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阿片类镇痛中的药物基因组学考量

Pharmacogenomic considerations in opioid analgesia.

作者信息

Vuilleumier Pascal H, Stamer Ulrike M, Landau Ruth

机构信息

Klinik für Anästhesiologie und Schmerztherapie, Inselspital Universität Bern, Switzerland;

出版信息

Pharmgenomics Pers Med. 2012;5:73-87. doi: 10.2147/PGPM.S23422. Epub 2012 Aug 23.

Abstract

Translating pharmacogenetics to clinical practice has been particularly challenging in the context of pain, due to the complexity of this multifaceted phenotype and the overall subjective nature of pain perception and response to analgesia. Overall, numerous genes involved with the pharmacokinetics and dynamics of opioids response are candidate genes in the context of opioid analgesia. The clinical relevance of CYP2D6 genotyping to predict analgesic outcomes is still relatively unknown; the two extremes in CYP2D6 genotype (ultrarapid and poor metabolism) seem to predict pain response and/or adverse effects. Overall, the level of evidence linking genetic variability (CYP2D6 and CYP3A4) to oxycodone response and phenotype (altered biotransformation of oxycodone into oxymorphone and overall clearance of oxycodone and oxymorphone) is strong; however, there has been no randomized clinical trial on the benefits of genetic testing prior to oxycodone therapy. On the other hand, predicting the analgesic response to morphine based on pharmacogenetic testing is more complex; though there was hope that simple genetic testing would allow tailoring morphine doses to provide optimal analgesia, this is unlikely to occur. A variety of polymorphisms clearly influence pain perception and behavior in response to pain. However, the response to analgesics also differs depending on the pain modality and the potential for repeated noxious stimuli, the opioid prescribed, and even its route of administration.

摘要

由于疼痛这种多方面表型的复杂性以及疼痛感知和镇痛反应的整体主观性,将药物遗传学转化为临床实践在疼痛领域尤其具有挑战性。总体而言,众多参与阿片类药物反应药代动力学和药效学的基因是阿片类镇痛背景下的候选基因。CYP2D6基因分型预测镇痛效果的临床相关性仍相对未知;CYP2D6基因型的两个极端情况(超快代谢和慢代谢)似乎能预测疼痛反应和/或不良反应。总体而言,将基因变异性(CYP2D6和CYP3A4)与羟考酮反应及表型(羟考酮向吗啡酮的生物转化改变以及羟考酮和吗啡酮的总体清除率)联系起来的证据水平很强;然而,尚无关于羟考酮治疗前基因检测益处的随机临床试验。另一方面,基于药物遗传学检测预测对吗啡的镇痛反应更为复杂;尽管曾希望简单的基因检测能使吗啡剂量个体化以提供最佳镇痛效果,但这不太可能实现。多种多态性明显影响对疼痛的感知和行为反应。然而,对镇痛药的反应也因疼痛类型、反复有害刺激的可能性、所开阿片类药物甚至其给药途径而异。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3e97/3513230/ed99d2bf3c23/pgpm-5-073f1.jpg

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