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短期选择性培育急性乙醇戒断后出现的药物戒断惊厥及对惊厥剂的易感性。

Drug withdrawal convulsions and susceptibility to convulsants after short-term selective breeding for acute ethanol withdrawal.

作者信息

Metten P, Belknap J K, Crabbe J C

机构信息

Portland Alcohol Research Center, Department of Behavioral Neuroscience, Oregon Health Sciences University and Department of Veteran's Affairs Medical Center, Portland 97201, USA.

出版信息

Behav Brain Res. 1998 Sep;95(1):113-22. doi: 10.1016/s0166-4328(97)00216-7.

Abstract

High Alcohol Withdrawal (HAW) and Low Alcohol Withdrawal (LAW) mice were selectively bred from a foundation population of C57BL6/J (B6) x DBA/2J (D2) F2 intercross progeny for display of intense or mild handling-induced withdrawal convulsions, respectively, following a single injection of a hypnotic dose of ethanol (alcohol; 4 g/kg). The HAW line had significantly greater alcohol withdrawal severity scores compared to the LAW line after only a single generation of selection; the magnitude of the line difference was 8-fold by the fourth selected generation. We tested these lines for severity of withdrawal convulsions following the benzodiazepine, diazepam; the gaseous anesthetic, nitrous oxide; the imidazopyridine, zolpidem and the barbiturate, pentobarbital. In all cases, HAW mice had significantly greater withdrawal severity than mice of the LAW line. These results indicate that some genes influencing withdrawal convulsion severity following ethanol also affect withdrawal from other CNS depressants. D2 mice are more sensitive to a variety of convulsants than B6 mice (and have more severe withdrawal convulsions). We, therefore, tested separate groups of mice of both selectively bred lines for threshold sensitivity to pentylenetetrazol (PTZ), N-methyl-D-aspartate (NMDA) and kainic acid (KA). No line differences were detected. These results indicate that genes influencing severity of withdrawal from several depressant drugs are largely different from those affecting susceptibility to GABAergic or glutamatergic convulsants.

摘要

高酒精戒断(HAW)小鼠和低酒精戒断(LAW)小鼠是从C57BL6/J(B6)×DBA/2J(D2)F2杂交后代的基础种群中选择性培育出来的,分别用于在单次注射催眠剂量的乙醇(酒精;4克/千克)后表现出强烈或轻微的处理诱导戒断惊厥。仅经过一代选择后,HAW品系的酒精戒断严重程度评分就显著高于LAW品系;到第四个选择代时,品系差异的幅度达到了8倍。我们测试了这些品系在使用苯二氮䓬类药物地西泮、气态麻醉剂氧化亚氮、咪唑吡啶类药物唑吡坦和巴比妥类药物戊巴比妥后戒断惊厥的严重程度。在所有情况下,HAW小鼠的戒断严重程度都显著高于LAW品系的小鼠。这些结果表明,一些影响乙醇戒断惊厥严重程度的基因也会影响从其他中枢神经系统抑制剂的戒断。D2小鼠对多种惊厥剂比B6小鼠更敏感(并且有更严重的戒断惊厥)。因此,我们测试了两个选择性培育品系的单独小鼠组对戊四氮(PTZ)、N-甲基-D-天冬氨酸(NMDA)和 kainic 酸(KA)的阈值敏感性。未检测到品系差异。这些结果表明,影响从几种抑制剂药物戒断严重程度的基因与影响对GABA能或谷氨酸能惊厥剂易感性的基因在很大程度上是不同的。

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