利用真实世界的药物使用情况和基因型数据评估药物基因检测的价值。

IF 6.3 2区 医学 Q1 PHARMACOLOGY & PHARMACY
Kaisa Litonius, Noora Kulla, Petra Falkenbach, Kati Kristiansson, E Katriina Tarkiainen, Liisa Ukkola-Vuoti, Kristiina Cajanus, Mari Korhonen, Sofia Khan, Johanna Sistonen, Arto Orpana, Mats Lindstedt, Tommi Nyrönen, Markus Perola, Miia Turpeinen, Ville Kytö, Aleksi Tornio, Mikko Niemi
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引用次数: 0

摘要

药物基因检测在临床治疗中的应用一直进展缓慢,除少数例外情况外,还因缺乏关于如何最有针对性地进行检测的实际证据而受到阻碍。在这项以登记为基础的回顾性研究中,我们分析了全国范围内 142.5 万名内科或外科病房出院患者的队列以及 2178 名大学医院患者的队列,了解他们购买和开具药物遗传学可操作性药物处方的情况。药物基因变异是从大学医院患者子集(n = 930)的全基因组基因型数据中获得的。我们调查了与接受药物遗传学可操作性药物相关的因素,并开发了一个基于文献的先期药物遗传学面板检测成本效益模型。在为期 2 年的随访中,全国范围内有 60.4% 的患者至少购买了一种药物基因作用药物,其中最常见的是布洛芬(25.0%)和可待因(19.4%)。在基因分型子群中,98.8%的人携带至少一种可操作的药物基因型,23.3%的人拥有至少一对可操作的基因-药物配对。患有肌肉骨骼或心血管疾病的患者在住院期间更容易接受可作用的药物。成本效益模型包括大学医院队列中的常用药物,包括昂丹司琼(19.4%)、辛伐他汀(7.4%)、氯吡格雷(5.0%)、华法林(5.1%)、(ES)西酞普兰(5.3%)和硫唑嘌呤(0.5%)。如果对所有大学医院的患者进行无针对性的先期药物基因检测,模型显示,在不考虑检测成本的情况下,2 年内每位患者可节省 17.49 欧元的直接医疗系统成本。因此,针对最有可能接受药物遗传学可操作性药物的患者群体进行先期药物遗传学检测可能是合理的。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Value of Pharmacogenetic Testing Assessed with Real-World Drug Utilization and Genotype Data.

Implementation of pharmacogenetic testing in clinical care has been slow and with few exceptions is hindered by the lack of real-world evidence on how to best target testing. In this retrospective register-based study, we analyzed a nationwide cohort of 1,425,000 patients discharged from internal medicine or surgical wards and a cohort of 2,178 university hospital patients for purchases and prescriptions of pharmacogenetically actionable drugs. Pharmacogenetic variants were obtained from whole genome genotype data for a subset (n = 930) of the university hospital patients. We investigated factors associated with receiving pharmacogenetically actionable drugs and developed a literature-based cost-benefit model for pre-emptive pharmacogenetic panel testing. In a 2-year follow-up, 60.4% of the patients in the nationwide cohort purchased at least one pharmacogenetically actionable drug, most commonly ibuprofen (25.0%) and codeine (19.4%). Of the genotyped subset, 98.8% carried at least one actionable pharmacogenetic genotype and 23.3% had at least one actionable gene-drug pair. Patients suffering from musculoskeletal or cardiovascular diseases were more prone to receive pharmacogenetically actionable drugs during inpatient episode. The cost-benefit model included frequently dispensed drugs in the university hospital cohort, comprising ondansetron (19.4%), simvastatin (7.4%), clopidogrel (5.0%), warfarin (5.1%), (es)citalopram (5.3%), and azathioprine (0.5%). For untargeted pre-emptive pharmacogenetic testing of all university hospital patients, the model indicated saving €17.49 in direct healthcare system costs per patient in 2 years without accounting for the cost of the test itself. Therefore, it might be reasonable to target pre-emptive pharmacogenetic testing to patient groups most likely to receive pharmacogenetically actionable drugs.

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来源期刊
CiteScore
12.70
自引率
7.50%
发文量
290
审稿时长
2 months
期刊介绍: Clinical Pharmacology & Therapeutics (CPT) is the authoritative cross-disciplinary journal in experimental and clinical medicine devoted to publishing advances in the nature, action, efficacy, and evaluation of therapeutics. CPT welcomes original Articles in the emerging areas of translational, predictive and personalized medicine; new therapeutic modalities including gene and cell therapies; pharmacogenomics, proteomics and metabolomics; bioinformation and applied systems biology complementing areas of pharmacokinetics and pharmacodynamics, human investigation and clinical trials, pharmacovigilence, pharmacoepidemiology, pharmacometrics, and population pharmacology.
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