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细胞色素 P450 2C19 酶、细胞色素 P450 2C9 酶和细胞色素 P450 2D6 酶等位基因变异及其对药物代谢的可能影响:一项回顾性研究。

Cytochrome P450 2C19 enzyme, Cytochrome P450 2C9 enzyme, and Cytochrome P450 2D6 enzyme allelic variants and its possible effect on drug metabolism: A retrospective study.

机构信息

Faculty of Pharmacy, Lithuanian University of Health Sciences.

Department of Genetics and Molecular Medicine, Hospital of Lithuanian University of Health Sciences.

出版信息

Medicine (Baltimore). 2021 Mar 19;100(11):e24545. doi: 10.1097/MD.0000000000024545.

Abstract

The objective of the present study was to assess the allelic variations of Cytochrome P450 (CYP) enzymes Cytochrome P450 2C19 (CYP2C19), Cytochrome P450 2C9 (CYP2C9), and Cytochrome P450 2D6 (CYP2D6) as they play a major role in drug metabolism. The interindividual genetic variabilities of these enzymes can account for different responsiveness as well as concentration fluctuations for a particular drug.During the period of 2017 to 2018 a total of 54 patients have received pharmacogenetic testing at the Department of Genetics and Molecular Medicine at Kaunas Clinics. According to the genotype-metabolic phenotypes of CYP2C19, CYP2D6, CYP2C9 enzymes patients were classified according to the guidelines by Clinical Pharmacogenetics Implementation Consortium (CPIC): normal metabolizers (NMs), intermediate metabolizers (IMs), rapid metabolizers (RMs), ultrarapid metabolizers (UMs), and poor metabolizers (PMs).CYP2C19 enzyme allelic distribution: 18 patients (33.33%) with ∗1/∗1 genotype were NMs; 14 patients (25.93%) with ∗1/∗2; ∗2/∗17 genotypes were classified as IMs; 15 patients (27.78%) possessed ∗1/∗17 genotype and were RMs; 4 patients (7.4%) had ∗17/∗17 genotype with increased enzyme activity compared with RMs, were classified as UMs; 3 patients (5.56%) had ∗2/∗2 genotype and were marked as PMs. CYP2D6 enzyme allelic distribution: 26 patients (48.148%) contained ∗1/∗1,∗2/∗2,∗1/∗2,∗1/∗41,∗2/∗41 genotypes with normal enzymatic function so were accounted as NMs; 21 patients (38.89%) with ∗1/∗5, ∗2/∗4, ∗10/∗41, ∗1/∗4, ∗1/∗3, ∗2/∗5, ∗2/∗4, ∗2/∗6 genotypes were accounted as IMs; 2 patients (3.7%) possessed ∗2XN genotype and were accounted as UMs and 5 patients (9.26%) possessed ∗4/∗5,∗4/∗10,∗4/∗9,∗4/∗41 genotypes and had non-functional enzymatic activity so were accounted as PMs; CYP2C9 enzyme allelic distribution: 44 patients (81.48%) with∗1/∗1 genotype were NMs; 10 patients (18.52%) with ∗1/∗2;∗1/∗3 genotypes were IMs.The results of our study indicate that deviations from the normal enzymatic activity is common amongst Lithuanian people and combinatory genotyping of CYP2D6, CYP2C9, and CYP2C19 has to be promoted as an advanced method because of most commonly prescribed medicines like analgesics, antihypertensive, antidepressants are metabolized by multiple pathways involving enzymes in the CYP450 family.

摘要

本研究的目的是评估细胞色素 P450(CYP)酶细胞色素 P450 2C19(CYP2C19)、细胞色素 P450 2C9(CYP2C9)和细胞色素 P450 2D6(CYP2D6)的等位基因变异,因为它们在药物代谢中起着重要作用。这些酶的个体遗传变异性可以解释特定药物的不同反应性和浓度波动。

在 2017 年至 2018 年期间,共有 54 名患者在考纳斯诊所的遗传学部接受了遗传药理学检测。根据 CYP2C19、CYP2D6 和 CYP2C9 酶的基因型-代谢表型,根据临床药物遗传学实施联盟(CPIC)的指南,患者被分类为:正常代谢者(NMs)、中间代谢者(IMs)、快速代谢者(RMs)、超快代谢者(UMs)和不良代谢者(PMs)。

CYP2C19 酶等位基因分布:18 名(33.33%)具有∗1/∗1 基因型的患者为 NMs;14 名(25.93%)具有∗1/∗2;∗2/∗17 基因型的患者为 IMs;15 名(27.78%)具有∗1/∗17 基因型且酶活性高于 RMs 的患者为 RMs;4 名(7.4%)具有∗17/∗17 基因型,与 RMs 相比,酶活性增加,被归类为 UMs;3 名(5.56%)具有∗2/∗2 基因型,被标记为 PMs。

CYP2D6 酶等位基因分布:26 名(48.148%)患者含有具有正常酶功能的∗1/∗1、∗2/∗2、∗1/∗2、∗1/∗41、∗2/∗41 基因型,被归类为 NMs;21 名(38.89%)患者具有∗1/∗5、∗2/∗4、∗10/∗41、∗1/∗4、∗1/∗3、∗2/∗5、∗2/∗4、∗2/∗6 基因型,被归类为 IMs;2 名(3.7%)患者具有∗2XN 基因型,被归类为 UMs,5 名(9.26%)患者具有∗4/∗5、∗4/∗10、∗4/∗9、∗4/∗41 基因型,且无功能性酶活性,被归类为 PMs;

CYP2C9 酶等位基因分布:44 名(81.48%)具有∗1/∗1 基因型的患者为 NMs;10 名(18.52%)具有∗1/∗2;∗1/∗3 基因型的患者为 IMs。

我们的研究结果表明,立陶宛人普遍存在正常酶活性的偏差,并且由于最常开的药物如止痛药、抗高血压药、抗抑郁药是由涉及 CYP450 家族酶的多种途径代谢的,因此需要推广 CYP2D6、CYP2C9 和 CYP2C19 的组合基因分型作为一种先进的方法。

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