Department of Clinical Pharmacy & Pharmacology, University of Groningen, University Medical Center Groningen, Groningen, the Netherlands.
Division of Nephrology, Tufts Medical Center, Boston, MA.
Am J Kidney Dis. 2014 Dec;64(6):860-6. doi: 10.1053/j.ajkd.2014.08.018. Epub 2014 Oct 16.
The currently established end points for clinical trials of progression of chronic kidney disease (CKD) are end-stage renal disease and doubling of serum creatinine level, which approximates a 57% decline in estimated glomerular filtration rate (eGFR). There is increased interest in using alternative end points in clinical trials to shorten trial duration and reduce sample size. As part of an evaluation of using lesser declines in GFR as alternative end points, we examined the associations of various levels of eGFR decline with the subsequent development of established end points and assess the consistency of alternate levels of eGFR decline across varying clinical manifestations of kidney disease and interventions.
Observational analysis of randomized controlled trials.
SETTING & PARTICIPANTS: 9,488 participants in 37 randomized controlled trials in CKD.
Alternative end points, defined as 30% and 40% declines in eGFR from baseline to month 12. Effect modification by baseline eGFR, proteinuria, cause of disease, and interventions.
Established end point, defined as end-stage renal disease, eGFR<15mL/min/1.73m(2), or doubling of serum creatinine level.
From baseline to 12 months, 16.1% and 7.8% of participants had eGFR declines of ≥30% or ≥40%, respectively. Over a median follow-up of 2.0 (IQR, 1.2-3.1) years after the 12-month baseline period, 2,661 established end points were observed. A strong linear association was observed between eGFR decline and subsequent established end points. HRs for the established end point for 30% and 40% decreases in eGFR compared to a 0% decline were 9.6 (95% CI, 7.3-12.6) and 20.3 (95% CI, 14.1-29.3), respectively. The associations were consistent regardless of baseline eGFR, proteinuria, causes of disease, and interventions.
Observational study subject to residual confounding.
The strong associations between lesser declines in eGFR and the subsequent development of established end points were consistent across different clinical characteristics of kidney disease and interventions and support implementation of alternative end points in clinical trials of CKD progression.
目前,慢性肾脏病(CKD)进展临床试验的终点是终末期肾病和血清肌酐水平翻倍,这相当于估算肾小球滤过率(eGFR)下降 57%。人们越来越感兴趣的是在临床试验中使用替代终点来缩短试验持续时间和减少样本量。作为使用 GFR 较小下降作为替代终点评估的一部分,我们研究了各种 eGFR 下降水平与随后建立的终点之间的关系,并评估了不同临床表现和干预措施下替代水平的 GFR 下降的一致性。
对随机对照试验进行观察性分析。
37 项 CKD 随机对照试验中的 9488 名参与者。
替代终点,定义为从基线到第 12 个月 eGFR 下降 30%和 40%。由基线 eGFR、蛋白尿、疾病原因和干预措施引起的效应修饰。
定义为终末期肾病、eGFR<15mL/min/1.73m(2)或血清肌酐水平翻倍的既定终点。
从基线到 12 个月,分别有 16.1%和 7.8%的参与者 eGFR 下降≥30%或≥40%。在基线后 12 个月中位数随访 2.0(IQR,1.2-3.1)年后,观察到 2661 个既定终点。eGFR 下降与随后的既定终点之间存在很强的线性关系。与 eGFR 下降 0%相比,eGFR 下降 30%和 40%的既定终点的 HR 分别为 9.6(95%CI,7.3-12.6)和 20.3(95%CI,14.1-29.3)。这些关联在不同的基线 eGFR、蛋白尿、疾病原因和干预措施下是一致的。
观察性研究受到残余混杂因素的影响。
较小的 eGFR 下降与既定终点的后续发展之间的强烈关联在不同的肾脏疾病和干预措施的临床特征之间是一致的,并支持在 CKD 进展的临床试验中实施替代终点。
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