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DJ-1 cooperates with PYCR1 in cell protection against oxidative stress.

Biochem Biophys Res Commun. 2013 Jun 28;436(2):289-94. Epub 2013 Jun 04
Tatsuki Yasuda 1 , Yusuke Kaji , Tomohiro Agatsuma , Takeshi Niki , Mitsuhiro Arisawa , Satoshi Shuto , Hiroyoshi Ariga , Sanae M M Iguchi-Ariga
Tatsuki Yasuda 1 , Yusuke Kaji , Tomohiro Agatsuma , Takeshi Niki , Mitsuhiro Arisawa , Satoshi Shuto , Hiroyoshi Ariga , Sanae M M Iguchi-Ariga
+ et al

[No authors listed]

Author information
  • 1 Graduate School of Life Science, Hokkaido University, Sapporo 060-8589, Japan.

摘要


DJ-1, a product of the DJ-1/PARK7 gene, has been suggested to play various functions involved in transcriptional regulation, protease activity, anti-oxidative stress activity, and regulation of mitochondrial complex I. Such a variety of functions of DJ-1 are supposed to be realized through interactions with different partner proteins. Among the candidates for DJ-1-partner proteins detected in TOF-MAS analyses of the cellular proteins co-immunoprecipitated with DJ-1, we focused here pyrroline-5-carboxylate reductase 1, PYCR1, a final key enzyme for proline biosynthesis. DJ-1 directly bound to PYCR1 in vivo and in vitro. DJ-1 and PYCR1 colocalized in mitochondria, and both were suggested to be involved in regulation of mitochondrial membrane potential, but differently. DJ-1 enhanced the enzymatic activity of PYCR1 in vitro. The cells knocked down for DJ-1 and PYCR1 showed lower viability under oxidative stress conditions. No additive nor synergistic results were obtained for the cells that had been knocked down for both DJ-1 and PYCR1, suggesting that DJ-1 and PYCR1 are on the same pathway of anti-oxidative stress protection of the cells.