去甲右美沙芬-美芬妥因-表型患者中口服和输注西酞普兰治疗后西酞普兰对映体的血浆浓度和心血管效应与主要抑郁症。

Plasma Concentrations and Cardiovascular Effects of Citalopram Enantiomers After Oral Versus Infusion Citalopram Therapy in Dextromethorphan-Mephenytoin-Phenotyped Patients With Major Depression.

机构信息

Department of Psychiatry, University Hospital of Lausanne (DP-CHUV), Prilly-Lausanne, Switzerland.

Service de Psychiatrie II, University of Strasbourg, Strasbourg, France.

出版信息

Ther Drug Monit. 2021 Jun 1;43(3):436-442. doi: 10.1097/FTD.0000000000000824.

DOI:10.1097/FTD.0000000000000824

PMID:33060488

Abstract

BACKGROUND

Authors compared plasma concentrations of citalopram (CIT) enantiomers and their metabolites in patients with depression administered either intravenously (IV) or as oral racemic CIT. Then, plasma concentrations were related to the metabolism of probes used for phenotyping patients with depression for CYP2C19 and CYP2D6 activity and cardiovascular functions.

METHODS

Dextromethorphan-mephenytoin-phenotyped patients with depression were administered racemic CIT (days 1 and 2: 20 mg/d; days 3-10: 40 mg/d) either orally or as a slow-drop infusion for 10 days and were then orally administered the drug for another 32 days. Blood probes were collected at the time of minimal and maximal concentrations on day 10, immediately before and 2 hours after drug administration, and on days 21 and 42. Plasma CIT and its metabolites were assayed by stereoselective high-performance liquid chromatography.

RESULTS

The following concentrations (ng/mL) were noted in the group receiving active IV infusion (IV-POS group, n = 27) of racemic CIT on day 10, before drug administration: escitalopram (S-CIT): 24 ± 10.2; R-citalopram (R-CIT): 45 ± 14.5; S-desmethyl-CIT: 13 ± 4.4; and R-desmethyl-CIT: 17 ± 8.2. In patients receiving oral administration (POS-POS group, n = 25), the values were 30 ± 12.7, 51 ± 17.4, 13 ± 4.6, and 17 ± 7.9 ng/mL, respectively. In the IV-POS group, 3 patients were poor dextromethorphan (CYP2D6) metabolizers; in the POS-POS group, one was a poor mephenytoin (CYP2C19) metabolizer. On day 10, before CIT treatment, S/R-CIT and S/R-mephenytoin ratios were significantly correlated, determined at baseline. Overall, CIT reduced the heart rate but did not significantly modify QTc. No relationship was found between any cardiovascular parameters and pharmacokinetic and pharmacogenetic data.

CONCLUSIONS

Owing to CIT's high bioavailability, the plasma concentrations of its enantiomers remained largely independent on the administration route. CYP2C19 preferentially demethylated S-CIT after CIT therapy.

摘要

背景

作者比较了抑郁症患者静脉注射（IV）或口服消旋西酞普兰（CIT）时西酞普兰（CIT）对映体及其代谢物的血浆浓度。然后，将血浆浓度与用于对抑郁症患者进行表型分析的探针的代谢相关联，这些探针用于 CYP2C19 和 CYP2D6 活性和心血管功能。

方法

右美沙芬-美芬妥因-表型患者接受口服或静脉输注西酞普兰（第 1 天和第 2 天：20 mg/d；第 3-10 天：40 mg/d），每天 10 天，然后再口服药物 32 天。在第 10 天最小和最大浓度时、给药前、给药后 2 小时以及第 21 天和第 42 天采集血液探针。通过立体选择性高效液相色谱法测定血浆西酞普兰及其代谢物。

结果

在接受活性 IV 输注（IV-POS 组，n = 27）的患者中，在第 10 天，在给药前，注意到以下浓度（ng/mL）：艾司西酞普兰（S-CIT）：24 ± 10.2；R-西酞普兰（R-CIT）：45 ± 14.5；S-去甲基西酞普兰：13 ± 4.4；和 R-去甲基西酞普兰：17 ± 8.2。在接受口服给药的患者（POS-POS 组，n = 25）中，值分别为 30 ± 12.7、51 ± 17.4、13 ± 4.6 和 17 ± 7.9 ng/mL。在 IV-POS 组中，有 3 名患者是差的右美沙芬（CYP2D6）代谢物；在 POS-POS 组中，1 名患者是差的美芬妥因（CYP2C19）代谢物。在第 10 天，CIT 治疗前，S/R-CIT 和 S/R-美芬妥因的比值在基线时显著相关。总体而言，CIT 降低了心率，但对 QTc 没有显著影响。未发现任何心血管参数与药代动力学和遗传药理学数据之间存在关系。