首页> 外文期刊>The Journal of Pharmacology and Experimental Therapeutics: Official Publication of the American Society for Pharmacology and Experimental Therapeutics >Daily Treatment with Diazepam Differentially Modifies Sensitivity to the Effects of #gamma#-Aminobutyric Acid_A Modulators on Schedule-Controlled Responding in Rhesus Monkeys
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Daily Treatment with Diazepam Differentially Modifies Sensitivity to the Effects of #gamma#-Aminobutyric Acid_A Modulators on Schedule-Controlled Responding in Rhesus Monkeys

机译:地西p的每日治疗差异性地改变了对#gamma#-氨基丁酸_A调节剂对恒河猴日程控制响应的影响的敏感性。

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摘要

The present study examined how daily treatment with the benzodiazepine (BZ) diazepam modifies the effects of positive modulators acting at different sites on the #gamma#-aminobutyric acid_A (GABA_A) receptor complex and negative modulators acting at BZ sites on the receptor complex. GABA_A modulators were administered alone or in combination with acute or chronic diazepam to rhesus moneys (n = 4) responding under a multiple fixed ratio (FR-FR) schedule of food presentation and stimulus-shock termination (SST). There was mutual antagonism between the rate-decreasing effects of diazepam (5.6 mg/kg, p.o.) and high efficacy BZ site negative modulators [ethyl #beta_carboline-3-carboxylate (#beta#-CCE), methyl #beta#-carboline-3-carboxylate (#beta#-CCM) and methyl-6,7-dimethoxyl-4-ethyl-#beta#-3-carboxylate (DMCM)]. Antagonism of #beta#-CCE, #beta#-CCM, and DMCM by diazepam daily. In contrast, daily diazepam treatment enhanced the rate-decreasing effects of Ro 15-4513 (ethyl 8-azido-6-dihydro-5-methyl-6-oxo-4H-imidazo[1,5-#alpha#]-[1,4]benzodiazepine-3-carboxylate) and flumazenil. Chronic diazepam elicited cross-tolerance to the BZ triazolam and not to the barbiturate pentobarbital or the neuroactive steroid pregnanolone. These results suggest that tolerance to the ratedecreasing effects of BZs is not accompanied by cross-tolerance to positive GABA_A modulators acting at other sites on the receptor complex. Moreover, changes in sensitivity to negative GABA_A modulators during chronic diazepam treatment appeared to be related to negative efficacy and not clearly related to the precipitation of withdrawal for all drugs. These results indicate that changes in sensitivity to the behavioral effects of drugs that act at different sites on the GABA_A receptor complex might be especially useful for identifying and characterizing the functional consequences of GABA_A receptor heterogeneity.
机译:本研究研究了苯二氮卓(BZ)地西epa的日常治疗如何改变作用于#γ#-氨基丁酸_A(GABA_A)受体复合物上不同位点的正调节剂和作用于受体复合物上BZ位点上的负调节剂的作用。 GABA_A调节剂可以单独给予,也可以与急性或慢性地西epa合用,对恒河猴金钱(n = 4)产生食物反应和刺激休克终止(SST)的多重固定比率(FR-FR)计划。地西epa的降速作用(5.6 mg / kg,口服)与高效BZ位负调节剂[乙基#beta_carboline-3-羧酸盐(#beta#-CCE),甲基#beta#-carboline- 3-羧酸盐(#beta#-CCM)和6,7-二甲氧基-4-乙基-#β#-3-羧酸甲酯(DMCM)]。地西epa每天对#beta#-CCE,#beta#-CCM和DMCM的拮抗作用。相反,每日地西di治疗可增强Ro 15-4513(乙基8-叠氮基-6-二氢-5-甲基-6-氧代-4H-咪唑并[1,5-#alpha#]-[1 ,4]苯并二氮杂-3-羧酸盐)和氟马西尼。慢性地西epa引起对BZ三唑仑的交叉耐受,而不是对巴比妥类戊巴比妥或神经活性类固醇孕烷醇酮交叉耐受。这些结果表明,对BZs的降速作用的耐受性不与对在受体复合物其他位点起作用的正GABA_A调节剂的交叉耐受性相伴。此外,在慢性地西epa治疗期间,对阴性GABA_A调节剂的敏感性变化似乎与阴性疗效有关,而与所有药物的停药沉淀没有明显关系。这些结果表明,对作用于GABA_A受体复合物不同位点的药物的行为影响的敏感性变化,对于鉴定和表征GABA_A受体异质性的功能后果可能特别有用。

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