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一种细胞色素 P450 表型检测鸡尾酒在女性志愿者中引起意外不良反应。

A cytochrome P450 phenotyping cocktail causing unexpected adverse reactions in female volunteers.

机构信息

Institute of Public Health, Clinical Pharmacology, University of Southern Denmark, J.B. Winslowsvej 19, 5000, Odense, Denmark,

出版信息

Eur J Clin Pharmacol. 2013 Dec;69(12):1997-9. doi: 10.1007/s00228-013-1561-1. Epub 2013 Aug 6.

DOI:10.1007/s00228-013-1561-1
PMID:23917460
Abstract

BACKGROUND

A four-drug cytochrome P450 (CYP) phenotyping cocktail was developed to rapidly and safely determine CYP2D6, CYP2C19, CYP2C9 and CYP1A2 enzyme activity and phenotype.

METHODS

The cocktail consisted of the single CYP phenotyping probes of 50 mg tramadol (CYP2D6), 20 mg omeprazole (CYP2C19), 25 mg losartan (CYP2C9) and 200 mg caffeine (CYP1A2) and was administered as a single oral dose. For enzyme activity measurements, urine was collected as 8 h post-administration and blood was sampled at 4 h. The enzyme activity was determined by metabolic ratios of molar concentrations of the drugs and their enzyme catalyzed metabolites and was correlated to the relevant genotypes.

RESULTS

In a pilot study in 12 healthy male volunteers the CYP genotype-phenotype correlation and robustness of the cocktail was successfully determined without detection of any adverse drug reactions. In the subsequent population study, four female volunteers experienced unexpected and unacceptable moderate and severe adverse reactions (ARs) of headache, dizziness, nausea, vomiting, blue fingers, nails and lips and difficulties in urinating, which led to the study being prematurely terminated after inclusion of only 22 subjects (15 males, 7 females) [corrected].

CONCLUSION

Attention must be paid to adverse reactions when designing new combinations of phenotype cocktails regardless of the doses and drugs involved. We specifically warn against the combination of tramadol, omeprazole, losartan and caffeine.

摘要

背景

开发了一种包含四种药物的细胞色素 P450(CYP)表型鸡尾酒,以快速、安全地测定 CYP2D6、CYP2C19、CYP2C9 和 CYP1A2 酶活性和表型。

方法

该鸡尾酒由单 CYP 表型探针组成,包括 50 毫克曲马多(CYP2D6)、20 毫克奥美拉唑(CYP2C19)、25 毫克氯沙坦(CYP2C9)和 200 毫克咖啡因(CYP1A2),作为单次口服剂量给药。为了进行酶活性测量,在给药后 8 小时收集尿液,并在 4 小时时抽取血液样本。酶活性通过药物和其酶催化代谢物摩尔浓度的代谢比来确定,并与相关基因型相关联。

结果

在 12 名健康男性志愿者的初步研究中,成功确定了 CYP 基因型-表型相关性和鸡尾酒的稳健性,未检测到任何不良反应。在随后的人群研究中,有 4 名女性志愿者经历了意想不到的、无法接受的中度和重度不良反应(ARs),包括头痛、头晕、恶心、呕吐、蓝手指、指甲和嘴唇以及排尿困难,这导致在仅纳入 22 名受试者(15 名男性,7 名女性)后提前终止了研究[纠正]。

结论

无论涉及的剂量和药物如何,在设计新的表型鸡尾酒组合时都必须注意不良反应。我们特别警告不要将曲马多、奥美拉唑、氯沙坦和咖啡因组合使用。

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