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新型钙拮抗剂莫那普利对心脏传导系统的体外和体内心电图评估

In vitro and in vivo electrocardiographic evaluation of the novel calcium antagonist monatepil on cardiac conduction system.

作者信息

Nose I, Kataoka T, Honda Y, Yamada T, Ikeno A, Fukuya F, Minato H, Takeyama K, Hosoki K, Karasawa T

机构信息

Department of Pharmacology, Dainippon Pharmaceutical Co., Ltd., Suita, Osaka, Japan.

出版信息

Arzneimittelforschung. 1993 Jul;43(7):722-8.

PMID:8369002
Abstract

Effects of monatepil ([(+/-)-N-(6,11-dihydrodibenzo[b, e]thiepin-11-yl)-4-(p-fluorophenyl)-1-piperazinebutyramide]m aleate, AJ-2615, CAS 103377-41-9), a novel calcium antagonist, on the cardiac conduction system were compared by electrocardiography with those of the existing calcium antagonists (diltiazem, verapamil and nifedipine) in isolated rabbit heart preparations in vitro and in anesthetized and conscious dogs in vivo. Monatepil (10(-7) mol/l) prolonged the atrio-His bundle conduction time (AH interval) in the Langendorff perfused rabbit heart, like diltiazem, verapamil and nifedipine. This prolongation was decreased to 1/10 in the presence of 3.6% bovine serum albumin. In anesthetized dogs, monatepil (0.1-1.0 mg/kg i.v.), unlike diltiazem and verapamil, did not prolong AH interval. In conscious dogs, monatepil even at 100 mg/kg p.o. did not affect electrocardiograms. At the high dose of 300 mg/kg p.o., only a slight prolongation of the QT interval was found, but the QTc interval was not affected. Diltiazem at 10 mg/kg p.o. caused a prolongation of the PR interval and a disappearance of QRS waves. In conscious renal hypertensive dogs, repeated administration of monatepil (10 mg/kg/d p.o. for 29 days) had little effect on the conduction system of the heart examined by electrocardiograms, albeit a persistent fall in blood pressure continued throughout the administration period. The above results suggest that monatepil is a highly safe drug in the treatment of hypertension.

摘要

通过心电图,在体外分离的兔心标本以及体内麻醉和清醒犬中,比较了新型钙拮抗剂莫那地尔(马来酸[(±)-N-(6,11-二氢二苯并[b,e]硫氮杂卓-11-基)-4-(对氟苯基)-1-哌嗪丁酰胺],AJ-2615,CAS 103377-41-9)与现有钙拮抗剂(地尔硫卓、维拉帕米和硝苯地平)对心脏传导系统的影响。莫那地尔(10⁻⁷mol/L)可延长Langendorff灌注兔心的房室束传导时间(AH间期),地尔硫卓、维拉帕米和硝苯地平也有同样作用。在存在3.6%牛血清白蛋白的情况下,这种延长作用降低至十分之一。在麻醉犬中,与地尔硫卓和维拉帕米不同,莫那地尔(0.1 - 1.0mg/kg静脉注射)不会延长AH间期。在清醒犬中,即使口服莫那地尔100mg/kg也不会影响心电图。口服高剂量300mg/kg时,仅发现QT间期略有延长,但QTc间期未受影响。口服10mg/kg地尔硫卓会导致PR间期延长和QRS波消失。在清醒肾性高血压犬中,重复给予莫那地尔(10mg/kg/d口服,共29天)对通过心电图检查的心脏传导系统影响很小,尽管在给药期间血压持续下降。上述结果表明,莫那地尔在治疗高血压方面是一种高度安全的药物。

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