居住在社区的老年人群中的药物相互作用及其与不良健康后果的关系：一项前瞻性队列研究

IF 2.9 3区医学 Q2 PHARMACOLOGY & PHARMACY

Clinical Drug Investigation Pub Date : 2024-06-01 Epub Date: 2024-06-15 DOI:10.1007/s40261-024-01369-9

John E Hughes, Kathleen E Bennett, Caitriona Cahir

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引用次数: 0

摘要

背景：在社区居住的老年人群中，有关药物相互作用（DDI）与健康结果之间关系的证据非常有限：我们估算了爱尔兰社区老年人群中可能具有重要临床意义的 DDI 发生率，并研究了 DDI 与（1）药物不良事件（ADE）、（2）急诊就医率和（3）与健康相关的生活质量（HRQoL）之间的关联：这是一项前瞻性队列研究，研究对象是爱尔兰 15 家全科诊所 2010 年招募的年龄≥ 70 岁的社区老年人（N = 904）（第 1 波），并利用相关的全国药房报销数据对其进行了为期 2 年的跟踪调查（第 2 波，2012-2013 年）。其中包括配发两种或两种以上药物的个人（第 1 波：N = 842；第 2 波：N = 763）。对基线、随访和每项健康结果前 6 个月的 DDI 患病率进行了估算。采用多层次回归法建立 DDI 暴露与随访健康结果之间的关联模型。报告了DDI流行率、调整后发病率比（aIRR）、调整后几率比（aOR）、β系数和多级回归分析得出的稳健标准误差（RSE）以及95%置信区间（CIs）：在第一阶段，196 人（23.3% [95% CI 20.5-26.3]）可能暴露于≥ 1 个 DDI，在第二阶段增加到 345 人（45.2% [41.7-48.9]）。随访 2 年时，ADE 中位数为 3（四分位数间距 [IQR 2-5]）；229 人（30.1%）≥ 1 次急诊就医，平均 EQ-5D 为 0.74 (± 0.23)。在随访中，DDI暴露与急诊就医之间的关联缺乏证据（aOR = 1.38 [0.42-4.53]）。DDI暴露与ADEs数量增加（aIRR = 1.26 [1.03-1.55]）和EQ-5D效用下降（β = - 0.07, [-0.11 to -0.04]，RSE = 0.02）有关。阿司匹林-华法林、克拉霉素-强的松龙、胺碘酮-呋塞米、克拉霉素-沙丁胺醇、罗伐他汀-华法林、胺碘酮-比索洛尔和阿司匹林-尼可地尔是这些健康结果发生前6个月常见的DDI：我们发现，在第 1 波和第 2 波之间，DDI 发生率增加了两倍。DDI暴露与ADEs的增加和2年随访时HRQoL的下降有关。常见的DDI涉及抗凝剂、心血管药物和抗菌药物，应针对这些药物进行优化。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

Drug-Drug Interactions and Their Association with Adverse Health Outcomes in the Older Community-Dwelling Population: A Prospective Cohort Study.

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Drug-Drug Interactions and Their Association with Adverse Health Outcomes in the Older Community-Dwelling Population: A Prospective Cohort Study.

Background: Evidence on associations between drug-drug interactions (DDIs) and health outcomes in the older community-dwelling population is limited.

Objective: We estimate potentially clinically important DDI prevalence and examine the association between DDIs and (1) adverse drug events (ADEs), (2) emergency hospital attendance and (3) health-related quality of life (HRQoL) in an older community-dwelling population in Ireland.

Methods: This is a prospective cohort study of community-dwelling older adults (N = 904) aged ≥ 70 years from 15 general practices in Ireland recruited in 2010 (wave-1) and followed-up over 2 years (wave-2; 2012-2013), with linked national pharmacy claims data. Individuals dispensed two or more drugs (wave-1: N = 842; wave-2: N = 763) were included. DDI prevalence at baseline, follow-up and 6 months prior to each health outcome was estimated. Multi-level regression was used to model the association between DDI-exposure and health outcomes at follow-up. DDI prevalence, adjusted incidence-rate ratios (aIRR), adjusted odds ratios (aOR), β coefficients and robust standard error (RSE) from multi-level regression analyses, and 95% confidence intervals (CIs) are reported.

Results: At wave-1, n = 196 (23.3% [95% CI 20.5-26.3]), individuals were potentially exposed to ≥ 1 DDI, increasing to n = 345 (45.2% [41.7-48.9]) at wave-2. At 2-year follow-up, the median number of ADEs was 3 (interquartile range [IQR 2-5]); 229 (30.1%) had ≥ 1 emergency hospital attendance, and the mean EQ-5D was 0.74 (± 0.23). Evidence for the association between DDI-exposure and emergency hospital attendance at follow-up was lacking (aOR = 1.38 [0.42-4.53]). DDI-exposure was associated with an increasing number of ADEs (aIRR = 1.26 [1.03-1.55]), and decreasing EQ-5D utility (β = - 0.07, [-0.11 to -0.04], RSE = 0.02). Aspirin-warfarin, clarithromycin-prednisolone, amiodarone-furosemide, clarithromycin-salbutamol, rosuvastatin-warfarin, amiodarone-bisoprolol, and aspirin-nicorandil were common DDIs 6 months preceding these health outcomes.

Conclusions: We found a two-fold increase in DDI prevalence between wave 1 and 2. DDI exposure was associated with increasing ADEs and declining HRQoL at 2-year follow-up. Common DDIs involved anticoagulants, cardiovascular and antimicrobial drugs, which should be targeted for medicine optimisation.

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来源期刊

Clinical Drug Investigation 医学-药学

CiteScore

5.90

自引率

3.10%

发文量

108

审稿时长

6-12 weeks

期刊介绍： Clinical Drug Investigation provides rapid publication of original research covering all phases of clinical drug development and therapeutic use of drugs. The Journal includes: -Clinical trials, outcomes research, clinical pharmacoeconomic studies and pharmacoepidemiology studies with a strong link to optimum prescribing practice for a drug or group of drugs. -Clinical pharmacodynamic and clinical pharmacokinetic studies with a strong link to clinical practice. -Pharmacodynamic and pharmacokinetic studies in healthy volunteers in which significant implications for clinical prescribing are discussed. -Studies focusing on the application of drug delivery technology in healthcare. -Short communications and case study reports that meet the above criteria will also be considered. Additional digital features (including animated abstracts, video abstracts, slide decks, audio slides, instructional videos, infographics, podcasts and animations) can be published with articles; these are designed to increase the visibility, readership and educational value of the journal’s content. In addition, articles published in Clinical Drug Investigation may be accompanied by plain language summaries to assist readers who have some knowledge, but non in-depth expertise in, the area to understand important medical advances.