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Impact of CYP2C19 phenotypes on escitalopram metabolism and an evaluation of pupillometry as a serotonergic biomarker

机译:CYP2C19表型对艾司西酞普兰代谢的影响和瞳孔测量的评估作为血清素能生物标志物

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摘要

PURPOSE: To investigate the impact of cytochrome P450 2C19 (CYP2C19) phenotypes on escitalopram metabolism and to evaluate pupillometry as a serotonergic biomarker. METHODS: This was a double-blind, crossover design study with single and multiple doses of 10 mg escitalopram and placebo in panels of CYP2C19 extensive (EM) and poor metabolisers (PM). Pupillometry was measured by a NeurOptics Pupillometer-PLR. RESULTS: Five PM and eight EM completed the study. The CYP2C19 phenotype significantly affected the metabolism of escitalopram. The area under the time-plasma concentration curve (AUC(0-24)) was 1.8-fold higher in PM than in EM after both single and multiple doses. Escitalopram treatment did not affect the maximum pupil size, but it did statistically significantly decrease the relative amplitude of the pupil light reflex compared to the placebo; this effect was equal in both phenotype groups. CONCLUSIONS: The CYP2C19 polymorphism affects escitalopram metabolism, but the difference does not justify dose adjustment. The puzzling results from pupillometry can be due to interplay between a central and a local serotonergic effect. Based on these results, pupillometry can not be recommended as a serotonergic biomarker.
机译:目的:研究细胞色素P450 2C19(CYP2C19)表型对依他普仑代谢的影响,并评价瞳孔测量法作为血清素能生物标志物。方法:这是一项双盲,交叉设计研究,在CYP2C19广泛(EM)和弱代谢者(PM)组中单次和多次服用10 mg依他普仑和安慰剂。瞳孔测定法是通过NeurOptics Pupillometer-PLR测量的。结果:五个下午和八个EM完成了研究。 CYP2C19表型显着影响依他普仑的代谢。在单次和多次给药后,PM的时间血浆浓度曲线下面积(AUC(0-24))比EM高1.8倍。依西酞普兰治疗不影响最大瞳孔大小,但与安慰剂相比,统计学上显着降低了瞳孔光反射的相对幅度。在两个表型组中,这种效果均相同。结论:CYP2C19基因多态性影响依他普仑的代谢,但该差异不能证明剂量调整是合理的。瞳孔测量法令人困惑的结果可能是由于中央和局部血清素能作用之间的相互作用。基于这些结果,不能推荐使用瞳孔测量法作为血清素能生物标志物。

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