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首页> 外文期刊>Brain & Development >A major influence of CYP2C19 genotype on the steady-state concentration of N-desmethylclobazam.
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A major influence of CYP2C19 genotype on the steady-state concentration of N-desmethylclobazam.

机译:CYP2C19基因型对N-去甲基克洛赞的稳态浓度的主要影响。

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N-desmethylclobazam (N-CLB), the major metabolite of clobazam (CLB), exerts a large influence on therapeutic and adverse effects of CLB. A substantial inter-individual variability has been observed in the ratios of N-CLB concentration/CLB dose and of the N-CLB/CLB concentration. We document here a genotype-phenotype correlation between CYP2C19 polymorphisms and those ratios. Patients with two mutated CYP2C19 alleles show significantly higher ratios than those with the wild type genotype: patients with one mutated allele exhibited intermediate trait. That is, the degree of elevation in the ratios was dependent on the number of mutated alleles of CYP2C19 (gene-dose effect). The N-CLB concentration/CLB dose ratio of patients with two mutated alleles was more than six fold higher than that of wild type patients. Thus, the serum N-CLB/CLB concentration ratio may be a valuable parameter to screen for patients at risk for side effects. Such precautions may be clinically relevant in populations where the mutant allele frequency is high, such as in Asian populations ( approximately 35%). Patients co-medicated with CYP3A4 inducer showed lower CLB concentration/CLB dose ratios and higher N-CLB/CLB concentration ratios. The overall effect of CYP3A4 inducer on N-CLB metabolism, however, was small and, thus, we conclude that the CYP2C19 genotype is the major determinant of the N-CLB concentration. For this reason it is crucial for the better management of epilepsy and other chronic illnesses in general to establish the correlation of genotype of CYP enzymes and pharmacokinetics/dynamics of drugs.
机译:N-desmethylclobazam(N-CLB)是clobazam(CLB)的主要代谢产物,对CLB的治疗和不良反应影响很大。在N-CLB浓度/ CLB剂量与N-CLB / CLB浓度之比中观察到了很大的个体间差异。我们在此处记录了CYP2C19多态性与这些比率之间的基因型-表型相关性。 CYP2C19等位基因有两个突变的患者比野生型基因型的患者具有更高的比率:一个等位基因突变的患者表现出中间性状。即,比率的升高程度取决于CYP2C19的突变等位基因的数目(基因剂量效应)。具有两个突变等位基因的患者的N-CLB浓度/ CLB剂量比比野生型患者高六倍以上。因此,血清N-CLB / CLB浓度比可能是筛查有副作用风险的患者的重要参数。此类预防措施在突变等位基因频率较高的人群中,例如在亚洲人群中(约35%),在临床上可能是相关的。与CYP3A4诱导剂合用的患者显示出较低的CLB浓度/ CLB剂量比和较高的N-CLB / CLB浓度比。 CYP3A4诱导剂对N-CLB代谢的总体作用很小,因此,我们得出结论,CYP2C19基因型是N-CLB浓度的主要决定因素。由于这个原因,对于总体上更好地治疗癫痫和其他慢性疾病至关重要的是,确定CYP酶基因型与药物的药代动力学/动力学之间的相关性。

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