首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >The Effect of Chronic Ethanol Consumption and Withdrawal on mu-Opioid and Dopamine D_1 and D_2 Receptor Density in Fawn-Hooded Rat Brain
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The Effect of Chronic Ethanol Consumption and Withdrawal on mu-Opioid and Dopamine D_1 and D_2 Receptor Density in Fawn-Hooded Rat Brain

机译:长期摄入和戒除乙醇对小鹿山羊大脑中阿片类药物和多巴胺D_1和D_2受体密度的影响

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摘要

Previous studies have implicated the dopamine and opioid systems in the induction and maintenance of ethanol consumption. This study investigated, in alcohol-prefering Fawn-Hooded (FH) rats, whether chronic free-choice ethanol consumption and subsequent withdrawal cause alterations in central mu-opioid, dopamine D_1, and D_2 receptor density using autoradiography. Fh rats were given a free choice between a 5% ethanol solution and tap water (n = 25) and displayed a mean ethanol consumption of 5.6 g/kg/day. A parallel group of FH rats (n = 5) only had access to tap water. Rats were then withdrawn from ethanol for 0, 1, 2, 5, or 10 days and killed by cervical dislocation and decapitation. Increases in mu-opioid receptor density were observed in the nucleus accumbens and ventral tegmental area upon withdrawal compared with the ethanol naive group. In the lateral amygdala, binding in all withdrawal groups was significantly different from the ethanol naive FH rats, and also from the chronic ethanol rats. An increase in dopamine D_1 receptor density was observed in the substantia nigra, pars reticulata in the 5-and 10-day withdrawal groups compared with ethanol naive. Accumbal dopamine D_2 receptor density ( + 25-30%) increased in the 10-day withdrawal group compared with both naive and chronic ethanol groups. These findings demonstrate that the opioid and dopamine systems are susceptible to modulation by chronic ethanol consumption and withdrawal in the FH rat. Furthermore, although acute ethanol withdrawal results in modulation of mu-opioid receptors, effects on dopamine receptors are delayed and only become evident 5 to 10 days after withdrawal.
机译:先前的研究已经将多巴胺和阿片样物质系统牵涉到乙醇消耗的诱导和维持中。这项研究使用放射自显影技术在嗜酒精的小鹿(FH)大鼠中调查了长期自由选择乙醇的摄入和随后的戒断是否会引起中枢mu阿片类药物,多巴胺D_1和D_2受体密度的改变。 Fh大鼠可在5%乙醇溶液和自来水之间自由选择(n = 25),平均乙醇消耗量为5.6 g / kg /天。一组平行的FH大鼠(n = 5)仅能获得自来水。然后从乙醇中撤出大鼠0、1、2、5或10天,并通过颈椎脱位和断头处死。与无酒精乙醇组相比,停药后伏隔核和腹侧被盖区的阿片类药物受体密度增加。在外侧杏仁核中,所有戒断组的结合均与未使用过乙醇的FH大鼠以及慢性使用过的乙醇大鼠显着不同。与单纯乙醇相比,在戒断5天和10天的黑质,网状黑斑中观察到多巴胺D_1受体密度增加。与单纯和慢性乙醇组相比,停药10天组的累积多巴胺D_2受体密度(+ 25-30%)增加。这些发现表明,在FH大鼠中,阿片类药物和多巴胺系统易受慢性乙醇消耗和戒断的调节。此外,尽管急性乙醇戒断导致对阿片受体的调节,但对多巴胺受体的作用被延迟,仅在戒断后5至10天才显现出来。

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