Apperloo Ellen M, Tuttle Katherine R, Pavo Imre, Haupt Axel, Taylor Rebecca, Wiese Russell J, Hemmingway Andrea, Cherney David Z I, Sattar Naveed, Heerspink Hiddo J L
Department of Clinical Pharmacy and Pharmacology, University of Groningen, University Medical Center Groningen, Groningen, the Netherlands.
Providence Medical Research Center, Providence Inland Northwest Health, Spokane, WA.
Diabetes Care. 2025 Mar 1;48(3):430-436. doi: 10.2337/dc24-1773.
Tirzepatide, a long-acting, glucose-dependent insulinotropic polypeptide/glucagon-like peptide 1 receptor agonist, reduced urine albumin-to-creatinine ratio (UACR) and estimated glomerular filtration rate (eGFR) decline in people with type 2 diabetes and high cardiovascular risk in the SURPASS-4 trial. To examine the generalizability of these findings, we assessed change from baseline in UACR for tirzepatide (5, 10, and 15 mg) compared with active and placebo treatment in a broad population from the SURPASS-1-5 trials.
This post hoc analysis examined data from the overall pooled SURPASS-1-5 population and subgroups defined by baseline UACR ≥30 mg/g. A mixed model for repeated measures was used to analyze on-treatment data from baseline to the end-of-treatment visit. Study identifier was included in the model as a covariate.
The adjusted mean percent change from baseline in UACR for tirzepatide 5, 10, or 15 mg compared with all pooled comparators was -19.3% (95% CI -25.5, -12.5), -22.0% (-28.1, -15.3), and -26.3 (-32.0, -20.0), respectively, at week 40/42. Results were similar across pooled placebo, active, and insulin comparator studies. UACR lowering appeared more pronounced in subgroups with UACR ≥30 mg/g. Mediation analysis findings suggested that approximately one-half of the reduction in albuminuria associated with tirzepatide may be weight loss related. There was no difference in eGFR between tirzepatide and pooled comparators at week 40/42.
In this post hoc analysis in people with type 2 diabetes, including those with chronic kidney disease, tirzepatide was associated with a clinically relevant decreased UACR versus comparators, suggesting a potential kidney-protective effect.
替尔泊肽是一种长效的、葡萄糖依赖性促胰岛素多肽/胰高血糖素样肽-1受体激动剂,在SURPASS-4试验中,它降低了2型糖尿病和心血管疾病高风险患者的尿白蛋白肌酐比值(UACR)并减缓了估计肾小球滤过率(eGFR)下降。为检验这些结果的普遍性,我们在SURPASS-1-5试验的广泛人群中评估了替尔泊肽(5、10和15毫克)与活性药物及安慰剂治疗相比,UACR自基线的变化情况。
这项事后分析检查了SURPASS-1-5总体合并人群以及基线UACR≥30毫克/克定义的亚组的数据。采用重复测量混合模型分析从基线到治疗结束访视的治疗期数据。研究标识符作为协变量纳入模型。
在第40/42周时,与所有合并的对照药物相比,替尔泊肽5毫克、10毫克或15毫克组UACR自基线调整后的平均百分比变化分别为-19.3%(95%CI -25.5,-12.5)、-22.0%(-28.1,-15.3)和-26.3(-32.0,-20.0)。在合并的安慰剂、活性药物和胰岛素对照研究中结果相似。在UACR≥30毫克/克的亚组中,UACR降低似乎更明显。中介分析结果表明,替尔泊肽所致蛋白尿减少中约一半可能与体重减轻有关。在第40/42周时,替尔泊肽与合并对照药物之间的eGFR无差异。
在这项针对2型糖尿病患者(包括慢性肾脏病患者)的事后分析中,与对照药物相比,替尔泊肽与临床上相关的UACR降低有关,提示其具有潜在的肾脏保护作用。
