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丙泊酚、戊巴比妥和α-香豆素对大鼠大脑皮质中t-[35S]丁基双环磷硫代酸盐结合的影响。

Effects of propofol, pentobarbital and alphaxalone on t-[35S]butylbicyclophosphorothionate binding in rat cerebral cortex.

作者信息

Concas A, Santoro G, Mascia M P, Maciocco E, Dazzi L, Biggio G

机构信息

Department of Experimental Biology, University of Cagliari, Italy.

出版信息

Eur J Pharmacol. 1994 Apr 15;267(2):207-13. doi: 10.1016/0922-4106(94)90172-4.

Abstract

The effects of propofol, pentobarbital, alphaxalone, etomidate and diazepam on t-[35S]butylbicyclophosphorothionate ([35S]TBPS) binding to membrane preparations from rat cerebral cortex were studied in the absence of gamma-aminobutyric acid (GABA). Addition of low concentrations (3-10 microM) of propofol to washed membrane preparations (devoid of GABA) markedly enhanced [35S]TBPS binding (maximal enhancement, 85%), whereas higher concentrations (50-100 microM) inhibited this parameter. Diazepam also enhanced [35S]TBPS binding in this preparation (maximal enhancement, 38%). In contrast, pentobarbital, alphaxalone and etomidate decreased [35S]TBPS binding in a concentration-dependent manner. The propofol-induced increase in [35S]TBPS binding in washed membranes was completely reversed by the addition of GABA at a concentration (0.3 microM) that alone did not modify [35S]TBPS binding (78% increase with 10 microM propofol alone, 33% decrease in the additional presence of GABA). The ability of GABA to reverse the effect of propofol on [35S]TBPS binding in washed membranes was shared by pentobarbital (200 microM) and alphaxalone (3 microM); etomidate (20 microM) only partially antagonized the effect of propofol. Diazepam at a concentration (30 microM) that alone had no effect on [35S]TBPS binding failed to modify the propofol-induced increase in [35S]TBPS binding, whereas at a concentration (3 microM) that alone increased [35S]TBPS binding the effect of diazepam was additive with that of propofol. The addition of bicuculline to washed membranes failed to abolish the increase in [35S]TBPS binding induced by propofol or diazepam, but completely antagonized the effects of pentobarbital, alphaxalone and etomidate.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

在不存在γ-氨基丁酸(GABA)的情况下,研究了丙泊酚、戊巴比妥、α-香豆素、依托咪酯和地西泮对大鼠大脑皮质膜制剂上t-[35S]丁基双环磷硫代酸盐([35S]TBPS)结合的影响。向洗涤过的膜制剂(不含GABA)中添加低浓度(3 - 10 microM)的丙泊酚可显著增强[35S]TBPS结合(最大增强85%),而较高浓度(50 - 100 microM)则抑制该参数。地西泮也可增强该制剂中的[35S]TBPS结合(最大增强38%)。相反,戊巴比妥、α-香豆素和依托咪酯以浓度依赖的方式降低[35S]TBPS结合。在洗涤过的膜中,添加浓度为0.3 microM的GABA可完全逆转丙泊酚诱导的[35S]TBPS结合增加,该浓度的GABA单独作用时不改变[35S]TBPS结合(单独使用10 microM丙泊酚时增加78%,同时存在GABA时减少33%)。戊巴比妥(200 microM)和α-香豆素(3 microM)与GABA一样,能够逆转丙泊酚对洗涤过的膜中[35S]TBPS结合的作用;依托咪酯(20 microM)仅部分拮抗丙泊酚的作用。浓度为30 microM的地西泮单独对[35S]TBPS结合无影响,不能改变丙泊酚诱导的[35S]TBPS结合增加,而浓度为3 microM的地西泮单独可增加[35S]TBPS结合,其作用与丙泊酚相加。向洗涤过的膜中添加荷包牡丹碱不能消除丙泊酚或地西泮诱导的[35S]TBPS结合增加,但可完全拮抗戊巴比妥、α-香豆素和依托咪酯的作用。(摘要截短于250字)

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