College of Integrated Chinese and Western Medicine, Hebei University of Chinese Medicine, Shijiazhuang 050035, China.
College of Integrated Chinese and Western Medicine, Hebei University of Chinese Medicine, Shijiazhuang 050035, China; New Drug Evaluation Center, Shijiazhuang Yiling Pharmaceutical Co., Ltd, Shijiazhuang 050035, China.
Phytomedicine. 2023 Apr;112:154688. doi: 10.1016/j.phymed.2023.154688. Epub 2023 Jan 31.
Sophoridine (SR) has shown the potential to be an antiarrhythmic agent. However, SR's electrophysiological properties and druggability research are relatively inadequate, which limits the development of SR as an antiarrhythmic candidate.
To facilitate the development process of SR as an antiarrhythmic candidate, we performed integrated studies on the electrophysiological properties of SR in vitro and ex vivo to gain more comprehensive insights into the multi-ion channel blocking effects of SR, which provided the foundation for the further drugability studies in antiarrhythmic and safety studies. Firstly, SR's electrophysiological properties and antiarrhythmic potentials were recorded and assessed at the cell and tissue levels by comprehensively integrating the patch clamp with the Electrical and Optical Mapping systems. Subsequently, the antiarrhythmic effects of SR were validated by aconitine and ouabain-induced arrhythmia in vivo. Finally, the safety of SR as an antiarrhythmic candidate compound was evaluated based on the guidelines of the Comprehensive in Vitro Proarrhythmia Assay (CiPA).
The antiarrhythmic effect of SR was evaluated at the in vitro, ex vivo, and in vivo levels.
Isolated primary cardiomyocytes and stable cell lines were prepared to explore the electrophysiologic properties of being a multiple ion-channel blocker in vitro by whole-cell patch clamp. Using electrical and optical mapping, the negative chronotropic effect of SR was determined in langendorff-perfused rat or guinea-pig hearts.The antiarrhythmic activity of SR was assessed by the ex vivo tachyarrhythmia models induced by left coronary artery ligation (LCAL) and isoproterenol (ISO). Canonical models of aconitine and ouabain-induced arrhythmia were used to verify the antiarrhythmic effects in vivo. Finally, the pro-arrhythmic risk of SR was detected in Human-Induced Pluripotent Stem Cell-Derived Cardiomyocytes (hSCCMs) using a Microelectrode array (MEA).
Single-cell patch assay validated the multiple ion-channel blockers of SR in transient outward current potassium currents (Ito), l-type calcium currents (ICa-l), and rapid activation delayed rectifier potassium currents (IKr). SR ex vivo depressed heart rates (HR) and ventricular conduction velocity (CV) and prolonged Q-T intervals in a concentration-dependent manner. Consistent with the changes in HRs, SR extended the active time of hearts and increased the action potential duration measured at 90% repolarization (APD90). SR could also significantly lengthen the onset time and curtail the duration of spontaneous ventricular tachycardia (VT) in the ex vivo arrhythmic model induced by LCAL. Meanwhile, SR could also significantly upregulate the programmed electrical stimulation (PES) frequency after the ISO challenge in forming electrical alternans and re-entrant excitation. Furthermore, SR exerted antiarrhythmic effects in the tachyarrhythmia models induced by aconitine and ouabain in vivo. Notably, the pro-arrhythmic risk of SR was shallow for a moderate inhibition of the human ether-à-go-go-related gene (hERG) channel. Moreover, SR prolonged field potential duration (FPDc) of hSCCMs in a concentration-dependent manner without early after depolarization (EAD) and arrhythmia occurrence.
Our results indicated that SR manifested as a multiple ion-channel blocker in the electrophysiological properties and exerts antiarrhythmic effects ex vivo and in vivo. Meanwhile, due to the low pro-arrhythmic risk in the hERG inhibition assay and the induction of EAD, SR has great potential as a leading candidate in the treatment of ventricular tachyarrhythmia.
槐定碱(SR)已显示出作为抗心律失常药物的潜力。然而,SR 的电生理特性和可药性研究相对不足,这限制了 SR 作为抗心律失常候选药物的发展。
为了促进 SR 作为抗心律失常候选药物的开发进程,我们在体外和体内水平上对 SR 的电生理特性进行了综合研究,以更全面地了解 SR 对多种离子通道的阻断作用,为进一步的抗心律失常和安全性研究中的药物开发提供了基础。首先,通过综合整合膜片钳与电光学映射系统,在细胞和组织水平上记录和评估了 SR 的电生理特性和抗心律失常潜力。随后,通过在体乌头碱和哇巴因诱导的心律失常验证了 SR 的抗心律失常作用。最后,根据全面体外致心律失常试验(CiPA)的指导原则评估了 SR 作为抗心律失常候选化合物的安全性。
在体外、体内和体内水平评估了 SR 的抗心律失常作用。
制备分离的原代心肌细胞和稳定细胞系,通过全细胞膜片钳技术研究 SR 作为多种离子通道阻断剂的体外电生理特性。利用电光学映射技术,在 Langendorff 灌注的大鼠或豚鼠心脏中确定 SR 的负变时作用。通过左冠状动脉结扎(LCAL)和异丙肾上腺素(ISO)诱导的体外心动过速模型评估 SR 的抗心律失常活性。使用乌头碱和哇巴因诱导的心律失常的典型模型在体内验证其抗心律失常作用。最后,利用微电极阵列(MEA)在人诱导多能干细胞衍生的心肌细胞(hSCCMs)中检测 SR 的致心律失常风险。
单细胞膜片钳实验验证了 SR 对瞬时外向钾电流(Ito)、L 型钙电流(ICa-l)和快速激活延迟整流钾电流(IKr)的多离子通道阻断作用。SR 在体外以浓度依赖的方式降低心率(HR)和心室传导速度(CV),并延长 Q-T 间期。与 HR 的变化一致,SR 延长了心脏的激活时间,并增加了在 90%复极时测量的动作电位持续时间(APD90)。SR 还可以显著延长 LCAL 诱导的体外心律失常模型中自发性室性心动过速(VT)的起始时间,并缩短其持续时间。同时,SR 还可以在 ISO 挑战后显著上调程控电刺激(PES)频率,形成电交替和折返兴奋。此外,SR 在体内乌头碱和哇巴因诱导的心动过速模型中发挥了抗心律失常作用。值得注意的是,SR 对人 ether-à-go-go-related gene(hERG)通道的中度抑制表现出低致心律失常风险。此外,SR 以浓度依赖的方式延长 hSCCMs 的场电位持续时间(FPDc),而无早期后除极(EAD)和心律失常发生。
我们的结果表明,SR 在电生理特性上表现为多种离子通道阻断剂,并在体外和体内发挥抗心律失常作用。同时,由于 hERG 抑制试验和 EAD 诱导的致心律失常风险较低,SR 作为治疗室性心动过速的候选药物具有很大的潜力。
