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首页> 外文期刊>European Journal of Pharmacology: An International Journal >An orally active motilin receptor antagonist, MA-2029, inhibits motilin-induced gastrointestinal motility, increase in fundic tone, and diarrhea in conscious dogs without affecting gastric emptying.
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An orally active motilin receptor antagonist, MA-2029, inhibits motilin-induced gastrointestinal motility, increase in fundic tone, and diarrhea in conscious dogs without affecting gastric emptying.

机译:口服活性胃动素受体拮抗剂MA-2029在不影响胃排空的情况下,抑制胃动素诱导的肠胃蠕动,底语调增高和腹泻。

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摘要

The pharmacological properties of MA-2029, a selective and competitive motilin receptor antagonist, were investigated in conscious dogs after oral administration. Gastrointestinal contractile activity was recorded by chronically implanted force transducers. The proximal gastric volume was measured with a barostat under constant pressure. Gastric emptying was examined using the paracetamol absorption test. MA-2029 (0.3-10 mg/kg, p.o.) administered in the interdigestive state inhibited gastrointestinal contractions induced by motilin (3 microg/kg, i.v.) in a dose-dependent manner. MA-2029 (0.3-3 mg/kg, p.o.) also inhibited the occurrence of spontaneous phase III contractions, even though MA-2029 had no effect on basal gastrointestinal motility or basal gastric emptying even at 10 and 30 mg/kg p.o. The inhibitory effect of MA-2029 on motilin-induced gastrointestinal motility corresponded to its plasma concentration. Motilin (0.3 microg/kg/h, i.v. infusion) reduced the proximal gastric volume by about 50% of control during isobaric distension. This effect was also inhibited by MA-2029 (1-10 mg/kg, p.o.) in a dose-dependent manner. In the digestive state, injection of motilin (3 microg/kg, i.v.) induced diarrhea in 9 of 11 dogs. MA-2029 (1-30 mg/kg, p.o.) reduced the incidence of diarrhea induced by motilin in a dose-dependent manner. The results indicate that MA-2029 inhibits hypermotility induced by motilin in conscious dogs without having an effect on the basal gastrointestinal tone or gastric emptying rate. MA-2029 may be useful in treating gastrointestinal disorders in which the pathogenesis involves the elevation of circulating motilin.
机译:口服给药后,在有意识的狗中研究了选择性和竞争性胃动素受体拮抗剂MA-2029的药理特性。长期植入的力传感器记录了胃肠道的收缩活动。在恒压下用恒压器测量近端胃体积。使用对乙酰氨基酚吸收测试检查胃排空。以消化间状态给药的MA-2029(0.3-10mg / kg,p.o。)以剂量依赖的方式抑制了由胃动素(3μg/ kg,静脉内)引起的胃肠道收缩。 MA-2029(0.3-3 mg / kg,p.o.)也抑制了自发的III期收缩的发生,即使MA-2029即使在10和30 mg / kg p.o时对基础胃肠动力或基础胃排空也没有影响。 MA-2029对胃动素诱导的胃肠蠕动的抑制作用与其血浆浓度相对应。在等压膨胀期间,胃动素(0.3微克/千克/小时,静脉输注)使近端胃体积减少了对照的约50%。 MA-2029(1-10 mg / kg,p.o.)也以剂量依赖的方式抑制了这种作用。在消化状态下,胃动素注射(3微克/千克,静脉注射)在11只狗中的9只引起腹泻。 MA-2029(1-30 mg / kg,p.o.)以剂量依赖性方式降低了胃动素引起的腹泻的发生率。结果表明,MA-2029抑制了由动胃素引起的清醒犬的运动过度,而对基础胃肠道张力或胃排空率没有影响。 MA-2029可用于治疗胃肠道疾病,其中发病机理涉及循环胃动素的升高。

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