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4β-羟基胆固醇水平与精神科患者 CYP3A4 底物喹硫平的稳态血清浓度显著相关。

4β-Hydroxycholesterol level significantly correlates with steady-state serum concentration of the CYP3A4 substrate quetiapine in psychiatric patients.

机构信息

Center for Psychopharmacology, Diakonhjemmet Hospital, Oslo, Norway.

NORMENT, KG Jebsen Centre for Psychosis Research, Institute of Clinical Medicine, University of Oslo, Oslo, Norway.

出版信息

Br J Clin Pharmacol. 2017 Nov;83(11):2398-2405. doi: 10.1111/bcp.13341. Epub 2017 Jul 21.

Abstract

AIM

4β-Hydroxycholesterol (4βOHC) is sensitive towards induction or inhibition of CYP3A4, but its potential usefulness as a dosing biomarker remains to be demonstrated. The aim of this study was to investigate the correlation between 4βOHC levels and steady-state concentrations (Css) of quetiapine, a CYP3A4 substrate with high presystemic metabolism, in psychiatric patients.

METHODS

Serum samples from 151 patients treated with quetiapine as immediate release (IR; n = 98) or slow release (XR; n = 53) tablets were included for analysis of 4βOHC. In all patients, Css of quetiapine had been measured at trough level, i.e. 10-14 and 17-25 h post-dosing for IR and XR tablets, respectively. Correlations between 4βOHC levels and dose-adjusted Css (C/D ratios) of quetiapine were tested by univariate (Spearman's) and multivariate (multiple linear regression) analyses. Gender, age (≥60 vs. <60 years) and tablet formulation were included as potential covariates in the multivariate analysis.

RESULTS

Correlations between 4βOHC levels and quetiapine C/D ratios were highly significant both for IR- and XR-treated patients (P < 0.0001). Estimated Spearman r values were -0.47 (95% confidence interval -0.62, -0.30) and -0.56 (-0.72, -0.33), respectively. The relationship between 4βOHC level and quetiapine C/D ratio was also significant in the multiple linear regression analysis (P < 0.001), including gender (P = 0.023) and age (P = 0.003) as significant covariates.

CONCLUSIONS

The present study shows that 4βOHC level is significantly correlated with steady-state concentration of quetiapine. This supports the potential usefulness of 4βOHC as a phenotype biomarker for individualized dosing of quetiapine and other drugs where systemic exposure is mainly determined by CYP3A4 metabolism.

摘要

目的

4β-羟基胆固醇(4βOHC)对 CYP3A4 的诱导或抑制较为敏感,但作为剂量标志物的潜在用途仍有待证实。本研究旨在探讨精神科患者中,4βOHC 水平与 CYP3A4 高首过代谢底物喹硫平的稳态浓度(Css)之间的相关性。

方法

纳入 151 例接受喹硫平(速释片,n=98;控释片,n=53)治疗的患者血清样本进行 4βOHC 分析。所有患者均在谷浓度时(即速释片和控释片分别为给药后 10-14 和 17-25 h)测定了喹硫平的 Css。通过单变量(Spearman 相关)和多变量(多元线性回归)分析来检验 4βOHC 水平与喹硫平剂量调整 Css(C/D 比值)之间的相关性。在多变量分析中,将性别、年龄(≥60 岁与<60 岁)和片剂制剂纳入潜在协变量。

结果

对于速释片和控释片治疗的患者,4βOHC 水平与喹硫平 C/D 比值之间的相关性均非常显著(P<0.0001)。估计的 Spearman r 值分别为-0.47(95%置信区间-0.62,-0.30)和-0.56(-0.72,-0.33)。在多元线性回归分析中,4βOHC 水平与喹硫平 C/D 比值之间的关系也具有统计学意义(P<0.001),包括性别(P=0.023)和年龄(P=0.003)作为显著协变量。

结论

本研究表明,4βOHC 水平与喹硫平的稳态浓度显著相关。这支持了 4βOHC 作为喹硫平和其他主要由 CYP3A4 代谢决定全身暴露的药物个体化给药的表型生物标志物的潜在用途。

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