Food and Drug Administration, Center for Drug Evaluation and Research, Office of Surveillance and Epidemiology, Department of Epidemiology, Silver Spring, MD, USA.
BMJ. 2013 Nov 5;347:f6320. doi: 10.1136/bmj.f6320.
To characterize risk of hypotension requiring admission to hospital in middle aged and older men treated with tamsulosin for benign prostatic hyperplasia.
Population based retrospective cohort study (between patient methodology) and self controlled case series (within patient methodology).
Healthcare claims data from the IMS Lifelink database in the United States.
Men aged 40-85 years with private US healthcare insurance entering the cohort at their first dispensing for tamsulosin or for a 5α reductase inhibitor (5ARI) between January 2001 and June 2011 after a minimum of six months' enrolment.
Hypotension requiring admission to hospital. Cox proportional hazards models estimated rate ratios at time varying intervals during follow-up: weeks 1-4, 5-8, and 9-12 after tamsulosin initiation; weeks 1-4, 5-8, and 9-12 after restarting tamsulosin (after a four week gap); and maintenance tamsulosin treatment (remaining exposed person time). Covariates included age, calendar year, demographics, antihypertensive use, healthcare use, and a Charlson comorbidity score. A self controlled case series, having implicit control for time invariant covariates, was additionally conducted.
Among 383,567 new users of study drugs (tamsulosin 297,596; 5ARI 85,971), 2562 admissions to hospital for severe hypotension were identified. The incidence for hypotension was higher for tamsulosin (42.4 events per 10,000 person years) than for 5ARIs (31.3 events per 10,000 person years) or all accrued person time (29.1 events per 10,000 person years). After tamsulosin initiation, the cohort analysis identified an increased rate of hypotension during weeks 1-4 (rate ratio 2.12 (95% confidence interval 1.29 to 3.04)) and 5-8 (1.51 (1.04 to 2.18)), and no significant increase at weeks 9-12. The rate ratio for hypotension also increased at weeks 1-4 (1.84 (1.46 to 2.33)) and 5-8 (1.85 (1.45 to 2.36)) after restarting tamsulosin, as did maintenance tamsulosin treatment (1.19 (1.07 to 1.32)). The self controlled case series gave similar results as the cohort analysis.
We observed a temporal association between tamsulosin use for benign prostatic hyperplasia and severe hypotension during the first eight weeks after initiating treatment and the first eight weeks after restarting treatment. This association suggests that physicians should focus on improving counseling strategies to warn patients regarding the "first dose phenomenon" with tamsulosin.
描述接受坦索罗辛治疗的中老年男性良性前列腺增生症患者发生需要住院的低血压风险。
基于人群的回顾性队列研究(患者间方法)和自我对照病例系列研究(患者内方法)。
美国 IMS Lifelink 数据库中的医疗保健索赔数据。
年龄在 40-85 岁之间、有私人医疗保险的美国男性,在 2001 年 1 月至 2011 年 6 月期间首次开出坦索罗辛或 5α 还原酶抑制剂(5ARI)处方后进入队列,至少有 6 个月的入组时间。
需要住院治疗的低血压。在随访期间的时间变化间隔内,Cox 比例风险模型估计了率比:坦索罗辛开始后第 1-4 周、第 5-8 周和第 9-12 周;坦索罗辛重新开始治疗(4 周间隔后)的第 1-4 周、第 5-8 周和第 9-12 周;维持坦索罗辛治疗(剩余暴露的人时)。协变量包括年龄、日历年度、人口统计学、抗高血压药物使用、医疗保健使用和 Charlson 合并症评分。还进行了具有内在时间不变协变量控制的自我对照病例系列研究。
在 383567 名新使用研究药物的患者(坦索罗辛 297596 例;5ARI 85971 例)中,有 2562 例因严重低血压住院。坦索罗辛(每 10000 人年 42.4 例事件)的低血压发生率高于 5ARI(每 10000 人年 31.3 例事件)或所有累积的人时(每 10000 人年 29.1 例事件)。在坦索罗辛开始治疗后,队列分析发现第 1-4 周(比值比 2.12(95%置信区间 1.29 至 3.04))和第 5-8 周(1.51(1.04 至 2.18))期间低血压的发生率增加,而第 9-12 周无显著增加。在重新开始坦索罗辛治疗后,第 1-4 周(比值比 1.84(1.46 至 2.33))和第 5-8 周(1.85(1.45 至 2.36))期间低血压的发生率也增加,维持坦索罗辛治疗时(比值比 1.19(1.07 至 1.32))也增加。自我对照病例系列研究给出了与队列分析相似的结果。
我们观察到坦索罗辛治疗良性前列腺增生症与治疗开始后前 8 周和重新开始治疗后前 8 周之间严重低血压之间存在时间关联。这种关联表明,医生应专注于改进咨询策略,警告患者坦索罗辛的“首剂量现象”。
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