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小鼠对苯二氮䓬受体配体低温效应敏感性的品系差异。

Strain differences in sensitivity to the hypothermic effects of benzodiazepine receptor ligands in mice.

作者信息

Jackson H C, Nutt D J

机构信息

Reckitt & Colman Psychopharmacology Unit, Department of Pharmacology, School of Medical Sciences, Bristol, UK.

出版信息

Psychopharmacology (Berl). 1992;109(3):365-8. doi: 10.1007/BF02245884.

Abstract

The hypothermic effects of intraperitoneal (IP) administration of the full benzodiazepine agonist loprazolam (1, 10 mg/kg); the partial agonist Ro 17-1812 (1, 10 mg/kg); the benzodiazepine receptor antagonist flumazenil (10, 20 mg/kg); the benzodiazepine inverse agonists Ro 15-4513 (1, 3, 10 mg/kg) and Ro 19-4603 (0.03, 0.1, 0.3 mg/kg) and the beta-carboline inverse agonists FG 7142 (10, 30 mg/kg) and DMCM (1, 3, 10 mg/kg) were investigated in three strains of mice. TO mice were less sensitive than CBA/cA and DBA/2 mice, since only loprazolam and the partial and full beta-carboline inverse agonists FG 7142 and DMCM lowered body temperature in these animals. CBA/cA mice were particularly sensitive to the hypothermic effects of loprazolam and Ro 17-1812, and also responded to the beta-carboline but not the benzo diazepine inverse agonists. In contrast, DBA/2 mice responded with moderate hypothermia to loprazolam, Ro 17-1812, and to the partial inverse agonist Ro 15-4513, and exhibited marked hypothermia in response to the more efficacious benzodiazepine inverse agonist Ro 19-4603 and to FG 7142 and DMCM. Flumazenil did not alter body temperature. DBA/2 mice were also more sensitive to the convulsant activity of inverse agonists than TO mice. CBA/cA mice exhibited enhanced sensitivity to the convulsant, but not the hypothermic, effects of Ro 19-4603, showing dissociation of these responses. The mechanisms underlying the genetic differences in sensitivity of mice to the hypothermic and convulsant action of the different ligands are unknown and warrant further investigation.

摘要

研究了腹腔注射全效苯二氮䓬激动剂氯普唑仑(1、10mg/kg)、部分激动剂Ro 17 - 1812(1、10mg/kg)、苯二氮䓬受体拮抗剂氟马西尼(10、20mg/kg)、苯二氮䓬反向激动剂Ro 15 - 4513(1、3、10mg/kg)和Ro 19 - 4603(0.03、0.1、0.3mg/kg)以及β-咔啉反向激动剂FG 7142(10、30mg/kg)和DMCM(1、3、10mg/kg)对三种品系小鼠的体温降低作用。TO小鼠比CBA/cA和DBA/2小鼠敏感性低,因为只有氯普唑仑以及部分和全效β-咔啉反向激动剂FG 7142和DMCM能降低这些动物的体温。CBA/cA小鼠对氯普唑仑和Ro 17 - 1812的体温降低作用特别敏感,并且对β-咔啉有反应,但对苯二氮䓬反向激动剂无反应。相比之下,DBA/2小鼠对氯普唑仑、Ro 17 - 1812和部分反向激动剂Ro 15 - 4513表现出中度体温降低,对更有效的苯二氮䓬反向激动剂Ro 19 - 4603以及FG 7142和DMCM表现出明显的体温降低。氟马西尼不改变体温。DBA/2小鼠对反向激动剂的惊厥活性也比TO小鼠更敏感。CBA/cA小鼠对Ro 19 - 4603的惊厥作用而非体温降低作用表现出增强的敏感性,显示出这些反应的解离。小鼠对不同配体的体温降低和惊厥作用敏感性的遗传差异背后的机制尚不清楚,值得进一步研究。

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