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新型十氢喹啉衍生物的抗心律失常特性及内皮作用

Antiarrhythmic profile and endothelial action of novel decahydroquinoline derivatives.

作者信息

Kozlovski Valery I, Vdovichenko Vladimir P, Chlopicki Stefan, Malchik Sergey S, Praliyev Kaldybek D, Zcilkibayev Oral T

机构信息

Department of Experimental Pharmacology, Jagiellonian University Medical College, Grzegórzecka 16, PL 31-531 Kraków, Poland.

出版信息

Pol J Pharmacol. 2004 Nov-Dec;56(6):767-74.

Abstract

We tested antiarrhythmic and endothelial action of novel decahydroquinoline derivatives. Antiarrhythmic activity was analyzed using models of aconitine-, calcium chloride-, and adrenaline-induced arrhythmias in rats. Potency to induce nitric oxide (NO)-dependent coronary vasodilation was assessed in isolated guinea pig heart perfused according to Langendorff technique. Among 15 novel decahydroquinoline derivatives (D1-15), four of them displayed antiarrhythmic activity (D12-D15). D12-D15 compounds were more active in the model of aconitine-induced arrhythmias than in calcium chloride-induced arrhythmias and were inactive in the model of adrenaline-induced arrhythmias. Profile of antiarrhythmic activity of D12-D15 compounds was similar to that of quinidine and procainamide. Interestingly, in the isolated guinea pig heart D14 and D15 (10(-5) M) induced coronary vasodilation, that was mediated by endothelium-derived NO. In conclusion, novel decahydroquinoline derivatives described here (D12-D15) show antiarrhythmic activity typical of antiarrhythmic drugs of class I. Importantly, some of these compounds (D14, D15) release NO from coronary endothelium, which may provide an additional therapeutic benefit.

摘要

我们测试了新型十氢喹啉衍生物的抗心律失常和内皮作用。使用乌头碱、氯化钙和肾上腺素诱导大鼠心律失常的模型分析抗心律失常活性。根据Langendorff技术,在离体豚鼠心脏中评估诱导一氧化氮(NO)依赖性冠状动脉舒张的能力。在15种新型十氢喹啉衍生物(D1 - 15)中,其中四种具有抗心律失常活性(D12 - D15)。D12 - D15化合物在乌头碱诱导的心律失常模型中比在氯化钙诱导的心律失常模型中更具活性,而在肾上腺素诱导的心律失常模型中无活性。D12 - D15化合物的抗心律失常活性谱与奎尼丁和普鲁卡因胺相似。有趣的是,在离体豚鼠心脏中,D14和D15(10^(-5) M)诱导冠状动脉舒张,这是由内皮衍生的NO介导的。总之,本文所述的新型十氢喹啉衍生物(D12 - D15)显示出I类抗心律失常药物典型的抗心律失常活性。重要的是,其中一些化合物(D14、D15)可从冠状动脉内皮释放NO,这可能提供额外的治疗益处。

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