Inhibition of Mitochondrial Respiratory Chain by Arylthiolated 2, 3-Ethylenedioxy-1, 4-benzoquinones

• Published in: Chemical & pharmaceutical bulletin Vol. 38; no. 4; pp. 1100 - 1103
• Main Authors: KISHI, Takeo, OKAMOTO, Tadashi, HAMA, Shihoko, SAYO, Hiroteru, KATO, Fumino, MORI, Koichi
• Format: Journal Article
• Language: English
• Published: Tokyo The Pharmaceutical Society of Japan 01.01.1990; 公益社団法人日本薬学会; Maruzen
• Subjects: Animals; arylthiolated 2, 3-ethylenedioxyl-1, 4-benzoquinone; beef heart mitochondria; benzoquinone; Biological and medical sciences; Cattle; Cell structures and functions; coenzyme Q; coenzyme Q analog; cytochrome; difference spectra; electron transport; Fundamental and applied biological sciences. Psychology; In Vitro Techniques; Mitochondria and cell respiration; Mitochondria, Heart - drug effects; Mitochondria, Heart - metabolism; Molecular and cellular biology; NADH oxidase; Oxygen Consumption - drug effects; Quinones - pharmacology; respiratory chain; structure-activity; Subcellular Fractions - drug effects; Subcellular Fractions - metabolism; succinate oxidase; Heart; Vertebrata; Mitochondria; Mammalia; Bovine; Structure activity relation; Benzoquinone derivatives; Artiodactyla; Antagonist; Inhibition; Ungulata; Site of action
• ISSN: 0009-2363; 1347-5223
• DOI: 10.1248/cpb.38.1100

A series of arylthiolated 2, 3-ethylenedioxy-1, 4-benzoquinones as a coenzyme Q (CoQ) antagonist was tested for inhibition of succinate oxidase and reduced nicotinamide adenine dinucleotide (NADH) oxidase systems in the mitochondrial respiratory chain. The following characteristics were revealed : (1) 2, 3-ethylenedioxy, 5-arylthio and 5, 6-diarylthio groups were confirmed to be favorable for inhibition of both systems; (2) these analogs were more effective in the succinate oxidase system than in the NADH oxidase system; (3) 4' substituents on the benzene side ring had little effect on inhibitory activity; (4) the acting sites of these analogs had no strict stereospecificity. The reduced minus oxidized difference spectra revealed that these analogs inhibited the succinate oxidase system at the site between succinate and CoQ, and the NADH oxidase system at the site after cytochrome a+a3, suggesting these analogs might act as antagonists of CoQ in the succinate oxidase system. However, 5-(4'-nitrophenylthio)-2, 3-ethylenedioxyl-1, 4-benzoquinone (If) strongly inhibited only the succinate oxidase system at the site after cytochrome a+a3.