Effects of cisapride on gastrointestinal motor activity and gastric emptying of disopyramide.

T Kuroda, Y Yoshihara, H Nakamura, T Azumi, T Inatome, H Fukuzaki, H Takanashi, K Yogo, M Akima
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引用次数: 6

Abstract

The effects of cisapride on the gastrointestinal contractile activity and pharmacokinetics of disopyramide were determined in beagle dogs and patients with arrhythmia. In the animal experiments, the gastric motor index was significantly decreased by i.v. administration of disopyramide in a dose-dependent fashion. The peak decrease of the motor index was observed within 5 min after i.v. injection of disopyramide; the motor index then recovered gradually to the level present prior to drug administration. I.v. administration of cisapride (0.5 mg/kg) markedly increased gastrointestinal contractile activity following the decrease induced by disopyramide pretreatment (5 mg/kg, i.v.). In the clinical studies, the gastric emptying test was performed using the acetaminophen method. A significant correlation between plasma concentrations of disopyramide and gastric emptying time has been found (p < 0.001). The combination of disopyramide (100 mg t.i.d.) and cisapride (2.5 mg t.i.d.) significantly increased gastric emptying compared with that induced by disopyramide alone. The peak plasma concentration of disopyramide in association with cisapride oral administration was significantly higher, and the apparent absorption rate constant and lag time of disopyramide were about 2-fold higher and 2-fold shorter, respectively, than for disopyramide alone. Cisapride, acting as a cholinergic agonist, may counteract the anticholinergic effect of disopyramide on gastric motility. As a factor influencing drug absorption, gastric emptying is of importance, as it determines the rate of drug delivery to the small intestine. Therefore, the oral administration of disopyramide with cisapride may be useful for patients with delayed gastric emptying.

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西沙必利对胃肠运动活动和胃排空的影响。
研究了西沙必利对beagle犬和心律失常患者胃肠道收缩活性和药代动力学的影响。在动物实验中,胃运动指数明显降低静脉给药双双酰胺呈剂量依赖性。静脉注射双酰胺后5 min内运动指数下降幅度最大;运动指数逐渐恢复到服药前的水平。西沙必利(0.5 mg/kg)静脉注射后,胃肠道收缩活性明显增加,而非双嘧菌胺预处理(5mg /kg,静脉注射)。在临床研究中,胃排空试验采用对乙酰氨基酚法。血浆双酰胺浓度与胃排空时间有显著相关性(p < 0.001)。与单用双双酰胺相比,双双酰胺(100mg t.i.d)和西沙必利(2.5 mg t.i.d)联合用药显著增加胃排空。口服西沙必利联合用药时,血药浓度峰值明显升高,其表观吸收速率常数和滞后时间分别比单独用药高约2倍和短约2倍。西沙必利作为一种胆碱能激动剂,可以抵消二酰胺对胃运动的抗胆碱能作用。胃排空是影响药物吸收的一个重要因素,因为它决定了药物进入小肠的速度。因此,对于胃排空延迟的患者,口服西沙必利和双双酰胺可能是有用的。
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