AstraZeneca R&D, CVGI Innovative Medicine, Bioscience, Mölndal, Sweden.
J Cardiovasc Pharmacol Ther. 2013 May;18(3):290-300. doi: 10.1177/1074248412470512. Epub 2013 Jan 10.
To examine the electrophysiological, hemodynamic, and antiarrhythmic effects of the novel antiarrhythmic agent AZ13395438.
The ion channel-blocking potency of AZ13395438 was assessed in Chinese hamster ovary cells stably expressing various human cardiac ion channels and in human atrial myocytes. The in vivo electrophysiological, hemodynamic, and antiarrhythmic effects of intravenously administered AZ13395438 were examined in anesthetized rabbits, in anesthetized naive dogs, and in dogs subjected to rapid atrial pacing (RAP) for 8 weeks. Pharmacokinetic/pharmacodynamic (PKPD) modeling was applied to predict the potency of AZ13395438 in increasing atrial and ventricular refractoriness.
AZ13395438 potently and predominantly blocked the atrial repolarizing potassium currents I(Kur), I(Ach), and I(to) in vitro. In vivo, AZ13395438 caused a concentration-dependent and selective increase in atrial refractoriness with no or small effects on ventricular refractoriness and repolarization and on hemodynamics in both rabbits and dogs. The PKPD modeling predicted unbound plasma concentrations of AZ13395438 of 0.20 ± 0.039, 0.38 ± 0.084, and 0.34 ± 0.057 µmol/L to increase the right atrial effective refractory period by 20 milliseconds in the rabbit and in the naive and the RAP dogs, respectively. In the RAP dog with atrial fibrillation (AF), AZ13395438 significantly increased AF cycle length and successfully converted AF to sinus rhythm in 12 of the 12 occasions at an unbound plasma concentration of 0.48 ± 0.076 µmol/L. During saline infusion, conversion was seen only in 4 of the 10 occasions (P = .003 vs AZ13395438). Furthermore, AZ13395438 reduced AF inducibility by burst pacing from 100% to 25% (P < .001).
AZ13395438 can be characterized as a mixed potassium ion channel-blocking agent that selectively prolongs atrial versus ventricular refractoriness and shows promising antiarrhythmic efficacy in a clinically relevant animal model of AF.
研究新型抗心律失常药物 AZ13395438 的电生理、血流动力学和抗心律失常作用。
在稳定表达各种人心血管离子通道的中国仓鼠卵巢细胞和人心房肌细胞中评估 AZ13395438 的离子通道阻断效力。在麻醉兔、麻醉未处理犬和 8 周快速心房起搏(RAP)犬中,静脉给予 AZ13395438 后,检测其体内电生理、血流动力学和抗心律失常作用。应用药代动力学/药效动力学(PKPD)模型预测 AZ13395438 增加心房和心室不应期的效力。
AZ13395438 体外强力且主要抑制心房复极化钾电流 I(Kur)、I(Ach)和 I(to)。体内,AZ13395438 呈浓度依赖性选择性增加心房不应期,对心室不应期和复极以及兔和犬的血流动力学无或仅有轻微影响。PKPD 模型预测 AZ13395438 的游离血浆浓度分别为 0.20 ± 0.039、0.38 ± 0.084 和 0.34 ± 0.057 µmol/L 时,可使兔、未处理犬和 RAP 犬右房有效不应期分别增加 20 毫秒。在 RAP 犬心房颤动(AF)中,AZ13395438 使 AF 周期长度显著增加,在游离血浆浓度为 0.48 ± 0.076 µmol/L 时,12 次中有 12 次成功将 AF 转为窦性心律。在盐水输注期间,仅在 10 次中有 4 次转换(P =.003 与 AZ13395438 相比)。此外,AZ13395438 将起搏诱发 AF 的诱发性从 100%降低至 25%(P <.001)。
AZ13395438 可被描述为一种混合钾离子通道阻断剂,可选择性延长心房与心室不应期,在临床相关的 AF 动物模型中表现出有希望的抗心律失常疗效。
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