潜在不适当用药对中年患者多重用药相关死亡风险的影响:一项全国队列研究。
Contribution of Potentially Inappropriate Medications to Polypharmacy-Associated Risk of Mortality in Middle-Aged Patients: A National Cohort Study.
作者信息
Guillot Jordan, Justice Amy C, Gordon Kirsha S, Skanderson Melissa, Pariente Antoine, Bezin Julien, Rentsch Christopher T
机构信息
Veterans Aging Cohort Study Coordinating Center, VA Connecticut Healthcare System, West Haven, CT, 06516, USA.
Department of General Internal Medicine, Yale School of Medicine, New Haven, CT, 06511, USA.
出版信息
J Gen Intern Med. 2024 Dec;39(16):3261-3270. doi: 10.1007/s11606-024-08817-4. Epub 2024 Jun 3.
BACKGROUND
The role of potentially inappropriate medications (PIMs) in mortality has been studied among those 65 years or older. While middle-aged individuals are believed to be less susceptible to the harms of polypharmacy, PIMs have not been as carefully studied in this group.
OBJECTIVE
To estimate PIM-associated risk of mortality and evaluate the extent PIMs explain associations between polypharmacy and mortality in middle-aged patients, overall and by sex and race/ethnicity.
DESIGN
Observational cohort study.
SETTING
Department of Veterans Affairs (VA), the largest integrated healthcare system in the US.
PARTICIPANTS
Patients aged 41 to 64 who received a chronic medication (continuous use of ≥ 90 days) between October 1, 2008, and September 30, 2017.
MEASUREMENT
Patients were followed for 5 years until death or end of study period (September 30, 2019). Time-updated polypharmacy and hyperpolypharmacy were defined as 5-9 and ≥ 10 chronic medications, respectively. PIMs were identified using the Beers criteria (2015) and were time-updated. Cox models were adjusted for demographic, behavioral, and clinical characteristics.
RESULTS
Of 733,728 patients, 676,935 (92.3%) were men, 479,377 (65.3%) were White, and 156,092 (21.3%) were Black. By the end of follow-up, 104,361 (14.2%) patients had polypharmacy, 15,485 (2.1%) had hyperpolypharmacy, and 129,992 (17.7%) were dispensed ≥ 1 PIM. PIMs were independently associated with mortality (HR 1.11, 95% CI 1.04-1.18). PIMs also modestly attenuated risk of mortality associated with polypharmacy (HR 1.07, 95% CI 1.03-1.11 before versus HR 1.05, 95% CI 1.01-1.09 after) and hyperpolypharmacy (HR 1.18, 95% CI 1.09-1.28 before versus HR 1.12, 95% CI 1.03-1.22 after). Patterns varied when stratified by sex and race/ethnicity.
LIMITATIONS
The predominantly male VA patient population may not represent the general population.
CONCLUSION
PIMs were independently associated with increased mortality, and partially explained polypharmacy-associated mortality in middle-aged people. Other mechanisms of injury from polypharmacy should also be studied.
背景
已在65岁及以上人群中研究了潜在不适当用药(PIMs)在死亡率方面的作用。虽然人们认为中年个体对多重用药危害的易感性较低,但该群体中的PIMs尚未得到如此仔细的研究。
目的
评估与PIMs相关的死亡风险,并评估PIMs在多大程度上解释了中年患者中多重用药与死亡率之间的关联,总体情况以及按性别和种族/民族划分的情况。
设计
观察性队列研究。
设置
美国最大的综合医疗系统退伍军人事务部(VA)。
参与者
2008年10月1日至2017年9月30日期间接受慢性药物治疗(连续使用≥90天)的41至64岁患者。
测量
对患者进行5年随访,直至死亡或研究期结束(2019年9月30日)。时间更新的多重用药和超多重用药分别定义为使用5 - 9种和≥10种慢性药物。使用Beers标准(2015年)识别PIMs并进行时间更新。Cox模型针对人口统计学、行为和临床特征进行了调整。
结果
在733,728名患者中,676,935名(92.3%)为男性,479,377名(65.3%)为白人,156,092名(21.3%)为黑人。随访结束时,104,361名(14.2%)患者存在多重用药,15,485名(2.1%)患者存在超多重用药,129,992名(17.7%)患者被开具了≥1种PIM。PIMs与死亡率独立相关(风险比[HR] 1.11,95%置信区间[CI] 1.04 - 1.18)。PIMs也适度降低了与多重用药相关的死亡风险(之前HR 1.07,95% CI 1.03 - 1.11,之后HR 1.05,95% CI 1.01 - 1.09)和超多重用药相关的死亡风险(之前HR 1.18,95% CI 1.09 - 1.28,之后HR 1.12,95% CI 1.03 - 1.22)。按性别和种族/民族分层时模式有所不同。
局限性
主要为男性的VA患者群体可能不代表一般人群。
结论
PIMs与死亡率增加独立相关,并部分解释了中年人群中多重用药相关的死亡率。还应研究多重用药导致伤害的其他机制。
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