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Development and validation of the maximal electro-shock seizure model in dogs

机译:犬最大电击惊厥模型的建立和验证

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The development and validation of the maximal electro-shock (MES) model using phenobarbital (Pb) as the positive control is described. This approach builds on previous work in rodent model systems, and has been adapted to dogs as a tool for pharmaceutical dose selection. Dogs, like rodents, exhibit generalized convulsions which manifest as progressive clinical signs in a dose (electrical current) dependent fashion. At the limit (300 mA, 200 msec) animals underwent clonic-tonic convulsions consistent with complete generalized (Grand Mal) seizures with a grade 3 clinical score (CS) and a menace response time of 98.5 +/- 24.4 sec (n = 8). Pretreatment of animals with Pb at 3, 10, and 30 mg/kg, in a 4-by-4 complete block crossover design (Latin-Square), resulted in a dose-dependant reduction in CS and menace response time. Estimates of plasma Pb concentration taken prior to MES induction showed a similar dose-dependent reduction in CS and menace response time with concentration. Using a cumulative logistic regression model, a predicted 50% probability of a CS = 1 was approximately 11.4 mg/kg. In addition, plasma Pb concentrations predicted a 50% probability of a CS = 1 occurs at plasma Pb concentration of approximately 16.0 mug/mL. Combined these data suggest that MES is a useful model for evaluating generalized convulsions in canines and may provide a tool for dose selection of novel pharmaceutical compounds.
机译:描述了使用苯巴比妥(Pb)作为阳性对照的最大电击(MES)模型的开发和验证。这种方法建立在啮齿动物模型系统的先前工作的基础上,并且已经适应了作为药物剂量选择工具的犬类。狗像啮齿动物一样,表现出全身性惊厥,表现为剂量(电流)依赖性的渐进性临床体征。在极限(300 mA,200毫秒)时,动物经历阵挛性抽搐,与完全广义(大马尔代夫)癫痫发作一致,临床评分为3级(CS),威胁反应时间为98.5 +/- 24.4秒(n = 8) )。用4×4完全嵌段交叉设计(拉丁广场)对动物分别用3、10和30 mg / kg的Pb进行预处理,导致剂量依赖性地降低CS和威胁响应时间。在MES诱导之前对血浆Pb浓度的估计显示,CS浓度和威胁响应时间随浓度的降低呈类似的剂量依赖性降低。使用累积逻辑回归模型,预计CS = 1的50%概率约为11.4 mg / kg。另外,血浆铅浓度预测在血浆铅浓度约为16.0杯/毫升时发生CS = 1的可能性为50%。结合这些数据表明,MES是评估犬类全身性惊厥的有用模型,并且可以为新型药物化合物的剂量选择提供工具。

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