Assessing the clinical impact of CYP2C9 pharmacogenetic variation on phenytoin prescribing practice and patient response in an integrated health system

Fohner Alison E.; Ranatunga Dilrini K.; Thai Khanh K.; Lawson Brian L.; Risch Neil; Oni-Orisan Akinyemi; Jelalian Aline T.; Rettie Allan E.; Liu Vincent X.; Schaefer Catherine A.

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Assessing the clinical impact of CYP2C9 pharmacogenetic variation on phenytoin prescribing practice and patient response in an integrated health system

机译：评估CYP2C9药物发生变化对综合卫生系统苯妥林苯妥的临床影响

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Objective To assess the impact of CYP2C9 variation on phenytoin patient response and clinician prescribing practice where genotype was unknown during treatment. Methods A retrospective analysis of Resource on Genetic Epidemiology Research on Adult Health and Aging cohort participants who filled a phenytoin prescription between 1996 and 2017. We used laboratory test results, medication dispensing records, and medical notes to identify associations of CYP2C9 genotype with phenytoin blood concentration, neurologic side effects, and medication dispensing patterns reflecting clinician prescribing practice and patient response. Results Among 993 participants, we identified 69% extensive, 20% high-intermediate, 10% low-intermediate, and 2% poor metabolizers based on CYP2C9 genotypes. Compared with extensive metabolizer genotype, low-intermediate/poor metabolizer genotype was associated with increased dose-adjusted phenytoin blood concentration [21.3 pg/mL, 95% confidence interval (CI): 13.6-29.0 pg/mL; P < 0.01] and increased risk of neurologic side effects (hazard ratio: 2.40, 95% CI: 1.24-4.64; P < 0.01). Decreased function CYP2C9 genotypes were associated with medication dispensing patterns indicating dose decrease, use of alternative anticonvulsants, and worse adherence, although these associations varied by treatment indication for phenytoin. Conclusion CYP2C9 variation was associated with clinically meaningful differences in clinician prescribing practice and patient response, with potential implications for healthcare utilization and treatment efficacy.

机译：目的评估CYP2C9变异对苯妥林患者反应和临床医生处方实践的影响，在治疗过程中未知。方法方法对成人健康和老化群体遗传流行病学资源研究的回顾性分析1996年至2017年之间的苯妥林素处方。我们使用实验室测试结果，药物分配记录和医疗说明，以鉴定CYP2C9基因型与苯妥林血液浓度的关联，神经系统副作用和药物分配模式反映了临床医生的处方实践和患者反应。结果在993名参与者之间，我们确定了69％的广泛，高中中间体，10％的低中间剂，10％，基于CYP2C9基因型为2％的代谢剂。与广泛的代谢物基因型相比，低中间/差的代谢物基因型与增加剂量调节的苯毒素血液浓度有关[21.3 pg / ml，95％置信区间（CI）：13.6-29.0 pg / ml; P <0.01]和神经系统副作用的风险增加（危险比：2.40,95％CI：1.24-4.64; P <0.01）。减少的功能CYP2C9基因型与指示剂量减少，使用替代抗刺抑制的药物分配模式以及较差的粘附性，尽管这些关联因苯妥汀的治疗指示而变化而差。结论CYP2C9变异与临床有意义的临床有意义的差异有关，临床医生规定实践和患者应答，对医疗保健利用和治疗疗效的潜在影响。

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《Pharmacogenetics and genomics》 |2019年第8期|共8页
作者
Fohner Alison E.; Ranatunga Dilrini K.; Thai Khanh K.; Lawson Brian L.; Risch Neil; Oni-Orisan Akinyemi; Jelalian Aline T.; Rettie Allan E.; Liu Vincent X.; Schaefer Catherine A.;
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作者单位

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

Univ Calif San Francisco Inst Human Genet San Francisco CA 94143 USA;

Univ Calif San Francisco Inst Human Genet San Francisco CA 94143 USA;

Kaiser Permanente Northern Calif Dept Neurol Walnut Creek CA USA;

Univ Washington Dept Med Chem Seattle WA 98195 USA;

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

Kaiser Permanente Northern Calif Div Res Oakland CA USA;

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正文语种 eng
中图分类药学;
关键词
adherence; anticonvulsant; dilantin; electronic health record; pharmacogenetics; precision medicine; prescribing; seizure;

机译：依恋;抗惊厥;稀释剂;电子健康记录;药物生物植物;精密药;处方;癫痫发作;

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1. Assessing the clinical impact of CYP2C9 pharmacogenetic variation on phenytoin prescribing practice and patient response in an integrated health system [J] . Fohner Alison E., Ranatunga Dilrini K., Thai Khanh K., Pharmacogenetics and genomics . 2019,第8期

机译：评估CYP2C9药物发生变化对综合卫生系统苯妥林苯妥的临床影响
2. Baseline Variation in Use of VA/DOD Clinical Practice Guideline Recommended Opioid Prescribing Practices Across VA Health Care Systems [J] . Buscaglia Alexander C., Paik Meenah C., Lewis Eleanor, The clinical journal of pain . 2015,第9期

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3. Clinical pharmacogenetics implementation consortium guidelines for CYP2C9 and HLA-B genotypes and phenytoin dosing [J] . CaudleK.E., RettieA.E., Whirl-CarrilloM., Clinical Pharmacology and Therapeutics . 2014,第5期

机译：CYP2C9和HLA-B基因型和苯妥英钠剂量的临床药物遗传学实施联合指南
4. Development of Gastric Retained System for Losartan and its Clinical Relevance in HealthyVolunteers with CYP2C9 Polymorphism [C] . Ray Ray-Neng Chen, Chiao-Ya Yu, Hsiu-O Ho, Annual meeting exposition of the Controlled Release Society . 2009

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6. Clinical Pharmacogenetics Implementation Consortium Guidelines for CYP2C9 and HLA‐B Genotypes and Phenytoin Dosing [O] . K E Caudle, A E Rettie, M Whirl‐Carrillo, -1

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Assessing the clinical impact of CYP2C9 pharmacogenetic variation on phenytoin prescribing practice and patient response in an integrated health system

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