クラスId抗不整脈薬ラノラジンのハロセン麻酔犬における心臓安全性薬理学的特徴
Introduction: Vaughan Williams classification was recently updated to include new antiarrhythmic mechanisms, in which class Id action is defined as Nav1.5 late current inhibition. We characterized in vivo cardiac safety pharmacological profile of typical Id drug ranolazine, which can also inhibit hE...
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| Published in | 日本薬理学会年会要旨集 p. 1-O-D3-2 |
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| Main Authors | , , , , , , , , , , |
| Format | Journal Article |
| Language | Japanese |
| Published |
公益社団法人 日本薬理学会
2021
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| Subjects | |
| Online Access | Get full text |
| ISSN | 2435-4953 |
| DOI | 10.1254/jpssuppl.94.0_1-O-D3-2 |
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| Abstract | Introduction: Vaughan Williams classification was recently updated to include new antiarrhythmic mechanisms, in which class Id action is defined as Nav1.5 late current inhibition. We characterized in vivo cardiac safety pharmacological profile of typical Id drug ranolazine, which can also inhibit hERG current. Methods: Ranolazine dihydrochloride in subclinical and clinically relevant doses, 0.3 and 3 mg/kg respectively, was i.v. infused over 10 min to the halothane-anesthetized dogs (n=5). Results: The subclinical dose increased the heart rate, cardiac output and atrioventricular conduction velocity. Meanwhile, the clinically relevant dose decreased the heart rate, ventricular contraction and mean blood pressure, which resulted in indirectly increasing the total peripheral vascular resistance. Also, it delayed the intra-ventricular conduction and ventricular late repolarization without significantly altering the intra-atrial conduction, ventricular early repolarization or post-repolarization refractoriness (PRR). Moreover, it prolonged the atrial and ventricular effective refractory periods. Conclusions: The clinically relevant dose of ranolazine did not alter the ventricular early repolarization or PRR in vivo, indicating the class Id action could attenuate hERG current-inhibition associated torsadogenic potential. |
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| AbstractList | Introduction: Vaughan Williams classification was recently updated to include new antiarrhythmic mechanisms, in which class Id action is defined as Nav1.5 late current inhibition. We characterized in vivo cardiac safety pharmacological profile of typical Id drug ranolazine, which can also inhibit hERG current. Methods: Ranolazine dihydrochloride in subclinical and clinically relevant doses, 0.3 and 3 mg/kg respectively, was i.v. infused over 10 min to the halothane-anesthetized dogs (n=5). Results: The subclinical dose increased the heart rate, cardiac output and atrioventricular conduction velocity. Meanwhile, the clinically relevant dose decreased the heart rate, ventricular contraction and mean blood pressure, which resulted in indirectly increasing the total peripheral vascular resistance. Also, it delayed the intra-ventricular conduction and ventricular late repolarization without significantly altering the intra-atrial conduction, ventricular early repolarization or post-repolarization refractoriness (PRR). Moreover, it prolonged the atrial and ventricular effective refractory periods. Conclusions: The clinically relevant dose of ranolazine did not alter the ventricular early repolarization or PRR in vivo, indicating the class Id action could attenuate hERG current-inhibition associated torsadogenic potential. |
| Author | 神林, 隆一 中瀬古(泉), 寛子 布井, 啓雄 後藤, 愛 廣川, 佳貴 杉山, 篤 渡邉, 善則 長澤(萩原), 美帆子 川合, 眞一 武井, 義則 松本, 明郎 |
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| SubjectTerms | antianginal agent antiarrhythmic agent |
| Title | クラスId抗不整脈薬ラノラジンのハロセン麻酔犬における心臓安全性薬理学的特徴 |
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