Acetylcholine Inhibits the Hypoxia-Induced Reduction of Connexin43 Protein in Rat Cardiomyocytes
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概要
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In a recent study, we demonstrated that vagal stimulation increases the survival of rats with myocardial infarction by inhibiting lethal arrhythmia through regulation of connexin43 (Cx43). However, the precise mechanisms for this effect remain to be elucidated. To investigate these mechanisms and the signal transduction for gap junction regulation, we investigated the effect of acetylcholine (ACh), a parasympathetic nerve system neurotransmitter, on the gap junction component Cx43 using H9c2 cells. When cells were subjected to hypoxia, the total Cx43 protein level was decreased. In contrast, pretreatment with ACh inhibited this effect. To investigate the signal transduction, cells were pretreated with <sc>L</sc>-NAME, a nitric oxide synthase inhibitor, followed by ACh and hypoxia. <sc>L</sc>-NAME was found to suppress the ACh effect. However, a NO donor, SNAP, partially inhibited the hypoxia-induced reduction in Cx43. To delineate the mechanisms of the decrease in Cx43 under hypoxia, cells were pretreated with MG132, a proteasome inhibitor. Proteasome inhibition produced a striking recovery of the decrease in the total Cx43 protein level under hypoxia. However, cotreatment with MG132 and ACh did not produce any further increase in the total Cx43 protein level. Functional studies using ACh or okadaic acid, a phosphatase inhibitor, revealed that both reagents inhibited the decrease in the dye transfer induced by hypoxia. These results suggest that ACh is responsible for restoring the decrease in the Cx43 protein level, resulting in functional activation of gap junctions.
- 社団法人 日本薬理学会の論文
- 2006-07-20
著者
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Sato Takayuki
Department of Cardiovascular Control, Kochi Medical School
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YAMASAKI Fumiyasu
Department of Clinical Laboratory, Kochi Medical School Hospital
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Yamasaki Fumiyasu
Department Of Clinical Laboratory Kochi Medical School
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Yamasaki Fumiyasu
高知大学 医学部循環制御学
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Yamasaki Fumiyasu
Deparment Of Clinical Laboratory Kochi Medical School
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Sato Takayuki
Department Of Cardiovascular Control Kochi Medical School
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Satoh Takayuki
Department Of Cardiovascular Control Kochi Medical School
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SUGIURA Tetsuro
Department of Laboratory Medicine, Kochi Medical School
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Zhang Yanan
Department Of Clinical Laboratory Kochi Medical School
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Kakinuma Yoshihiko
Department of Cardiovascular Control, Kochi Medical School
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Sugiura Tetsuro
Department Of Clinical Laboratory Medicine Kochi University
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ANDO Motonori
Department of Cardiovascular Control, Kochi Medical School
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KATARE Rajesh
Department of Cardiovascular Control, Kochi Medical School
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Katare G.
高知大学 医学部循環制御学
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Ando Motonori
Department Of Science Education Okayama University
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Rajesh Katare
Department Of Cardiovascular Control Kochi Medical School
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Katare Rajesh
Department Of Cardiovascular Control Kochi Medical School
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Sato Takayuki
Department Of Cardiovascular Dynamics Advanced Medical Engineering Center National Cardiovascular Ce
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Kakinuma Yoshihiko
Department Of Cardiovascular Control Kochi Medical School
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Sato Takayuki
Department Of Cadiovascula Dynamics National Cardiovascular Center Research Institute
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Andoh Motonori
Department Of Cardiovascular Control Kochi Medical School
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Yamasaki Fumiyasu
Department Of Laboratory Medicine Kochi Medical School
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Sugiura Tetsuro
Department Of Clinical Laboratory Medicine Kochi Medical School
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Sato Takayuki
Department Of Cardiovascular Control Kochi University Kochi Medical School
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Sato Takayuki
Department Of Biomolecular Engineering Graduate School Of Bioscience And Biotechnology Tokyo Institu
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