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神经节苷脂可减少乙醇依赖的发展,而不影响乙醇耐受性。

Gangliosides reduce the development of ethanol dependence without affecting ethanol tolerance.

作者信息

Snell L D, Szabó G, Tabakoff B, Hoffman P L

机构信息

Lohocl Research Corporation, Denver, Colorado, USA.

出版信息

J Pharmacol Exp Ther. 1996 Oct;279(1):128-36.

PMID:8858985
Abstract

Mice given an ethanol-containing liquid diet, as their sole source of nutrients and fluid, rapidly developed functional tolerance to and physical dependence on ethanol. The presence of physical dependence was demonstrated by measured signs of central nervous system hyperexcitability upon withdrawal of ethanol. The withdrawal hyperexcitability, which included tremors, handling-induced seizures and spontaneous clonic/tonic seizures, was more pronounced when mice consumed the ethanol-containing diet for 7 days, compared with 5 days. Daily treatment of the animals with either a ganglioside mixture (extracted bovine brain gangliosides, 250 or 500 mg/kg i.p.) or ganglioside GM1 (100 mg/kg i.p.) for the terminal two-thirds of the ethanol administration period resulted in a significant reduction in the ethanol withdrawal signs. On the other hand, tolerance to the hypnotic action of ethanol, tested 30 hr after withdrawal of ethanol, was unaffected by ganglioside treatment. Ganglioside GM1 given i.c.v. at a daily dose of 10 micrograms during the ethanol ingestion period was as effective as 100 mg/kg GM1 given i.p. in reducing signs of ethanol withdrawal. The daily administration of gangliosides during the feeding of the ethanol diet did not alter the animals' ethanol consumption, intoxication or blood ethanol levels at the time of ethanol withdrawal. A single dose of GM1 given either i.p. or i.c.v. 16 hr before withdrawal produced no effect on the measured ethanol withdrawal signs. Our prior work and the work of others has demonstrated a relationship between up-regulation of N-methyl-D-aspartate receptor numbers in brain and the manifestation of ethanol withdrawal signs. Daily administration of GM1, during the last 5 days of a 7-day period of ethanol ingestion, prevented the up-regulation of N-methyl-D-aspartate receptors in the hippocampus and reduced the ethanol withdrawal signs. Our data demonstrate that the daily administration of gangliosides during the period of ethanol consumption may prevent the development of ethanol physical dependence, while leaving ethanol tolerance intact.

摘要

给小鼠喂食含乙醇的液体饲料作为其唯一的营养和液体来源后,它们会迅速产生对乙醇的功能性耐受和身体依赖性。通过测量乙醇戒断时中枢神经系统过度兴奋的体征来证明身体依赖性的存在。与摄入含乙醇饲料5天相比,小鼠摄入含乙醇饲料7天时,戒断时的过度兴奋更为明显,包括震颤、处理诱发的癫痫发作和自发性阵挛/强直发作。在乙醇给药期的最后三分之二时间里,每天给动物腹腔注射神经节苷脂混合物(提取的牛脑苷脂,250或500毫克/千克)或神经节苷脂GM1(100毫克/千克),可显著减轻乙醇戒断症状。另一方面,在乙醇戒断30小时后测试的对乙醇催眠作用的耐受性不受神经节苷脂治疗的影响。在乙醇摄入期,每天脑室内注射剂量为10微克的神经节苷脂GM1,在减轻乙醇戒断症状方面与腹腔注射100毫克/千克GM1的效果相同。在喂食含乙醇饲料期间每天给予神经节苷脂,不会改变动物在乙醇戒断时的乙醇摄入量、中毒情况或血液乙醇水平。在戒断前16小时腹腔注射或脑室内注射单剂量的GM1,对测量的乙醇戒断症状没有影响。我们之前的工作以及其他人的工作表明,大脑中N-甲基-D-天冬氨酸受体数量的上调与乙醇戒断症状的表现之间存在关联。在7天乙醇摄入期的最后5天每天给予GM1,可防止海马体中N-甲基-D-天冬氨酸受体的上调,并减轻乙醇戒断症状。我们的数据表明,在乙醇摄入期间每天给予神经节苷脂可能会预防乙醇身体依赖性的发展,同时保持乙醇耐受性不变。

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