Unraveling the Role of COMT Polymorphism in Dopamine-Mediated Vasopressor Effects: An Observational Cross-Sectional Study.

IF 2.1 4区医学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY Current drug metabolism Pub Date : 2024-01-01 DOI:10.2174/0113892002293952240315064943

Kannan Sridharan, Anfal Jassim, Ali Mohammed Qader, Sheikh Abdul Azeez Pasha

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Abstract

Aims: To evaluate the association between rs4680 polymorphism in the COMT gene and the vasoconstrictive effects of commonly used vasopressors.

Background: Dopamine is a medication that is given intravenously to critically ill patients to help increase blood pressure. Catechol O-Methyl Transferase (COMT) breaks down dopamine and other catecholamines. There is a genetic variation in the COMT gene called rs4680 that can affect how well the enzyme works. Studies have shown that people with this genetic variation may have different blood pressure levels. However, no one has looked at how this genetic variation affects the way dopamine works to increase blood pressure.

Objectives: To investigate the impact of the rs4680 polymorphism in the COMT gene on the pharmacodynamic response to dopamine.

Methods: Critically ill patients administered dopamine were included following the consent of their legally acceptable representatives. Details on their demographic characteristics, diagnosis, drug-related details, changes in the heart rate, blood pressure, and urinary output were obtained. The presence of rs4680 polymorphism in the COMT gene was evaluated using a validated method.

Results: One hundred and seventeen patients were recruited, and we observed a prevalence of rs4680 polymorphism in 57.3% of our critically ill patients. Those with mutant genotypes were observed with an increase in the median rate of change in mean arterial pressure (mm Hg/hour) [wild: 8.9 (-22.6 to 49.1); heterozygous mutant: 5.9 (-34.1 to 61.6); and homozygous mutant: 19.5 (-2.5 to 129.2)] and lowered urine output (ml/day) [wild: 1080 (21.4 to 5900); heterozygous mutant: 380 (23.7 to 15800); and homozygous mutant: 316.7 (5.8 to 2308.3)].

Conclusion: V158M (rs4680) polymorphism is widely prevalent in the population and was significantly associated with altered effects as observed clinically. This finding suggests valuable insights into the molecular basis of COMT function and its potential impact on neurotransmitter metabolism and related disorders. Large-scale studies delineating the effect of these polymorphisms on various vasopressors are the need of the hour.

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揭示 COMT 多态性在多巴胺介导的血管加压效应中的作用：一项观察性横断面研究。

目的：评估 COMT 基因 rs4680 多态性与常用血管加压药的血管收缩效应之间的关联：背景：多巴胺是一种静脉注射给危重病人以帮助升高血压的药物。儿茶酚 O-甲基转移酶（COMT）可分解多巴胺和其他儿茶酚胺。COMT 基因中有一种名为 rs4680 的遗传变异，会影响这种酶的工作效率。研究表明，有这种基因变异的人可能会有不同的血压水平。然而，还没有人研究过这种基因变异如何影响多巴胺增加血压的作用方式：研究 COMT 基因 rs4680 多态性对多巴胺药效学反应的影响：方法：在征得合法代表的同意后，纳入使用多巴胺的重症患者。研究人员详细了解了患者的人口统计学特征、诊断、药物相关细节、心率、血压和尿量的变化。采用一种有效的方法评估了 COMT 基因中 rs4680 多态性的存在：我们共招募了 117 名患者，观察到 57.3% 的重症患者存在 rs4680 多态性。观察到突变基因型患者的平均动脉压（毫米汞柱/小时）中位数变化率增加[野生型：8.9（-22.6 至 49.1）；杂合子突变型：5.9（-34.1 至 61.6）；杂合子突变体：19.5（-2.5 至 129.2）]和尿量减少（毫升/天）[野生：1080（21.4 至 5900）；杂合子突变体：380（23.7 至 15800）；杂合子突变体：316.7（5.8 至 2308.3）]：V158M（rs4680）多态性在人群中广泛流行，与临床观察到的效应改变有显著关联。这一发现有助于深入了解 COMT 功能的分子基础及其对神经递质代谢和相关疾病的潜在影响。目前需要进行大规模研究，以确定这些多态性对各种血管加压素的影响。

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来源期刊

Current drug metabolism 医学-生化与分子生物学

CiteScore

4.30

自引率

4.30%

发文量

审稿时长

4-8 weeks

期刊介绍： Current Drug Metabolism aims to cover all the latest and outstanding developments in drug metabolism, pharmacokinetics, and drug disposition. The journal serves as an international forum for the publication of full-length/mini review, research articles and guest edited issues in drug metabolism. Current Drug Metabolism is an essential journal for academic, clinical, government and pharmaceutical scientists who wish to be kept informed and up-to-date with the most important developments. The journal covers the following general topic areas: pharmaceutics, pharmacokinetics, toxicology, and most importantly drug metabolism. More specifically, in vitro and in vivo drug metabolism of phase I and phase II enzymes or metabolic pathways; drug-drug interactions and enzyme kinetics; pharmacokinetics, pharmacokinetic-pharmacodynamic modeling, and toxicokinetics; interspecies differences in metabolism or pharmacokinetics, species scaling and extrapolations; drug transporters; target organ toxicity and interindividual variability in drug exposure-response; extrahepatic metabolism; bioactivation, reactive metabolites, and developments for the identification of drug metabolites. Preclinical and clinical reviews describing the drug metabolism and pharmacokinetics of marketed drugs or drug classes.