p38 MAPK
NR4A nuclear receptor
Tyrosine hydroxylase
Stress response
Content Type
Journal Article
Description
In Drosophila, the melanization reaction is an important defense mechanism against injury and invasion of microorganisms. Drosophila tyrosine hydroxylase (TH, also known as Pale) and dopa decarboxylase (Ddc), key enzymes in the dopamine synthesis pathway, underlie the melanin synthesis by providing the melanin precursors dopa and dopamine, respectively. It has been shown that expression of Drosophila TH and Ddc is induced in various physiological and pathological conditions, including bacterial challenge; however, the mechanism involved has not been fully elucidated. Here, we show that ectopic activation of p38 MAPK induces TH and Ddc expression, leading to upregulation of melanization in the Drosophila cuticle. This p38-dependent melanization was attenuated by knockdown of TH and Ddc, as well as by that of Drosophila HR38, a member of the NR4A family of nuclear receptors. In mammalian cells, p38 phosphorylated mammalian NR4As and Drosophila HR38 and potentiated these NR4As to transactivate a promoter containing NR4A-binding elements, with this transactivation being, at least in part, dependent on the phosphorylation. This suggests an evolutionarily conserved role for p38 MAPKs in the regulation of NR4As. Thus, p38-regulated gene induction through NR4As appears to function in the dopamine synthesis pathway and may be involved in immune and stress responses.
Journal Title
Journal of Cell Science
ISSN
00219533
14779137
NCID
AA00694823
AA11720335
Publisher
The Company of Biologists
Volume
124
Issue
17
Start Page
3006
End Page
3016
Published Date
2011-09-01
EDB ID
DOI (Published Version)
URL ( Publisher's Version )
FullText File
language
eng
TextVersion
Publisher
departments
Medical Sciences