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麻醉实践中镇痛药的药物基因组学:文献最新综述

Pharmacogenomics of analgesics in anesthesia practice: A current update of literature.

作者信息

Gray Keith, Adhikary Sanjib D, Janicki Piotr

机构信息

Department of Anesthesiology and Perioperative Medicine, Penn State College of Medicine, Hershey, Pennsylvania, USA.

出版信息

J Anaesthesiol Clin Pharmacol. 2018 Apr-Jun;34(2):155-160. doi: 10.4103/joacp.JOACP_319_17.

DOI:10.4103/joacp.JOACP_319_17
PMID:30104820
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6066884/
Abstract

The field of pharmacogenomics seeks to understand how an individual's unique gene sequence can affect their response to certain drugs. It is particularly relevant in anesthesia when the interindividual response to pain medication is essential. Codeine and tramadol are prodrugs metabolized by CYP2D6, polymorphisms of which can cause dangerous or even fatal levels of their metabolites, or decrease the level of metabolites to decrease their analgesic effect. Many other opioids are metabolized by CYP2D6 or CYP3A5, of which loss-of-function variants can cause dangerous levels of these drugs. The OCT1 transporter facilitates the movement of drugs into hepatocytes for metabolism, and variants of this transporter can increase serum levels of morphine and O-desmethyltramadol. Many NSAIDs are metabolized by CYP2C9, and there is concern that variants of this enzyme may lead to high serum levels of these drugs, causing gastrointestinal bleeding, however the data does not strongly support this. The gene encodes for P-glycoprotein which facilitates efflux of opioids away from their target receptors. The C3435T SNP may increase the concentration of opioids at target receptors, although the data is not conclusive. Catechol-O-Methyltransferase (COMT) is shown to indirectly upregulate opioid receptors. Certain haplotypes of COMT have been demonstrated to have an effect on opioid requirements. The gene codes for the mu-opioid receptor, and there is conflicting data regarding its effect on analgesia and opioid requirements. Overall, there is a fair amount of conflicting data in the above topics, suggesting that there is still a lot of research to be done on these topics, and that pain perception is multifactorial, likely including many common genetic variants.

摘要

药物基因组学领域旨在了解个体独特的基因序列如何影响其对某些药物的反应。这在麻醉领域尤为重要,因为个体对止痛药物的反应至关重要。可待因和曲马多是由CYP2D6代谢的前体药物,其多态性可导致其代谢产物达到危险甚至致命水平,或降低代谢产物水平以减弱其镇痛效果。许多其他阿片类药物由CYP2D6或CYP3A5代谢,其功能缺失变异可导致这些药物达到危险水平。OCT1转运蛋白促进药物进入肝细胞进行代谢,该转运蛋白的变异可提高吗啡和O-去甲基曲马多的血清水平。许多非甾体抗炎药由CYP2C9代谢,有人担心该酶的变异可能导致这些药物的血清水平升高,从而引起胃肠道出血,然而数据并不强烈支持这一点。该基因编码P-糖蛋白,它促进阿片类药物从其靶受体流出。C3435T单核苷酸多态性可能会增加阿片类药物在靶受体处的浓度,尽管数据尚无定论。儿茶酚-O-甲基转移酶(COMT)被证明可间接上调阿片受体。已证明COMT的某些单倍型对阿片类药物的需求量有影响。该基因编码μ-阿片受体,关于其对镇痛和阿片类药物需求量的影响,数据存在矛盾。总体而言,上述主题存在相当多相互矛盾的数据,这表明在这些主题上仍有大量研究要做,而且疼痛感知是多因素的,可能包括许多常见的基因变异。

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Single-nucleotide polymorphism C3435T in the ABCB1 gene is associated with opioid consumption in postoperative pain.单核苷酸多态性 C3435T 位于 ABCB1 基因中,与术后疼痛的阿片类药物消耗有关。
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