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Cardiovascular risk profile in individuals initiating treatment for overactive bladder – Challenges and learnings for comparative analysis using linked claims and electronic medical record databases

机译:开始膀胱过度活动症治疗的个体的心血管风险概况–使用关联的索赔和电子病历数据库进行比较分析的挑战和学习

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摘要

For managing overactive bladder (OAB), mirabegron, a β3 adrenergic receptor agonist, is typically used as second-line pharmacotherapy after antimuscarinics. Therefore, patients initiating treatment with mirabegron and antimuscarinics may differ, potentially impacting associated clinical outcomes. When using observational data to evaluate real-world safety and effectiveness of OAB treatments, residual bias due to unmeasured confounding and/or confounding by indication are important considerations. Falsification analysis, in which clinically irrelevant endpoints are tested as a reference, can be used to assess residual bias. The objective in this study was to compare baseline cardiovascular risk among OAB patients by treatment, and assess the presence of residual bias via falsification analysis of OAB patients treated with mirabegron or antimuscarinics, to determine whether clinically relevant comparisons across groups would be feasible. Linked electronic health record and claims data (Optum/Humedica) for OAB patients in the United States from 2011–2015 were available, with index defined as first date of OAB treatment during this period. Unadjusted characteristics were compared across groups at index and propensity-matching conducted. Falsification endpoints (hepatitis C, shingles, community-acquired pneumonia) were compared between groups using odds ratios (ORs) and 95% confidence intervals (CI). The study identified 10,311 antimuscarinic- and 408 mirabegron-treated patients. Mirabegron patients were predominantly older males, with more comorbidities. The analytic sample included 1,188 antimuscarinic patients propensity-matched to 396 mirabegron patients; after matching, no significant baseline differences remained. Estimates of falsification ORs were 0.7 (CI:0.3–1.7) for shingles, 1.5 (CI:0.3–8.2) for hepatitis C, 0.8 (CI:0.4–1.8) and 0.9 (CI:0.6–1.4) for pneumonia. While propensity matching successfully balanced observed covariates, wide CIs prevented definitive conclusions regarding residual bias. Accordingly, further observational comparisons by treatment group were not pursued. In real-world analysis, bias-detection methods could not confirm that differences in cardiovascular risk in patients receiving mirabegron versus antimuscarinics were fully adjusted for, precluding clinically relevant comparisons across treatment groups.
机译:为了控制膀胱过度活动症(OAB),通常将米拉贝隆(一种β3肾上腺素受体激动剂)用作抗毒蕈碱剂治疗后的二线药物治疗。因此,开始使用米拉贝隆和抗毒蕈碱药物治疗的患者可能会有所不同,可能会影响相关的临床结果。当使用观察数据评估OAB治疗的现实世界安全性和有效性时,由于未测混杂和/或适应症造成的残留偏差是重要的考虑因素。伪造分析(其中临床上不相关的端点均作为参考进行测试)可用于评估残留偏差。本研究的目的是通过治疗比较OAB患者的基线心血管风险,并通过对米拉贝隆或抗毒蕈碱药物治疗的OAB患者进行伪造分析评估残留偏倚的存在,以确定各组之间临床相关的比较是否可行。可获得2011年至2015年美国OAB患者的关联电子健康记录和索赔数据(Optum / Humedica),其索引定义为该期间OAB治疗的首次日期。在进行指数和倾向匹配时,对各组之间未经调整的特征进行了比较。使用比值比(OR)和95%置信区间(CI)比较各组之间的伪造终点(丙型肝炎,带状疱疹,社区获得性肺炎)。该研究确定了10,311例抗毒蕈碱药物和408例米拉贝隆治疗的患者。 Mirabegron患者主要是年龄较大的男性,合并症更多。分析样本包括倾向性匹配的1,188名抗毒蕈碱患者与396名米拉贝隆患者;匹配后,没有明显的基线差异。带状疱疹的假手术OR估计为:丙型肝炎为0.7(CI:0.3-1.7),丙型肝炎为1.5(CI:0.3-8.2),肺炎为0.8(CI:0.4-1.8)和0.9(CI:0.6-1.4)。虽然倾向匹配成功地平衡了观察到的协变量,但宽置信区间仍无法得出有关残余偏差的明确结论。因此,未进行治疗组的进一步观察比较。在现实世界的分析中,偏倚检测方法无法确认接受米拉贝隆和抗毒蕈碱药物治疗的患者的心血管风险差异是否已完全调整,从而排除了各治疗组之间的临床相关比较。

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