In vivo cardiovascular profile of ryanodine receptor 2 inhibitor M201-A: Utility as an anti-atrial fibrillatory drug for patients suffering from heart failure with preserved ejection fraction

IF 3 3区 医学 Q2 PHARMACOLOGY & PHARMACY Journal of pharmacological sciences Pub Date : 2024-08-22 DOI:10.1016/j.jphs.2024.08.004
Ryuichi Kambayashi , Ai Goto , Makoto Shinozaki , Hiroko Izumi-Nakaseko , Yoshinori Takei , Kunio Iwata , Noboru Kaneko , Atsushi Sugiyama
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Abstract

Atrial fibrillation (AF) and heart failure with preserved ejection fraction (HFpEF) often coexist; however, clinically available anti-AF drugs can exacerbate symptoms of HFpEF. M201-A suppressed ryanodine receptor-mediated diastolic Ca2+ leakage, possibly inhibiting common pathological processes toward AF and HFpEF. To bridge the basic information to clinical practice, we assessed its cardiohemodynamic, anti-AF and ventricular proarrhythmic profile using halothane-anesthetized dogs (n = 4). M201-A hydrochloride in doses of 0.03, 0.3 and 3 mg/kg/10 min was intravenously administered, providing peak plasma concentrations of 0.09, 0.81 and 5.70 μg/mL, respectively. The high dose of M201-A showed various cardiovascular actions. Namely, M201-A increased mean blood pressure and tended to enhance isovolumetric ventricular relaxation without suppressing ventricular contraction or decreasing cardiac output. M201-A enhanced atrioventricular conduction, but hardy affected intra-atrial/ventricular conduction. Importantly, M201-A prolonged effective refractory period more potently in the atrium than in the ventricle, indicating that it may become an atrial-selective antiarrhythmic drug. Meanwhile, M201-A prolonged QT interval/QTcV, and showed reverse frequency-dependent delay of ventricular repolarization. M201-A prolonged J-Tpeakc without prolonging Tpeak-Tend or terminal repolarization period, indicating the risk of causing torsade de pointes is negligible. Thus, M201-A is expected to become a hopeful therapeutic strategy for patients having pathology of both AF and HFpEF.

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雷诺丁受体 2 抑制剂 M201-A 的体内心血管特征:作为射血分数保留型心力衰竭患者抗心房颤动药物的用途
心房颤动(房颤)和射血分数保留型心力衰竭(HFpEF)常常同时存在;然而,临床上可用的抗房颤药物会加重HFpEF的症状。M201-A抑制了雷诺丁受体介导的舒张期Ca2+渗漏,可能抑制了房颤和射血分数保留型心力衰竭的共同病理过程。为了将基础信息与临床实践相结合,我们使用氟烷麻醉狗(n = 4)评估了 M201-A 的心血流动力学、抗房颤和室性心律失常特性。静脉注射盐酸 M201-A 的剂量分别为 0.03、0.3 和 3 毫克/千克/10 分钟,血浆峰浓度分别为 0.09、0.81 和 5.70 微克/毫升。高剂量的 M201-A 显示出多种心血管作用。也就是说,M201-A 能升高平均血压,并有增强等容心室松弛的趋势,而不会抑制心室收缩或降低心输出量。M201-A 可增强房室传导,但对心房内/心室传导有一定影响。重要的是,M201-A 延长心房有效折返期的作用强于心室,这表明它可能是一种心房选择性抗心律失常药物。同时,M201-A 可延长 QT 间期/QTcV,并表现出心室复极化的反向频率依赖性延迟。M201-A 可延长 J-Tpeakc 而不延长 Tpeak-Tend 或终末复极期,这表明其引起心动过速的风险可以忽略不计。因此,M201-A有望成为同时具有房颤和高频心衰病理特征的患者的一种治疗策略。
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来源期刊
CiteScore
6.20
自引率
2.90%
发文量
104
审稿时长
31 days
期刊介绍: Journal of Pharmacological Sciences (JPS) is an international open access journal intended for the advancement of pharmacological sciences in the world. The Journal welcomes submissions in all fields of experimental and clinical pharmacology, including neuroscience, and biochemical, cellular, and molecular pharmacology for publication as Reviews, Full Papers or Short Communications. Short Communications are short research article intended to provide novel and exciting pharmacological findings. Manuscripts concerning descriptive case reports, pharmacokinetic and pharmacodynamic studies without pharmacological mechanism and dose-response determinations are not acceptable and will be rejected without peer review. The ethnopharmacological studies are also out of the scope of this journal. Furthermore, JPS does not publish work on the actions of biological extracts unknown chemical composition.
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