Pharmacological Evidence Showing Significant Roles for Potassium Channels and Cytochrome P450 Epoxygenase Metabolites in the Relaxant Effects of Docosahexaenoic Acid on the Rat Aorta Contracted with U46619
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概要
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Docosahexaenoic acid (DHA) shows more pronounced relaxation when blood vessel is contracted with prostanoid receptor agonists than other stimulants. The present study was carried out to obtain information on the mechanisms underlying prostanoid receptor-selective relaxant action of DHA, particularly focusing on the possible roles for K+ channels and its cytochrome P450 (CYP) epoxygenase (EOX) metabolites. In endothelium-denuded rat thoracic aorta, DHA (10-5 M) almost completely relaxed U46619 (a TP receptor agonist)-contracted muscle without substantially affecting noradrenaline (NA)-induced contraction. DHA-induced relaxation was not affected by a BK channel inhibitor iberiotoxin (IbTX, 10-7 M) but was almost abolished by high-KCl (8 x 10-2 M) or 10-2 M tetraethylammonium (TEA) which non-selectively inhibits K+ channel activity. DHA also prominently relaxed U46619-contracted aorta even in the presence of CYP inhibitors (SKF525A or miconazole, each at 10-5 M). However, in the presence of these CYP inhibitors, the relaxant action of DHA was not affected by 10-2 M TEA. In supporting a significant role for CYP EOX metabolites in the blood vessel relaxation to DHA, 16,17-epoxy docosapentaenoic acid (16,17-EpDPE), but not 19,20-EpDPE, showed a potent relaxation in U46619-contracted aorta, and this action was significantly attenuated by 10-2 M TEA. The present findings suggest that the relaxant action of DHA shown in the rat aorta contracted through the stimulation with TP receptor is generated by DHA itself and its CYP EOX metabolites. The relaxant effect of DHA metabolites seems to be partly triggered by the activation of K+ channels though the role for BK channel is insignificant.
- 公益社団法人 日本薬学会の論文
著者
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Aoki Mika
Department Of Cardiology Nagoya University Graduate School Of Medicine
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Obara Keisuke
Department Of Biological Sciences Graduate School Of Science The University Of Tokyo
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Chino Daisuke
Department Of Pharmacology And Pharmacotherapy School Of Medicinal Pharmaceutical Sciences Nihon Pha
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Miyauchi Seiji
Department Of Biochemistry And Molecular Biology Medical College Of Georgia
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SATO Kyosuke
Department of Physiology, Kumamoto University School of Medicine
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Tanaka Yoshio
Department Of Applied Chemistry Faculty Of Engineering Yokohama National University
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Tanaka Yoshio
Department of Pharmacology, Toho University School of Pharmaceutical Sciences
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Miyauchi Seiji
Department of Pharmacokinetics, Toho University School of Pharmaceutical Sciences
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Nishioka Nanako
Department of Pharmacology, Toho University School of Pharmaceutical Sciences
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Kanai Keisuke
Department of Pharmacology, Toho University School of Pharmaceutical Sciences
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Chino Daisuke
Department of Chemical Pharmacology, Toho University School of Pharmaceutical Sciences
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Sato Kyosuke
Department of Chemical Pharmacology, Toho University School of Pharmaceutical Sciences
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Aoki Mika
Department of Pharmacology, Toho University School of Pharmaceutical Sciences
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