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具有精神活性的大麻素会降低啮齿动物的胃肠推进和蠕动。

Psychoactive cannabinoids reduce gastrointestinal propulsion and motility in rodents.

作者信息

Shook J E, Burks T F

机构信息

Department of Pharmacology, University of Arizona, Tucson.

出版信息

J Pharmacol Exp Ther. 1989 May;249(2):444-9.

PMID:2542532
Abstract

Marijuana has been reported to be an effective antinauseant and antiemetic in patients receiving cancer chemotherapy. Whether this is due to psychological changes, central antiemetic properties and/or direct effects on gastrointestinal (GI) function is not known. The purpose of these investigations was to determine whether the major constituents of marijuana and the synthetic cannabinoid nabilone have any effects on GI function which can be detected in rodent models of GI transit and motility. Intravenous delta 9-tetrahydrocannabinol (delta 9-THC) slowed the rate of gastric emptying and small intestinal transit in mice and in rats. Delta 9,11-THC, cannabinol and nabilone given i.v. also inhibited small intestinal transit in mice, but were less effective in reducing gastric emptying. Cannabidiol given i.v. had no effect on gastric emptying or intestinal transit. Those cannabinoids which inhibited GI transit did so at doses equal to, or lower, than those reported to produce central nervous system activity. In rats, delta 9-THC produced greater inhibition of gastric emptying and small intestinal transit than large bowel transit, indicating a selectivity for the more proximal sections of the gut. In addition, i.v. delta 9-THC decreased the frequency of both gastric and intestinal contractions without altering intraluminal pressure. Such changes probably reflect a decrease in propulsive activity, without change in basal tone. These data indicate that delta 9-THC, delta 9,11-THC, cannabinol and nabilone (but not cannabidiol) exert an inhibitory effect on GI transit and motility in rats.

摘要

据报道,大麻对接受癌症化疗的患者是一种有效的抗恶心和止吐药。这是否归因于心理变化、中枢性止吐特性和/或对胃肠(GI)功能的直接影响尚不清楚。这些研究的目的是确定大麻的主要成分和合成大麻素纳布隆是否对GI功能有任何影响,这可以在GI转运和运动的啮齿动物模型中检测到。静脉注射δ9-四氢大麻酚(δ9-THC)可减缓小鼠和大鼠的胃排空率和小肠转运。静脉注射δ9,11-THC、大麻酚和纳布隆也可抑制小鼠的小肠转运,但在减少胃排空方面效果较差。静脉注射大麻二酚对胃排空或肠道转运没有影响。那些抑制GI转运的大麻素在等于或低于据报道产生中枢神经系统活性的剂量时就会产生这种作用。在大鼠中,δ9-THC对胃排空和小肠转运的抑制作用大于大肠转运,表明对肠道近端部分具有选择性。此外,静脉注射δ9-THC可降低胃和肠收缩的频率,而不改变腔内压力。这种变化可能反映了推进活动的减少,而基础张力没有改变。这些数据表明,δ9-THC、δ9,11-THC、大麻酚和纳布隆(但不包括大麻二酚)对大鼠的GI转运和运动具有抑制作用。

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