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多潘立酮治疗胃轻瘫:临床疗效和副作用的人口统计学和药物遗传学特征。

Domperidone treatment for gastroparesis: demographic and pharmacogenetic characterization of clinical efficacy and side-effects.

机构信息

Gastroenterology Section, School of Medicine, Temple University School of Medicine, Parkinson Pavilion, 8th floor, 3401 North Broad Street, Philadelphia, PA 19140, USA.

出版信息

Dig Dis Sci. 2011 Jan;56(1):115-24. doi: 10.1007/s10620-010-1472-2. Epub 2010 Nov 10.

Abstract

BACKGROUND

Domperidone is a useful alternative to metoclopramide for treatment of gastroparesis due to better tolerability. Effectiveness and side-effects from domperidone may be influenced by patient-related factors including polymorphisms in genes encoding drug-metabolizing enzymes, drug transporters, and domperidone targets.

AIMS

The aim of this study was to determine if demographic and pharmacogenetic parameters of patients receiving domperidone are associated with response to treatment or side-effects.

METHODS

Patients treated with domperidone for gastroparesis provided saliva samples from which DNA was extracted. Fourteen single-nucleotide polymorphisms (SNPs) in seven candidate genes (ABCB1, CYP2D6, DRD2, KCNE1, KCNE2, KCNH2, KCNQ1) were used for genotyping. SNP microarrays were used to assess single-nucleotide polymorphisms in the ADRA1A, ADRA1B, and ADRA1D loci.

RESULTS

Forty-eight patients treated with domperidone participated in the study. DNA was successfully obtained from each patient. Age was associated with effectiveness of domperidone (p=0.0088). Genetic polymorphism in KCNH2 was associated with effectiveness of domperidone (p=0.041). The efficacious dose was associated with polymorphism in ABCB1 gene (p=0.0277). The side-effects of domperidone were significantly associated with the SNPs in the promoter region of ADRA1D gene.

CONCLUSIONS

Genetic characteristics associated with response to domperidone therapy included polymorphisms in the drug transporter gene ABCB1, the potassium channel KCNH2 gene, and α1D--adrenoceptor ADRA1D gene. Age was associated with a beneficial response to domperidone. If verified in a larger population, this information might be used to help determine which patients with gastroparesis might respond to domperidone and avoid treatment in those who might develop side-effects.

摘要

背景

多潘立酮的耐受性优于甲氧氯普胺,因此是治疗胃轻瘫的一种有效替代药物。多潘立酮的有效性和副作用可能受到患者相关因素的影响,包括编码药物代谢酶、药物转运体和多潘立酮靶标的基因的多态性。

目的

本研究旨在确定接受多潘立酮治疗的患者的人口统计学和药物遗传学参数是否与治疗反应或副作用相关。

方法

接受多潘立酮治疗胃轻瘫的患者提供唾液样本,从中提取 DNA。对七个候选基因(ABCB1、CYP2D6、DRD2、KCNE1、KCNE2、KCNH2、KCNQ1)中的 14 个单核苷酸多态性(SNP)进行基因分型。使用 SNP 微阵列评估 ADRA1A、ADRA1B 和 ADRA1D 基因座中的单核苷酸多态性。

结果

48 名接受多潘立酮治疗的患者参与了这项研究。每位患者的 DNA 均成功获得。年龄与多潘立酮的疗效相关(p=0.0088)。KCNH2 基因的遗传多态性与多潘立酮的疗效相关(p=0.041)。有效的剂量与 ABCB1 基因的多态性相关(p=0.0277)。多潘立酮的副作用与 ADRA1D 基因启动子区域的 SNP 显著相关。

结论

与多潘立酮治疗反应相关的遗传特征包括药物转运体基因 ABCB1、钾通道 KCNH2 基因和 α1D-肾上腺素能受体 ADRA1D 基因的多态性。年龄与多潘立酮的有益反应相关。如果在更大的人群中得到验证,这些信息可能有助于确定哪些胃轻瘫患者可能对多潘立酮有反应,并避免对可能出现副作用的患者进行治疗。

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