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药剂师主导的药物评估考虑了药物基因组学和药物诱导表型转化在治疗多种合并症中的应用:一例报告。

Pharmacist-Led Medication Evaluation Considering Pharmacogenomics and Drug-Induced Phenoconversion in the Treatment of Multiple Comorbidities: A Case Report.

机构信息

Office of Translational Research and Residency Programs, Tabula Rasa HealthCare, Moorestown, NJ 08057, USA.

Precision Pharmacotherapy Research & Development Institute, Tabula Rasa HealthCare, Orlando, FL 32827, USA.

出版信息

Medicina (Kaunas). 2021 Sep 10;57(9):955. doi: 10.3390/medicina57090955.

Abstract

Pharmacogenomic (PGx) information can guide drug and dose selection, optimize therapy outcomes, and/or decrease the risk of adverse drug events (ADEs). This report demonstrates the impact of a pharmacist-led medication evaluation, with PGx assisted by a clinical decision support system (CDSS), of a patient with multiple comorbidities. Following several sub-optimal pharmacotherapy attempts, PGx testing was recommended. The results were integrated into the CDSS, which supported the identification of clinically significant drug-drug, drug-gene, and drug-drug-gene interactions that led to the phenoconversion of cytochrome P450. The pharmacist evaluated PGx results, concomitant medications, and patient-specific factors to address medication-related problems. The results identified the patient as a CYP2D6 intermediate metabolizer (IM). Duloxetine-mediated competitive inhibition of CYP2D6 resulted in phenoconversion, whereby the patient's CYP2D6 phenotype was converted from IM to poor metabolizer for CYP2D6 co-medication. The medication risk score suggested a high risk of ADEs. Recommendations that accounted for PGx and drug-induced phenoconversion were accepted. After 1.5 months, therapy changes led to improved pain control, depression status, and quality of life, as well as increased heart rate, evidenced by patient-reported improved sleep patterns, movement, and cognition. This case highlights the pharmacist's role in using PGx testing and a CDSS to identify and mitigate medication-related problems to optimize medication regimen and medication safety.

摘要

药物基因组学(PGx)信息可以指导药物和剂量选择、优化治疗效果,和/或降低不良药物事件(ADEs)的风险。本报告展示了在临床决策支持系统(CDSS)辅助下,由药剂师主导的药物评估对一名患有多种合并症的患者的影响。在多次不理想的药物治疗尝试后,建议进行 PGx 检测。结果被整合到 CDSS 中,以支持识别临床上显著的药物-药物、药物-基因和药物-药物-基因相互作用,从而导致细胞色素 P450 的表型转化。药剂师评估了 PGx 结果、伴随用药和患者特定因素,以解决与药物相关的问题。结果确定患者为 CYP2D6 中间代谢物(IM)。度洛西汀介导的 CYP2D6 竞争性抑制导致表型转化,使患者的 CYP2D6 表型从 IM 转化为 CYP2D6 共用药的弱代谢者。药物风险评分提示 ADEs 的风险很高。考虑到 PGx 和药物诱导的表型转化的建议被接受。在 1.5 个月后,治疗方案的改变导致疼痛控制、抑郁状态和生活质量的改善,以及心率的增加,这可以从患者报告的睡眠模式、活动和认知的改善中得到证明。本病例突出了药剂师在使用 PGx 测试和 CDSS 来识别和减轻与药物相关的问题,以优化药物治疗方案和药物安全性方面的作用。

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