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利用重复抽取脑脊液对未束缚的个体大鼠同时进行卡马西平中枢浓度、递质胺代谢及运动活性的监测。

Concurrent monitoring of central carbamazepine and transmitter amine metabolism and motor activity in individual unrestrained rats using repetitive withdrawal of cerebrospinal fluid.

作者信息

Sokomba E N, Patsalos P N, Lolin Y I, Curzon G

机构信息

Department of Neurochemistry, Institute of Neurology, London.

出版信息

Neuropharmacology. 1988 Apr;27(4):409-15. doi: 10.1016/0028-3908(88)90150-5.

DOI:10.1016/0028-3908(88)90150-5
PMID:2901673
Abstract

A method for repeated withdrawal of cerebrospinal fluid (CSF) from the cisterna magna was used in a pharmacokinetic and behavioural study of conscious, freely-moving rats, given the antiepileptic drug carbamazepine (35 mg/kg i.p.). Pharmacokinetic constants (i.e. time to peak concentration, peak concentration, area under the curve and t 1/2) for the drug and its primary metabolite carbamazepine-10,11-epoxide and also concentrations of acidic metabolites of 5-hydroxytryptamine and dopamine were obtained for the CSF of individual rats. A pharmacodynamic constant, the effective concentration of drug in CSF for 50% inhibition of motor activity was also determined for each animal. The above data provides good indices of the corresponding values for carbamazepine and its metabolite in brain insofar as a separate experiment showed good correlations between CSF and brain for concentrations of both the drug and its metabolite. Carbamazepine appeared to be largely responsible for the depression of motor activity as the metabolite, at the levels attained, seemed to have little effect. The changes in motor activity were not associated with altered concentrations of the metabolites of 5-hydroxytryptamine or dopamine in the CSF. While the investigation did not reveal major advantages in monitoring the drug under study in CSF rather than in serum it illustrates the potential of the CSF method as a simple way to obtain neuropharmacokinetic and neuropharmacodynamic profiles of the action of drugs in individual rats.

摘要

在一项药代动力学和行为学研究中,对清醒、自由活动的大鼠腹腔注射抗癫痫药物卡马西平(35毫克/千克),采用了从枕大池反复抽取脑脊液(CSF)的方法。获得了该药物及其主要代谢产物卡马西平-10,11-环氧化物的药代动力学常数(即达峰时间、峰浓度、曲线下面积和t1/2),以及个体大鼠脑脊液中5-羟色胺和多巴胺酸性代谢产物的浓度。还为每只动物测定了一个药效学常数,即脑脊液中抑制50%运动活动的药物有效浓度。上述数据为卡马西平及其代谢产物在脑中的相应值提供了良好指标,因为一项单独实验表明,药物及其代谢产物在脑脊液和脑中的浓度之间具有良好的相关性。卡马西平似乎在很大程度上导致了运动活动的抑制,因为在所达到的水平上,代谢产物似乎几乎没有作用。运动活动的变化与脑脊液中5-羟色胺或多巴胺代谢产物浓度的改变无关。虽然该研究没有揭示在脑脊液而非血清中监测所研究药物的主要优势,但它说明了脑脊液方法作为一种获取个体大鼠药物神经药代动力学和神经药效学作用概况的简单方法的潜力。

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