Association of the OPRM1 variant rs1799971 (A118G) and clinical manifestations in tramadol poisoned patients: a cross-sectional study.

IF 3 3区 医学 Q2 TOXICOLOGY Clinical Toxicology Pub Date : 2024-06-01 Epub Date: 2024-07-01 DOI:10.1080/15563650.2024.2366921
Ali Ershad, Sahel Shafiee Dolat Abadi, Melika Ebrahimian, Seyed Kaveh Hadeiy, Naghmeh Zamani, Ali-Asghar Kolahi, Abolfazl Movafagh, Hossein Hassanian-Moghaddam
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Abstract

Introduction: The opioid receptor mu1 is a protein coding gene that can have different codes for a protein and may have variations (polymorphisms) affecting how opioids work. The aim of this study was to investigate the prevalence of the most common opioid receptor mu1 polymorphism (A118G) and any relationship between this polymorphism and features following tramadol overdose.

Materials and methods: This was a cross-sectional study of patients admitted with tramadol poisoning to an Iranian hospital. These patients were not taking any other drugs or medications and had no history of seizures.

Results: The results showed that among the 83 patients included in the study, 57 (69 per cent) had the AA genotype, 25 (30 per cent) had the AG genotype, and one (1 per cent) had the GG genotype for the opioid receptor mu1 A118G polymorphism. Nausea and/or vomiting occurred in nine (11 per cent) patients and dizziness in 38 (46 per cent) patients. Serious adverse events included seizures in 51 (60 per cent) patients and respiratory failure requiring mechanical ventilation in 21 (25 per cent) patients. However, there was no significant association between the opioid receptor mu1 A118G polymorphism and these adverse events.

Discussion: In our study, the frequency of the A allele was greater than the G allele, and the AA genotype was more prevalent than AG. The GG genotype was the least common among the polymorphisms of opioid receptor mu1 rs1799971. There was no significant association between the opioid receptor mu1 A118G polymorphism and symptoms in tramadol-poisoned patients. Although these allele proportions are similar to the results reported in other Caucasian populations, they are dissimilar to the findings in Chinese and Singaporean populations. In these Asian studies, the predominant allele was the G allele. It has been suggested that a mutated G allele will decrease the production of opioid receptor mu1-related messenger ribonucleic acid and related proteins, leading to fewer mu-opioid receptors in the brain.

Conclusions: This study found no significant association between the opioid receptor mu1 A118G polymorphism and adverse outcomes in tramadol-poisoned patients. However, more research is needed to draw more definitive conclusions due to the limited evidence and variability of opioid receptor mu1 polymorphisms in different populations.

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OPRM1变异体rs1799971 (A118G)与曲马多中毒患者临床表现的关系:一项横断面研究。
导言:阿片受体mu1是一种蛋白质编码基因,它可以为一种蛋白质编码不同的代码,并且可能存在影响阿片类药物作用方式的变异(多态性)。本研究旨在调查最常见的阿片受体mu1多态性(A118G)的发生率以及该多态性与曲马多用药过量后的特征之间的关系:这是一项横断面研究,研究对象是伊朗一家医院收治的曲马多中毒患者。这些患者没有服用任何其他药物,也没有癫痫发作史:结果显示,在纳入研究的 83 名患者中,有 57 人(69%)具有阿片受体 mu1 A118G 多态性的 AA 基因型,25 人(30%)具有 AG 基因型,1 人(1%)具有 GG 基因型。9名患者(11%)出现恶心和/或呕吐,38名患者(46%)出现头晕。严重不良事件包括 51 例(60%)患者出现癫痫发作,21 例(25%)患者出现呼吸衰竭,需要机械通气。然而,阿片受体mu1 A118G多态性与这些不良事件之间没有明显关联:讨论:在我们的研究中,A 等位基因的频率高于 G 等位基因,AA 基因型比 AG 基因型更普遍。在阿片受体 mu1 rs1799971 的多态性中,GG 基因型最少见。阿片受体mu1 A118G多态性与曲马多中毒患者的症状无明显关联。虽然这些等位基因比例与其他高加索人群的结果相似,但与中国和新加坡人群的研究结果不同。在这些亚洲研究中,主要的等位基因是 G 等位基因。有人认为,G 等位基因突变会减少阿片受体μ1 相关信使核糖核酸和相关蛋白质的产生,从而导致大脑中的μ阿片受体减少:本研究发现,阿片受体mu1 A118G多态性与曲马多中毒患者的不良预后无明显关联。然而,由于证据有限以及阿片受体mu1多态性在不同人群中的变异性,要得出更明确的结论还需要更多的研究。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Clinical Toxicology
Clinical Toxicology 医学-毒理学
CiteScore
5.70
自引率
12.10%
发文量
148
审稿时长
4-8 weeks
期刊介绍: clinical Toxicology publishes peer-reviewed scientific research and clinical advances in clinical toxicology. The journal reflects the professional concerns and best scientific judgment of its sponsors, the American Academy of Clinical Toxicology, the European Association of Poisons Centres and Clinical Toxicologists, the American Association of Poison Control Centers and the Asia Pacific Association of Medical Toxicology and, as such, is the leading international journal in the specialty.
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