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吡格列酮与膀胱癌风险:一项多人群汇总的累积暴露分析。

Pioglitazone and bladder cancer risk: a multipopulation pooled, cumulative exposure analysis.

作者信息

Levin Daniel, Bell Samira, Sund Reijo, Hartikainen Sirpa A, Tuomilehto Jaakko, Pukkala Eero, Keskimäki Ilmo, Badrick Ellena, Renehan Andrew G, Buchan Iain E, Bowker Samantha L, Minhas-Sandhu Jasjeet K, Zafari Zafar, Marra Carlo, Johnson Jeffrey A, Stricker Bruno H, Uitterlinden Andrè G, Hofman Albert, Ruiter Rikje, de Keyser Catherine E, MacDonald Thomas M, Wild Sarah H, McKeigue Paul M, Colhoun Helen M

机构信息

Diabetes Epidemiology Group, Population Health Sciences, University of Dundee, Dundee, UK.

出版信息

Diabetologia. 2015 Mar;58(3):493-504. doi: 10.1007/s00125-014-3456-9. Epub 2014 Dec 7.

Abstract

AIMS/HYPOTHESIS: The evidence on the association between pioglitazone use and bladder cancer is contradictory, with many studies subject to allocation bias. The aim of our study was to examine the effect of exposure to pioglitazone on bladder cancer risk internationally across several cohorts. The potential for allocation bias was minimised by focusing on the cumulative effect of pioglitazone as the primary endpoint using a time-dependent approach.

METHODS

Prescription, cancer and mortality data from people with type 2 diabetes were obtained from six populations across the world (British Columbia, Finland, Manchester, Rotterdam, Scotland and the UK Clinical Practice Research Datalink). A discrete time failure analysis using Poisson regression was applied separately to data from each centre to model the effect of cumulative drug exposure on bladder cancer incidence, with time-dependent adjustment for ever use of pioglitazone. These were then pooled using fixed and random effects meta-regression.

RESULTS

Data were collated on 1.01 million persons over 5.9 million person-years. There were 3,248 cases of incident bladder cancer, with 117 exposed cases and a median follow-up duration of 4.0 to 7.4 years. Overall, there was no evidence for any association between cumulative exposure to pioglitazone and bladder cancer in men (rate ratio [RR] per 100 days of cumulative exposure, 1.01; 95% CI 0.97, 1.06) or women (RR 1.04; 95% CI 0.97, 1.11) after adjustment for age, calendar year, diabetes duration, smoking and any ever use of pioglitazone. No association was observed between rosiglitazone and bladder cancer in men (RR 1.01; 95% CI 0.98, 1.03) or women (RR 1.00; 95% CI 0.94, 1.07).

CONCLUSIONS/INTERPRETATION: The cumulative use of pioglitazone or rosiglitazone was not associated with the incidence of bladder cancer in this large, pooled multipopulation analysis.

摘要

目的/假设:关于使用吡格列酮与膀胱癌之间关联的证据相互矛盾,许多研究存在分配偏倚。我们研究的目的是在国际上多个队列中检验暴露于吡格列酮对膀胱癌风险的影响。通过采用时间依赖性方法,将吡格列酮的累积效应作为主要终点,从而将分配偏倚的可能性降至最低。

方法

从全球六个人群(不列颠哥伦比亚、芬兰、曼彻斯特、鹿特丹、苏格兰以及英国临床实践研究数据链)获取2型糖尿病患者的处方、癌症和死亡率数据。使用泊松回归的离散时间失效分析分别应用于每个中心的数据,以模拟累积药物暴露对膀胱癌发病率的影响,并对曾使用吡格列酮进行时间依赖性调整。然后使用固定效应和随机效应meta回归对这些数据进行汇总。

结果

整理了101万人超过590万人年的数据。有3248例膀胱癌新发病例,其中117例为暴露病例,中位随访时间为4.0至7.4年。总体而言,在对年龄、日历年份、糖尿病病程、吸烟以及曾使用吡格列酮进行调整后,没有证据表明男性(每100天累积暴露的率比[RR]为1.01;95%置信区间0.97,1.06)或女性(RR为1.04;95%置信区间0.97,1.11)中吡格列酮的累积暴露与膀胱癌之间存在任何关联。在男性(RR为1.01;95%置信区间0.98,1.03)或女性(RR为1.00;95%置信区间0.94,1.07)中,未观察到罗格列酮与膀胱癌之间存在关联。

结论/解读:在这项大型的汇总多人群分析中,吡格列酮或罗格列酮的累积使用与膀胱癌的发病率无关。

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