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甲苯磺酸溴苄铵对奎尼丁诱导长QT间期犬心脏不应期不均一性和室颤阈值的影响。

Effects of bretylium tosylate on inhomogeneity of refractoriness and ventricular fibrillation threshold in canine hearts with quinidine-induced long QT interval.

作者信息

Inoue H, Toda I, Nozaki A, Matsuo H, Sugimoto T

出版信息

Cardiovasc Res. 1985 Oct;19(10):655-60. doi: 10.1093/cvr/19.10.655.

Abstract

We studied effects of bretylium tosylate (6 mg X kg-1, injected intravenously over 60s) on ventricular refractoriness and its inhomogeneity, and ventricular fibrillation threshold (VFT) in canine hearts with quinidine-induced long QT interval. In 3 anaesthetised open chest dogs, 30 mg X kg-1 of quinidine sulphate was injected intravenously over 5 min to produce QT prolongation. Effective refractory period (ERP) was determined at 8 test points of the right ventricle using extrastimuli. Temporal dispersion as an expression of inhomogeneity of ventricular refractoriness was estimated as the difference between the longest and the shortest ERP. VFT was determined using a train of pulses, 4 ms in duration and at 10 ms intervals. Effects of bretylium were determined from 30 to 60 min after injection. Quinidine-induced long QT interval did not change after bretylium (358 +/- 37 vs 348 +/- 26 ms) when transiently elevated blood pressure returned to the pre-bretylium level. Bretylium shortened ERP slightly (278 +/- 16 vs 268 +/- 14 ms, p less than 0.02) but did not shorten ERP after premature depolarisation (209 +/- 14 vs 209 +/- 15). However, temporal dispersion was significantly decreased by bretylium. VFT, which was lowered by quinidine (14.5 +/- 5.0 vs 8.5 +/- 2.9 mA, p less than 0.01), was elevated significantly by bretylium (21.9 +/- 6.9, p less than 0.001). These effects of bretylium might be attributed to the combination of its direct electrophysiology and indirect adrenergic actions.

摘要

我们研究了甲苯磺酸溴苄铵(6毫克/千克,静脉注射60秒)对奎尼丁诱导长QT间期犬心脏心室不应期及其不均一性以及心室颤动阈值(VFT)的影响。在3只麻醉开胸犬中,静脉注射30毫克/千克硫酸奎尼丁5分钟以延长QT间期。使用额外刺激在右心室的8个测试点测定有效不应期(ERP)。作为心室不应期不均一性表现的时间离散度通过最长和最短ERP之间的差值来估算。使用持续时间为4毫秒、间隔为10毫秒的脉冲序列测定VFT。在注射后30至60分钟确定溴苄铵的作用。当短暂升高的血压恢复到注射溴苄铵前的水平时,溴苄铵作用后奎尼丁诱导的长QT间期未改变(358±37对348±26毫秒)。溴苄铵略微缩短ERP(278±16对268±14毫秒,p<0.02),但在过早去极化后未缩短ERP(209±14对209±15)。然而,溴苄铵显著降低了时间离散度。被奎尼丁降低的VFT(14.5±5.0对8.5±2.9毫安,p<0.01)被溴苄铵显著升高(21.9±6.9,p<0.001)。溴苄铵的这些作用可能归因于其直接电生理作用和间接肾上腺素能作用的联合。

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