Kambayashi Ryuichi, Izumi-Nakaseko Hiroko, Goto Ai, Tsurudome Kazuya, Ohshiro Hironori, Izumi Taku, Hagiwara-Nagasawa Mihoko, Chiba Koki, Nishiyama Ryota, Oyama Satomi, Nunoi Yoshio, Takei Yoshinori, Matsumoto Akio, Sugiyama Atsushi
Department of Pharmacology, Faculty of Medicine, Toho University, Tokyo, Japan.
Sophion Bioscience K.K., Saitama, Japan.
Front Pharmacol. 2021 Apr 29;12:593021. doi: 10.3389/fphar.2021.593021. eCollection 2021.
Oseltamivir has been shown to prolong the atrial conduction time and effective refractory period, and to suppress the onset of burst pacing-induced atrial fibrillation . To better predict its potential clinical benefit as an anti-atrial fibrillatory drug, we performed translational studies by assessing anti-atrial fibrillatory effect along with and electropharmacological analyses. Oseltamivir in intravenous doses of 3 (n = 6) and 30 mg/kg (n = 7) was administered in conscious state to the persistent atrial fibrillation model dogs to confirm its anti-atrial fibrillatory action. The model was prepared by tachypacing to the atria of chronic atrioventricular block dogs for > 6 weeks. Next, oseltamivir in doses of 0.3, 3 and 30 mg/kg was intravenously administered to the halothane-anesthetized intact dogs to analyze its electrophysiological actions (n = 4). Finally, its effects of 10-1,000 μM on I, I, I, I and I were analyzed by using cell lines stably expressing Kir3.1/3.4, K1.5, hERG, Na1.5 or Ca1.2, respectively (n = 3 for I and I or n = 6 for I, I and I). Oseltamivir in doses of 3 and 30 mg/kg terminated the atrial fibrillation in 1 out of 6 and in 6 out of 7 atrial fibrillation model dogs, respectively without inducing any lethal ventricular arrhythmia. Its 3 and 30 mg/kg delayed inter-atrial conduction in a frequency-dependent manner, whereas they prolonged atrial effective refractory period in a reverse frequency-dependent manner in the intact dogs. The current assay indicated that IC values for I and I were 160 and 231 μM, respectively, but 1,000 µM inhibited I, I and I by 22, 19 and 13%, respectively. The extent of I blockade was enhanced at faster beating rate and more depolarized resting membrane potential. Oseltamivir effectively terminated the persistent atrial fibrillation, which may be largely due to the prolongation of the atrial effective refractory period and inter-atrial conduction time induced by I and I inhibitions along with I suppression. Thus, oseltamivir can exert a powerful anti-atrial fibrillatory action through its ideal multi-channel blocking property; and oseltamivir would become a promising seed compound for developing efficacious and safe anti-atrial fibrillatory drugs.
已证实奥司他韦可延长心房传导时间和有效不应期,并抑制猝发起搏诱发的心房颤动的发作。为了更好地预测其作为抗心房颤动药物的潜在临床益处,我们通过评估抗心房颤动作用以及电药理学分析进行了转化研究。将静脉注射剂量为3(n = 6)和30mg/kg(n = 7)的奥司他韦在清醒状态下给予持续性心房颤动模型犬,以确认其抗心房颤动作用。该模型通过对慢性房室传导阻滞犬的心房进行快速起搏>6周来制备。接下来,将剂量为0.3、3和30mg/kg的奥司他韦静脉注射给氟烷麻醉的完整犬,以分析其电生理作用(n = 4)。最后,分别使用稳定表达Kir3.1/3.4、K1.5、hERG、Na1.5或Ca1.2的细胞系分析其10 - 1000μM对I、I、I、I和I的作用(I和I的n = 3,I、I和I的n = 6)。剂量为3和30mg/kg的奥司他韦分别使6只心房颤动模型犬中的1只和7只中的6只的心房颤动终止,且未诱发任何致命性室性心律失常。其3和30mg/kg以频率依赖性方式延迟心房间传导,而在完整犬中它们以反向频率依赖性方式延长心房有效不应期。电流测定表明,I和I的IC值分别为160和231μM,但1000μM分别抑制I、I和I 22%、19%和13%。I阻断的程度在更快的搏动频率和更去极化的静息膜电位时增强。奥司他韦有效地终止了持续性心房颤动,这可能很大程度上归因于I和I抑制以及I抑制所诱导的心房有效不应期和心房间传导时间的延长。因此,奥司他韦可通过其理想的多通道阻断特性发挥强大的抗心房颤动作用;并且奥司他韦将成为开发有效且安全的抗心房颤动药物的有前景的先导化合物。
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