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曲美布汀和κ阿片类物质对犬声应激诱导的胃运动抑制的外周拮抗作用。

Peripheral antagonistic action of trimebutine and kappa opioid substances on acoustic stress-induced gastric motor inhibition in dogs.

作者信息

Gué M, Pascaud X, Hondé C, Junien J L, Buéno L

机构信息

Department of Pharmacology INRA, Fresnes, France.

出版信息

Eur J Pharmacol. 1988 Jan 27;146(1):57-63. doi: 10.1016/0014-2999(88)90486-4.

Abstract

The effects of intracerebroventricular (i.c.v.), intravenous (i.v.) and oral (p.o.) administration of trimebutine on the gastric motor inhibition induced by acoustic stress were investigated in fasted dogs fitted with strain-gauge transducers on the antrum and proximal jejunum. Started 40-50 min after the last migrating motor complex, a 1 h acoustic stress delayed by 111% the occurrence of the next gastric migrating motor complex without affecting the jejunal motor pattern. This inhibition of gastric migrating motor complex induced by acoustic stress was abolished by previous p.o. administration of trimebutine (1 mg/kg) but not by its i.v. (0.1 mg/kg) or i.c.v. (0.01 mg/kg) injection. The trimebutine blockade of gastric motor alterations induced by acoustic stress was suppressed after previous i.v. treatment with MR 2266 (0.3 mg/kg) but was unaffected by naloxone (0.3 mg/kg). Furthermore oral administration of U-50488H (10 micrograms/kg) and ethylketocyclazocine (10 micrograms/kg) respectively abolished and reduced the acoustic stress-induced delay of the occurrence of the gastric migrating motor complex. We concluded that trimebutine is able to antagonize the gastric motor disturbances induced in dogs by acoustic stress, probably by acting selectively on peripheral kappa receptors located in the wall of the proximal gut and directly stimulated from a mucosal site.

摘要

在禁食的犬身上,在胃窦和空肠近端安装应变片传感器,研究了脑室内(i.c.v.)、静脉内(i.v.)和口服(p.o.)给予曲美布汀对声应激诱导的胃运动抑制的影响。在最后一次移行性运动复合波后40 - 50分钟开始,1小时的声应激使下一次胃移行性运动复合波的出现延迟了111%,而不影响空肠运动模式。这种由声应激诱导的胃移行性运动复合波的抑制,在先前口服曲美布汀(1mg/kg)后被消除,但静脉注射(0.1mg/kg)或脑室内注射(0.01mg/kg)则无此作用。在用MR 2266(0.3mg/kg)进行静脉预处理后,曲美布汀对声应激诱导的胃运动改变的阻断作用被抑制,但不受纳洛酮(0.3mg/kg)影响。此外,分别口服U - 50488H(10μg/kg)和乙基酮环唑辛(10μg/kg)可消除和减少声应激诱导的胃移行性运动复合波出现的延迟。我们得出结论,曲美布汀能够拮抗犬因声应激诱导的胃运动紊乱,可能是通过选择性作用于位于近端肠道壁的外周κ受体,并从黏膜部位直接刺激这些受体来实现的。

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