Chronic Pain Management in a CYP2D6 Poor Metabolizer: A Case Report for Oxycodone.

Q2 Medicine
Deepa Pednekar, Joshua Russell, Chandni Bardolia, David Thacker, Nishita Shah Amin
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引用次数: 0

Abstract

The objective of this case report is to illustrate pharmacogenomics (PGx)-guided oxycodone treatment, given the conflicting data on the analgesic response from oxycodone in Cytochrome P450 (CYP)2D6 poor metabolizers (PMs). PGx-guided therapy can help improve treatment outcomes. This case report describes a 58-year-old patient who was prescribed oxycodone for chronic pain management. The patient presented with a history of inadequate pain control despite analgesic treatment with oxycodone (morphine milliequivalent [MME] = 22.5). Pharmacogenetic testing revealed that the patient was a CYP2D6 Poor Metabolizer (PM), which may shed light on the observed lack of analgesic response to oxycodone. The clinical pharmacist recommended switching to an alternative opioid not metabolized via the CYP2D6 pathway. The patient was subsequently switched to hydromorphone (MME = 16), resulting in improved pain control and fewer side effects. The newer hydromorphone dose accounted for a 30% MME dose reduction. The patient's initial average and worst pain score were 7 and 9 out of 10, respectively, per the numeric rating scale (NRS). Upon follow-up with the patient in two weeks, her average and worst pain scores improved to 3 and 3.5 out of 10, respectively, per the NRS. Further PGx testing results led to an overall positive outcome, such as her willingness to participate in physical therapy as a result of improved pain scores. This case highlights the importance of considering individual variability in drug metabolism when prescribing medications, particularly opioids such as oxycodone, to ensure optimal therapeutic outcomes and minimize the risk of adverse events in CYP2D6 PMs.

CYP2D6 代谢不良者的慢性疼痛治疗:关于羟考酮的病例报告。
本病例报告旨在说明药物基因组学(PGx)指导下的羟考酮治疗,因为细胞色素 P450 (CYP)2D6 代谢不良者(PMs)对羟考酮的镇痛反应存在相互矛盾的数据。PGx 指导疗法有助于改善治疗效果。本病例报告描述了一名 58 岁患者因慢性疼痛治疗而被处方羟考酮。尽管使用羟考酮(吗啡毫当量 [MME] = 22.5)进行了镇痛治疗,但患者仍有疼痛控制不佳的病史。药物基因检测显示,该患者属于 CYP2D6 代谢不良者(PM),这可能与观察到的对羟考酮缺乏镇痛反应有关。临床药剂师建议患者改用其他不通过 CYP2D6 途径代谢的阿片类药物。患者随后改用氢吗啡酮(MME = 16),结果疼痛控制得到改善,副作用也减少了。新的氢吗啡酮剂量使 MME 剂量减少了 30%。根据数字评分量表(NRS),患者最初的平均和最严重疼痛评分分别为 7 分和 9 分(满分 10 分)。两周后对患者进行随访时,根据 NRS,她的平均和最严重疼痛评分分别降至 3 分和 3.5 分(满分 10 分)。进一步的 PGx 测试结果带来了积极的整体结果,例如,由于疼痛评分的改善,她愿意参加物理治疗。本病例强调了在开具处方时考虑药物代谢个体差异的重要性,尤其是阿片类药物,如羟考酮,以确保最佳治疗效果,并将 CYP2D6 PMs 的不良事件风险降至最低。
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
Senior Care Pharmacist
Senior Care Pharmacist PHARMACOLOGY & PHARMACY-
CiteScore
1.30
自引率
0.00%
发文量
160
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