Corda M G, Sanna E, Concas A, Giorgi O, Ongini E, Nurchi V, Pintori T, Crisponi G, Biggio G
J Neurochem. 1986 Aug;47(2):370-4. doi: 10.1111/j.1471-4159.1986.tb04511.x.
We evaluated the effect of the two N-trifluoroethyl benzodiazepines, quazepam and its 2-oxo metabolite SCH 15725, which possess preferential affinity for type I benzodiazepine recognition sites, on the binding of [3H] gamma-aminobutyric acid ([3H]GABA) to rat brain membrane preparations. The study also included compounds such as diazepam and N-desalkyl-2-oxoquazepam (SCH 17514), which have equal affinity for the type I and type II receptor subtypes. Binding of [3H]GABA was studied in frozen-thawed and repeatedly washed cortical membranes incubated in 20 mM KH2PO4 plus 50 mM KCl, pH 7.4, at 4 degrees C in the absence and presence of quazepam or its metabolites. Addition of 10(-6) M quazepam increased by 30% specific [3H]GABA binding; as revealed by Scatchard plot analysis, the effect was due to an increase in the total number of GABA receptors. The effect of quazepam was concentration dependent, and it was shared by its active metabolite SCH 15725. The potency of quazepam and SCH 15725 in enhancing [3H]GABA binding was similar to that of diazepam, whereas CL 218872 and SCH 17514 were less active. Moreover, the [3H]GABA binding-enhancing effect of quazepam was mediated by an occupancy of benzodiazepine receptors, because it was specifically antagonized by 5 X 10(-6) M Ro15-1788.
我们评估了两种N-三氟乙基苯二氮䓬类药物夸西泮及其2-氧代代谢物SCH 15725对[3H]γ-氨基丁酸([3H]GABA)与大鼠脑膜制剂结合的影响,这两种药物对I型苯二氮䓬识别位点具有优先亲和力。该研究还包括地西泮和N-去烷基-2-氧代夸西泮(SCH 17514)等化合物,它们对I型和II型受体亚型具有同等亲和力。在4℃下,于20 mM KH2PO4加50 mM KCl、pH 7.4的条件下,在有无夸西泮或其代谢物存在的情况下,对冻融并反复洗涤的皮质膜中[3H]GABA的结合进行了研究。加入10(-6) M夸西泮可使特异性[3H]GABA结合增加30%;通过Scatchard图分析表明,这种作用是由于GABA受体总数增加所致。夸西泮的作用呈浓度依赖性,其活性代谢物SCH 15725也有此作用。夸西泮和SCH 15725增强[3H]GABA结合的效力与地西泮相似,而CL 218872和SCH 17514的活性较低。此外,夸西泮增强[3H]GABA结合的作用是由苯二氮䓬受体的占据介导的,因为它被5×10(-6) M Ro15-1788特异性拮抗。
