D-pipecolyl-leucyl-glycinamide, a substituted tripeptide analogue of the C-terminal part of oxytocin, influences tolerance to and dependence on ethanol in mice.

Alcohol and drug research Pub Date : 1987-01-01
G Szabó, G L Kovács, L Baláspiri, G Telegdy
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Abstract

The effects of graded doses of a substituted tripeptide analogue of the C-terminal part of oxytocin, D-Pip-Leu-GlyNH2 (DPLG), were investigated on the development of tolerance to the hypothermic effect of and dependence on alcohol in mice. Ethanol injection (4 g/kg i.p.) repeated on 3 consecutive days led to the development of tolerance in control and peptide-treated (0.005 microgram/mouse) animals. In the latter group, however, the level of tolerance was lower than in the control animals. The higher doses (0.05-5.0 micrograms/mouse) inhibited the development of tolerance. Repeated peptide administrations (5, 25, 125 micrograms/animal) did not affect the development of the dependence on alcohol which resulted from combined daily injections of tert-butanol (1.5 g/kg i.p.) and ethanol (3 g/kg i.p.). The severity of withdrawal was quantified via the convulsions induced with different doses of picrotoxin. When the peptide was injected only before the testing of withdrawal, DPLG markedly prolonged the onset of withdrawal signs.

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d -管酰-亮氨酸甘氨酸酰胺是一种取代的三肽类似物,与催产素c端部分相似,影响小鼠对乙醇的耐受性和依赖性。
本文研究了不同剂量的催产素c端取代三肽类似物D-Pip-Leu-GlyNH2 (DPLG)对小鼠低温酒精耐受和酒精依赖的影响。连续3天重复注射乙醇(4 g/kg / p)可使对照和肽处理(0.005微克/只)动物产生耐受性。然而,在后一组中,耐受水平低于对照动物。较高剂量(0.05 ~ 5.0微克/只)抑制耐受性的发展。重复给药(5、25、125微克/只动物)并不影响每日联合注射叔丁醇(1.5克/千克)和乙醇(3克/千克)导致的对酒精依赖的发展。通过不同剂量微毒素引起的惊厥来量化戒断的严重程度。当仅在戒断试验前注射肽时,DPLG显着延长了戒断症状的发作时间。
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Cyclo (Leu-Gly) attenuates the striatal dopaminergic supersensitivity induced by chronic morphine. Alcohol preference and regional brain monoamine contents of N/Nih heterogeneous stock rats. Toxicity of MDA (3,4-methylenedioxyamphetamine) considered for relevance to hazards of MDMA (Ecstasy) abuse. Alprazolam dependence in mice. Chronic cocaine administration induces opposite changes in dopamine receptors in the striatum and nucleus accumbens.
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