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长期给予乙醇会改变γ-氨基丁酸A受体基因的表达。

Chronic ethanol administration alters gamma-aminobutyric acidA receptor gene expression.

作者信息

Mhatre M C, Ticku M K

机构信息

Department of Pharmacology, University of Texas Health Science Center, San Antonio 78284-7764.

出版信息

Mol Pharmacol. 1992 Sep;42(3):415-22.

PMID:1383684
Abstract

Chronic ethanol (alcohol) administration has been associated with alterations in the binding and function of the gamma-aminobutyric acid (GABAA) receptor. To evaluate the mechanism underlying these changes, we measured the steady state levels of the mRNAs for the alpha 1, alpha 2, alpha 3, alpha 5, and alpha 6 subunits of the GABAA receptor after chronic ethanol administration to rats and ethanol withdrawal for 24 hr. The results indicated that chronic ethanol administration resulted in a 61% decline in the level of the GABAA receptor alpha 1 subunit mRNAs [3.8 and 4.3 kilobases (kb)] in the cerebral cortex in rats. The levels of the alpha 2 subunit mRNAs (6 and 3 kb) and the alpha 5 subunit mRNA (2.8 kb) were also reduced, by 61, 45, and 51%, respectively, whereas there was no change in the level of the alpha 3 subunit mRNA (3 kb). Furthermore, the ethanol-induced decrease in receptor mRNA levels persisted for 24 hr, after withdrawal of ethanol and returned to control values at 36 hr of withdrawal. alpha 1 mRNA levels in cerebellum also decreased by 28%. The level of the alpha 6 subunit mRNA, which selectively encodes Ro15-4513 binding sites, was found to be increased by approximately 76% in the cerebellum. Also, the photoaffinity labeling studies using [3H]Ro15-4513 indicated an increase in the levels of various protein components of the GABAA receptor, in the cerebellum and the cerebral cortex (e.g., 50- and 55-kDa proteins in the cerebellum and 41- and 50-kDa proteins in the cortex), after chronic ethanol treatment. The increase in alpha 6 mRNA in the cerebellum might be related to the increased labeling of the 55-kDa (approximately 56-kDa) protein and partially responsible for the increased binding, as reported previously by us. Because the alpha 6 subunit is not expressed in cortex, involvement of an as yet unknown subunit in this region cannot be ruled out. The effect of chronic ethanol treatment appears to be specific for GABAA receptor subunit mRNAs, because the same treatment did not alter the levels of glyceraldehyde-3-dehydrogenase mRNA or poly(A)+ RNA. In summary, these data indicate that chronic ethanol treatment results in an alteration in the regulation of expression of GABAA receptor subunit-encoding mRNAs, which could be due to alterations in transcription or mRNA stability.

摘要

长期给予乙醇(酒精)已被证明与γ-氨基丁酸(GABAA)受体的结合及功能改变有关。为了评估这些变化背后的机制,我们在对大鼠长期给予乙醇并戒断24小时后,测量了GABAA受体α1、α2、α3、α5和α6亚基mRNA的稳态水平。结果表明,长期给予乙醇导致大鼠大脑皮质中GABAA受体α1亚基mRNA水平(3.8和4.3千碱基(kb))下降了61%。α2亚基mRNA(6和3 kb)和α5亚基mRNA(2.8 kb)水平也分别降低了61%、45%和51%,而α3亚基mRNA(3 kb)水平没有变化。此外,乙醇诱导的受体mRNA水平下降在乙醇戒断后持续24小时,并在戒断36小时后恢复到对照值。小脑α1 mRNA水平也下降了28%。发现选择性编码Ro15 - 4513结合位点的α6亚基mRNA水平在小脑中增加了约76%。同样,使用[3H]Ro15 - 4513进行的光亲和标记研究表明,长期乙醇处理后,小脑和大脑皮质中GABAA受体的各种蛋白质成分水平增加(例如,小脑中50和55 kDa的蛋白质以及皮质中41和50 kDa的蛋白质)。如我们之前报道的,小脑中α6 mRNA的增加可能与55 kDa(约56 kDa)蛋白质标记增加有关,并部分导致结合增加。由于α6亚基在皮质中不表达,不能排除该区域中一个未知亚基的参与。长期乙醇处理的影响似乎对GABAA受体亚基mRNA具有特异性,因为相同处理并未改变甘油醛-3-脱氢酶mRNA或聚腺苷酸加尾RNA(poly(A)+ RNA)的水平。总之,这些数据表明长期乙醇处理导致GABAA受体亚基编码mRNA表达调控的改变,这可能是由于转录或mRNA稳定性的改变所致。

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