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Issue title: The Fifth Conference of the International CoQ10 Association, Kobe 2007 – 50th anniversary of CoQ10 discovery
Article type: Research Article
Authors: Takahashi, Takayuki; | Okuno, Masaaki; | Okamoto, Tadashi; | Kishi, Takeo
Affiliations: Laboratory of Biochemistry, Department of Health Sciences and Social Pharmacy, Faculty of Pharmaceutical Sciences, Kobe Gakuin University, Kobe, Japan | Cooperative Research Center of Life Sciences, Kobe Gakuin University, Kobe, Japan
Note: [] Corresponding author. Tel.: +81 78 974 1551; Fax: +81 78 974 4102; E-mail: [email protected]
Abstract: We purified an NADPH-dependent coenzyme Q reductase (NADPH-CoQ reductase) in rat liver cytosol and compared its enzymatic properties with those of the other CoQ_{10} reductases such as NADPH: quinone acceptor oxidoreductase 1 (NQO1), lipoamide dehydrogenase, thioredoxine reductase and glutathione reductase. NADPH-CoQ reductase was the only enzyme that preferred NADPH to NADH as an electron donor and was also different from the other CoQ_{10} reductases in the sensitivities to its inhibitors and stimulators. Especially, Zn^{2+} was the most powerful inhibitor for NADPH-CoQ reductase, but CoQ_{10} reduction by the other CoQ_{10} reductases could not be inhibited by Zn^{2+}. Furthermore, the reduction of the CoQ_{9} incorporated into HeLa cells was also inhibited by Zn^{2+} in the presence of pyrithione, a zinc ionophore. Moreover, NQO1 gene silencing in HeLa cells by transfection of a small interfering RNA resulted in lowering of both the NQO1 protein level and the NQO1 activity by about 75%. However, this transfection did not affect the NADPH-CoQ reductase activity and the reduction of CoQ_{9} incorporated into the cells. These results suggest that the NADPH-CoQ reductase located in cytosol may be the main enzyme responsible for the reduction of non-mitochondrial CoQ in cells.
Keywords: Antioxidant, coenzyme Q, NADPH-CoQ reductase, rat liver, ubiquinol, zinc
Journal: BioFactors, vol. 32, no. 1-4, pp. 59-70, 2008
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