住院老年人药物相互作用的检测和预防:基于细胞色素p450的新型软件的应用

Hubert Zakrzewski-Jakubiak BPharm, MSc , Julie Doan BPharm, MSc , Pamela Lamoureux BPharm , Dharmender Singh BPharm, MSc , Jacques Turgeon PhD , Cara Tannenbaum MD, MSc
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引用次数: 51

摘要

多药增加了基于细胞色素p450的药物-药物相互作用(cyp450 - ddi)的风险,导致治疗效果下降或药物毒性增加。目的探讨新型CYP450-DDI软件InterMED-Rx在协助药师检测老年住院患者CYP450-DDI中的作用,并确定药师对每一种CYP450-DDI如何干预的共识。方法一个老年药师共识小组首次建立了cyp450 - ddi临床相关药代动力学管理指南。一项前瞻性研究随后对新入住老年医院的患者进行了研究,这些患者的药物概况接受了InterMED-Rx的分析。记录干预的比率和类型。结果药师对如何管理cyp450 - ddi的共识初始仅为中等(Cohen’s κ, 0.51;95% CI, 0.39-0.62),但在审议后有所改善(Cohen’s κ, 0.79;95% ci, 0.70-0.88)。持续的分歧涉及对同一细胞色素具有相似亲和力的两种药物之间的相互作用。前瞻性研究招募了100名年龄82.3岁(65-96岁),平均(SD)为12.2(4.1)种药物(范围5 - 27)的多药(≥5种药物)患者。80%的患者使用InterMED-Rx检测到至少1种CYP450 DDI。共鉴定出238种cyp450 - ddi,涉及CYP3A4(70.2%)、CYP2D6(22.7%)和CYP2C9(3.4%)底物或抑制剂。19%的患者立即接受药物调整,39%的患者需要随访临床体征、症状和实验室检查,以确定是否需要未来的药物调整。在所有需要临床随访的患者中,超过一半(56%)在出院前进行了进一步的药物调整。结论使用InterMED-Rx软件识别存在药代动力学相互作用风险的老年患者,并促进旨在减少药物不良事件的干预。尽管在许多CYP450-DDI情况下,药剂师之间可以就如何干预达成共识,但某些情况允许多种干预策略。
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Detection and Prevention of Drug–Drug Interactions in the Hospitalized Elderly: Utility of New Cytochrome P450–Based Software

Background

Polypharmacy increases the risk of cytochrome P450–based drug–drug interactions (CYP450-DDIs), leading to decreased therapeutic efficacy or increased drug toxicity.

Objective

The aims of this study were to investigate the utility of a new CYP450-DDI software, InterMED-Rx, in aiding pharmacists in detecting CYP450-DDIs in hospitalized elderly patients and to ascertain pharmacists' agreement on how to intervene for each CYP450-DDI.

Methods

A consensus panel of geriatric pharmacists first established guidelines for managing clinically relevant pharmacokinetic CYP450-DDIs. A prospective study was then conducted of patients newly admitted to a geriatric hospital whose pharmaceutical profile underwent analysis with InterMED-Rx. Rates and types of interventions were recorded.

Results

Pharmacists' interrater agreement on how to manage CYP450-DDIs was initially only moderate (Cohen's κ, 0.51; 95% CI, 0.39–0.62), but improved subsequent to deliberation (Cohen's κ, 0.79; 95% CI, 0.70–0.88). Persistent disagreement involved interactions between 2 drugs with similar affinities for the same cytochrome. One hundred patients with polypharmacy (≥5 medications) aged 82.3 years (range, 65–96), with a mean (SD) of 12.2 (4.1) drugs (range, 5–27) were recruited for the prospective study. Eighty percent of patients had at least 1 CYP450 DDI detected with InterMED-Rx. A total of 238 CYP450-DDIs were identified involving CYP3A4 (70.2%), CYP2D6 (22.7%), and CYP2C9 (3.4%) substrates or inhibitors. Nineteen percent of patients received immediate medication adjustment, and 39% required follow-up of clinical signs, symptoms, and laboratory tests to determine whether future modification was needed. More than one half (56%) of all patients who required clinical follow-up had further medication adjustment prior to discharge.

Conclusions

Use of the InterMED-Rx software identified elderly patients at risk for pharmacokinetic interactions and facilitated interventions aimed at reducing adverse drug events. Although consensus can be reached among pharmacists on how to intervene for many CYP450-DDI scenarios, certain situations allow for multiple intervention strategies.

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来源期刊
American Journal Geriatric Pharmacotherapy
American Journal Geriatric Pharmacotherapy GERIATRICS & GERONTOLOGY-PHARMACOLOGY & PHARMACY
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