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首页> 外文期刊>Brain research bulletin >Gastric antisecretory effects of synthetic cannabinoids after central or peripheral administration in the rat.
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Gastric antisecretory effects of synthetic cannabinoids after central or peripheral administration in the rat.

机译:在大鼠中枢或外周给药后,合成大麻素的胃分泌抑制作用。

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Previous studies have revealed that cannabinoid (CB)-receptor agonists inhibit gastric acid secretion stimulated by indirectly acting agents, but not by histamine. Aiming to investigate whether central or peripheral mechanisms are involved, the effects of the synthetic CB-receptor agonists WIN55,212-2 and HU-210, administered either intracerebroventricularly (i.c.v.) or intravenously (i.v.) to the anaesthetized rat with lumen-perfused stomach, against gastric acid secretion induced by pentagastrin were tested. Injected i.c.v., both WIN55,212-2 (50 and 100mug/kg) and HU-210 (25, 50 and 100mug/kg) were ineffective on either basal secretion or acid output induced by pentagastrin (7.7mug/kg, i.v.). By contrast, i.v. injections of WIN55,212-2 (100 and 1000mug/kg) or HU-210 (10-100mug/kg) significantly inhibited pentagastrin-induced acid secretion, maximal reductions being 75.70 and 82.24% for WIN55,212-2 and HU-210, respectively. The gastric antisecretory effect of HU-210 was prevented by administration of the selective CB(1)-receptor antagonist SR141716A (1000mug/kg, i.v.). These results show that CB(1)-receptors mediating inhibition of gastric acid secretion in the rat are mainly peripherally located.
机译:先前的研究表明,大麻素(CB)受体激动剂可抑制间接作用剂而非组胺刺激的胃酸分泌。为了研究是否涉及中枢或外周机制,对经腔内灌注胃麻醉的脑室内(icv)或静脉内(iv)给予合成的CB受体激动剂WIN55,212-2和HU-210的作用,针对五肽胃泌素诱导的胃酸分泌进行了测试。经静脉注射,WIN55,212-2(50和100mug / kg)和HU-210(25、50和100mug / kg)都对五肽胃泌素诱导的基础分泌或酸输出(7.7mug / kg,静脉内)无效。相比之下,i.v。注射WIN55,212-2(100和1000mug / kg)或HU-210(10-100mug / kg)可以显着抑制五肽胃泌素诱导的酸分泌,WIN55,212-2和HU-210的最大减少量分别为75.70和82.24% , 分别。通过施用选择性CB(1)-受体拮抗剂SR141716A(1000mug / kg,i.v.)可预防HU-210的胃分泌抑制作用。这些结果表明介导抑制大鼠胃酸分泌的CB(1)受体主要位于外围。

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