Effects of pharmacogenetic profiles on pediatric pain relief and adverse events with ibuprofen and oxycodone.

IF 3.4 Q2 NEUROSCIENCES Pain Reports Pub Date : 2023-10-17 eCollection Date: 2023-12-01 DOI:10.1097/PR9.0000000000001113
Samina Ali, Aran Yukseloglu, Colin J Ross, Rhonda J Rosychuk, Amy L Drendel, Robin Manaloor, David W Johnson, Sylvie Le May, Bruce Carleton
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Abstract

Introduction: Individual genetic variation may influence clinical effects for pain medications. Effects of CYP2C9, CYP3A4, and CYP2D6 polymorphisms on clinical effectiveness and safety for ibuprofen and oxycodone were studied.

Objective: Primary objectives were to AU2 evaluate if allelic variations would affect clinical effectiveness and adverse events (AEs) occurrence.

Methods: This pragmatic prospective, observational cohort included children aged 4 to 16 years who were seen in a pediatric emergency department with an acute fracture and prescribed ibuprofen or oxycodone for at-home pain management. Saliva samples were obtained for genotyping of allelic variants, and daily telephone follow-up was conducted for 3 days. Pain was measured using the Faces Pain Scale-Revised.

Results: We included 210 children (n = 140 ibuprofen and n = 70 oxycodone); mean age was 11.1 (±SD 3.5) years, 33.8% were female. Median pain reduction on day 1 was similar between groups [ibuprofen 4 (IQR 2,4) and oxycodone 4 (IQR 2,6), P = 0.69]. Over the 3 days, the oxycodone group experienced more AE than the ibuprofen group (78.3% vs 53.2%, P < 0.001). Those with a CYP2C9*2 reduced function allele experienced less adverse events with ibuprofen compared with those with a normal functioning allele CYP2C9*1 (P = 0.003). Neither CYP3A4 variants nor CYP2D6 phenotype classification affected clinical effect or AE.

Conclusion: Although pain relief was similar, children receiving oxycodone experienced more AE, overall, than those receiving ibuprofen. For children receiving ibuprofen or oxycodone, pain relief was not affected by genetic variations in CYP2C9 or CYP3A4/CYP2D6, respectively. For children receiving ibuprofen, the presence of CYP2C9*2 was associated with less adverse events.

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布洛芬和羟考酮对儿童疼痛缓解和不良事件的药理学影响。
个体遗传变异可能影响止痛药的临床效果。研究CYP2C9、CYP3A4和CYP2D6多态性对布洛芬和羟考酮临床疗效和安全性的影响。目的:主要目的是AU2评估等位基因变异是否会影响临床疗效和不良事件(ae)的发生。方法:这个实用的前瞻性观察队列包括4至16岁的儿童,他们在儿科急诊科就诊,患有急性骨折,并处方布洛芬或羟考酮用于家庭疼痛管理。采集唾液样本进行等位变异基因分型,每天电话随访3天。疼痛测量采用面部疼痛量表-修订。结果:纳入210名儿童(n = 140布洛芬,n = 70羟考酮);平均年龄11.1(±SD 3.5)岁,女性占33.8%。第1天,两组间疼痛减轻的中位数相似[布洛芬4 (IQR 2,4)和羟考酮4 (IQR 2,6), P = 0.69]。3 d内,羟考酮组AE发生率高于布洛芬组(78.3% vs 53.2%, P < 0.001)。与功能正常的CYP2C9*1等位基因相比,CYP2C9*2功能降低的患者使用布洛芬的不良事件较少(P = 0.003)。CYP3A4变异和CYP2D6表型分型均不影响临床疗效或AE。结论:虽然疼痛缓解相似,但总体而言,接受羟考酮治疗的儿童比接受布洛芬治疗的儿童发生更多的AE。对于接受布洛芬或羟考酮治疗的儿童,疼痛缓解不受CYP2C9或CYP3A4/CYP2D6基因变异的影响。对于接受布洛芬治疗的儿童,CYP2C9*2的存在与较少的不良事件相关。
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来源期刊
Pain Reports
Pain Reports Medicine-Anesthesiology and Pain Medicine
CiteScore
7.50
自引率
2.10%
发文量
93
审稿时长
8 weeks
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