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麻醉大鼠长期口服Org 7797的抗心律失常、电生理及血流动力学效应

Antiarrhythmic, electrophysiological and haemodynamic effects of prolonged oral dosing with Org 7797 in the anaesthetized rat.

作者信息

Delbressine L, Harris N, Kane K A, Muir A W, Winslow E

机构信息

Organon Laboratories Limited, Newhouse, Lanarkshire, UK.

出版信息

J Pharm Pharmacol. 1992 Dec;44(12):996-1000. doi: 10.1111/j.2042-7158.1992.tb07081.x.

Abstract

The antiarrhythmic, electrophysiological and haemodynamic effects of chronic oral administration of Org 7797 ((16 alpha,17 beta)-17-methylamino-oestra-1,3,5(10)-triene-3, 16-diol-(Z)-2-butonedioate) were studied in rats. During dosing (10 mg kg-1 twice a day for 10 days) no effects on the electrocardiogram, monitored in conscious animals, were observed despite modest reductions (15-18%) in the maximum rate of depolarization of papillary muscle excised 1 or 6 h after completion of the dosing regime. Following anaesthesia, Org 7797 reduced the severity of arrhythmias induced by coronary artery occlusion and prevented the accompanying decrease in the ventricular fibrillation threshold (VFT) at 1 h after completion of dosing. By 6 h the effect on VFT had waned but protection against ischaemia-induced arrhythmias was retained despite a substantial decrease in Org 7797 plasma levels. Drug treatment did not modify arterial blood pressure, heart rate or stroke volume. We conclude that Org 7797 given chronically via the oral route exerts antiarrhythmic actions which may, at least in part, be due to sodium-channel block. In addition, our results suggest the presence of an active metabolite. The protective effects of Org 7797 were seen in the absence of electrocardiographic or haemodynamic changes suggesting that multiple oral doses of Org 7797 do not compromise normal cardiac function.

摘要

在大鼠中研究了长期口服Org 7797((16α,17β)-17-甲基氨基-雌-1,3,5(10)-三烯-3,16-二醇-(Z)-2-丁烯二酸酯)的抗心律失常、电生理和血流动力学效应。给药期间(每天两次,每次10 mg/kg,共10天),尽管在给药方案结束后1或6小时切除的乳头肌最大去极化速率适度降低(15 - 18%),但在清醒动物中监测到对心电图无影响。麻醉后,Org 7797降低了冠状动脉闭塞诱发的心律失常的严重程度,并在给药结束后1小时预防了伴随的心室颤动阈值(VFT)降低。到6小时时,对VFT的影响减弱,但尽管Org 7797血浆水平大幅下降,对缺血诱发的心律失常的保护作用仍然存在。药物治疗未改变动脉血压、心率或每搏输出量。我们得出结论,长期经口给予Org 7797可发挥抗心律失常作用,这可能至少部分归因于钠通道阻滞。此外,我们的结果表明存在一种活性代谢物。在没有心电图或血流动力学变化的情况下观察到Org 7797的保护作用,这表明多次口服Org 7797不会损害正常心脏功能。

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