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吸烟诱导的细胞色素P450(CYP)1A2和多态性CYP2D6在奥氮平稳态浓度中的作用。

Role of the smoking-induced cytochrome P450 (CYP)1A2 and polymorphic CYP2D6 in steady-state concentration of olanzapine.

作者信息

Carrillo Juan Antonio, Herráiz Angustias G, Ramos Sara Isabel, Gervasini Guillermo, Vizcaíno Sonia, Benítez Julio

机构信息

Department of Pharmacology and Psychiatry, Extremadura University School of Medicine, Badajoz, Spain.

出版信息

J Clin Psychopharmacol. 2003 Apr;23(2):119-27. doi: 10.1097/00004714-200304000-00003.

DOI:10.1097/00004714-200304000-00003
PMID:12640212
Abstract

This study investigated whether the smokinginducible cytochrome P450 (CYP) 1A2 and the polymorphic CYP2D6 play significant roles in the metabolism of olanzapine and its clinical effects at steady-state treatment. Caffeine and debrisoquine were used as measures of CYP1A2 and CYP2D6, respectively. After drug therapy for 15 days, the effect of olanzapine on the activities of CYP1A2 and CYP2D6 was also examined. Seventeen psychiatric patients (9 men and 8 women) were orally administered olanzapine, at a mean +/- standard deviation (SD) dosage of 10 mg/d for all smokers (n = 8) and 7.5 +/- 2.5 mg/d (range, 5-10 mg) for nonsmokers (n = 9;p <0.01). The plasma concentration-to-dose (C:D) ratio was closely correlated to the CYP1A2 activity ( s = -0.89;p <0.0001). The mean urinary caffeine indexes of nonsmokers and smokers were 17 +/- 8 and 101 +/- 44, respectively, indicating that smoking had induced a sixfold higher CYP1A2 activity (p <0.0001). Likewise, the olanzapine plasma C:D ratio (ng.mL.mg) was about fivefold lower in smokers (7.9 +/- 2.6) than in nonsmokers (1.56 +/- 1.1;p <0.0001). On day 15 of the antipsychotic therapy, the percentage decrease in Brief Psychiatric Rating Scale (BPRS) total score relative to the predosing score (in the drug-free period) was higher for nonsmokers than for smokers (30.4 +/- 10% vs. 12.5 +/- 14%;p <0.01). Six nonsmokers and three smokers experienced side effects with olanzapine. After 15 days of drug treatment, olanzapine had caused significant (p <0.0001) and substantial CYP1A2 inhibition (by 50%) in comparison with predosing values, and such inhibition can contribute to adverse drug interactions. In conclusion, smoking-induced increased CYP1A2 activity significantly diminished plasma olanzapine concentrations and the antipsychotic effect of the drug. The performance of a simple caffeine test may assist in individualization of the olanzapine dosage.

摘要

本研究调查了吸烟诱导型细胞色素P450(CYP)1A2和多态性CYP2D6在奥氮平代谢及其稳态治疗临床效果中是否起重要作用。分别使用咖啡因和异喹胍作为CYP1A2和CYP2D6的检测指标。在药物治疗15天后,还检测了奥氮平对CYP1A2和CYP2D6活性的影响。17名精神科患者(9名男性和8名女性)口服奥氮平,所有吸烟者(n = 8)的平均±标准差(SD)剂量为10 mg/d,非吸烟者(n = 9;p <0.01)的剂量为7.5±2.5 mg/d(范围为5 - 10 mg)。血浆浓度与剂量(C:D)比值与CYP1A2活性密切相关(r = -0.89;p <0.0001)。非吸烟者和吸烟者的平均尿咖啡因指数分别为17±8和101±44,表明吸烟使CYP1A2活性升高了6倍(p <0.0001)。同样,吸烟者的奥氮平血浆C:D比值(ng·mL·mg)(7.9±2.6)比非吸烟者(1.56±1.1;p <0.0001)低约5倍。在抗精神病治疗的第15天,非吸烟者的简明精神病评定量表(BPRS)总分相对于给药前评分(在无药期)的下降百分比高于吸烟者(30.4±10%对12.5±14%;p <0.01)。6名非吸烟者和3名吸烟者出现了奥氮平的副作用。药物治疗15天后,与给药前值相比,奥氮平导致了显著的(p <0.0001)且大幅度的CYP1A2抑制(达50%),这种抑制可能导致药物不良相互作用。总之,吸烟诱导的CYP1A2活性增加显著降低了血浆奥氮平浓度和药物的抗精神病效果。进行简单的咖啡因检测可能有助于奥氮平剂量的个体化。

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