联合应用稳健的尿液生物标志物评估慢性肾脏病进展。
Combining robust urine biomarkers to assess chronic kidney disease progression.
机构信息
Département « Croissance et Signalisation », Institut Necker Enfants Malades, INSERM U1151, CNRS UMR 8253, Université de Paris Cité, Paris, France; Service d'Explorations Fonctionnelles, Hôpital Necker Enfants Malades, Assistance Publique-Hôpitaux de Paris, Paris, France.
Département « Croissance et Signalisation », Institut Necker Enfants Malades, INSERM U1151, CNRS UMR 8253, Université de Paris Cité, Paris, France.
出版信息
EBioMedicine. 2023 Jul;93:104635. doi: 10.1016/j.ebiom.2023.104635. Epub 2023 Jun 6.
BACKGROUND
Urinary biomarkers may improve the prediction of chronic kidney disease (CKD) progression. Yet, data reporting the applicability of most commercial biomarker assays to the detection of their target analyte in urine together with an evaluation of their predictive performance are scarce.
METHODS
30 commercial assays (ELISA) were tested for their ability to quantify the target analyte in urine using strict (FDA-approved) validation criteria. In an exploratory analysis, LASSO (Least Absolute Shrinkage and Selection Operator) logistic regression analysis was used to identify potentially complementary biomarkers predicting fast CKD progression, determined as the CrEDTA clearance-based measured glomerular filtration rate (mGFR) decline (>10% per year) in a subsample of 229 CKD patients (mean age, 61 years; 66% men; baseline mGFR, 38 mL/min) from the NephroTest prospective cohort.
FINDINGS
Among the 30 assays, directed against 24 candidate biomarkers, encompassing different pathophysiological mechanisms of CKD progression, 16 assays fulfilled the FDA-approved criteria. LASSO logistic regressions identified a combination of five biomarkers including CCL2, EGF, KIM1, NGAL, and TGF-α that improved the prediction of fast mGFR decline compared to the kidney failure risk equation variables alone: age, gender, mGFR, and albuminuria. Mean area under the curves (AUC) estimated from 100 re-samples was higher in the model with than without these biomarkers, 0.722 (95% confidence interval 0.652-0.795) vs. 0.682 (0.614-0.748), respectively. Fully-adjusted odds-ratios (95% confidence interval) for fast progression were 1.87 (1.22, 2.98), 1.86 (1.23, 2.89), 0.43 (0.25, 0.70), 1.10 (0.71, 1.83), 0.55 (0.33, 0.89), and 2.99 (1.89, 5.01) for albumin, CCL2, EGF, KIM1, NGAL, and TGF-α, respectively.
INTERPRETATION
This study provides a rigorous validation of multiple assays for relevant urinary biomarkers of CKD progression which combination may improve the prediction of CKD progression.
FUNDING
This work was supported by Institut National de la Santé et de la Recherche Médicale, Université de Paris, Assistance Publique Hôpitaux de Paris, Agence Nationale de la Recherche, MSDAVENIR, Pharma Research and Early Development Roche Laboratories (Basel, Switzerland), and Institut Roche de Recherche et Médecine Translationnelle (Paris, France).
背景
尿生物标志物可能改善慢性肾脏病(CKD)进展的预测。然而,报告大多数商业生物标志物检测试剂盒用于检测尿液中目标分析物的适用性并评估其预测性能的数据仍然很少。
方法
使用严格的(FDA 批准)验证标准,对 30 种商业检测试剂盒(ELISA)进行了检测其定量分析尿液中目标分析物的能力。在一项探索性分析中,使用最小绝对收缩和选择算子(LASSO)逻辑回归分析,确定了潜在的互补生物标志物,这些标志物可预测快速 CKD 进展,这是通过 229 例 CKD 患者(平均年龄 61 岁;66%为男性;基线 mGFR 为 38mL/min)中 CrEDTA 清除率为基础的肾小球滤过率(mGFR)下降来确定的(每年>10%),这是从前瞻性队列研究中的 NephroTest 中获得的。
发现
在针对 24 种候选生物标志物的 30 种检测试剂盒中,涵盖了 CKD 进展的不同病理生理机制,有 16 种符合 FDA 批准的标准。LASSO 逻辑回归确定了包括 CCL2、EGF、KIM1、NGAL 和 TGF-α 在内的五种生物标志物的组合,与单独使用肾脏衰竭风险方程变量相比,这些生物标志物可改善快速 mGFR 下降的预测:年龄、性别、mGFR 和白蛋白尿。在 100 次重采样中估计的平均曲线下面积(AUC)在包含这些生物标志物的模型中更高,为 0.722(95%置信区间 0.652-0.795),而不包含这些生物标志物的模型为 0.682(0.614-0.748)。快速进展的完全调整比值比(95%置信区间)分别为 1.87(1.22, 2.98)、1.86(1.23, 2.89)、0.43(0.25, 0.70)、1.10(0.71, 1.83)、0.55(0.33, 0.89)和 2.99(1.89, 5.01),用于白蛋白、CCL2、EGF、KIM1、NGAL 和 TGF-α。
解释
本研究对多个与 CKD 进展相关的尿液生物标志物检测试剂盒进行了严格验证,其组合可能改善 CKD 进展的预测。
资金
本工作得到了法国国家健康与医学研究院、巴黎大学、巴黎公立医院集团、法国国家研究署、MSDAVENIR、罗氏制药研发(巴塞尔,瑞士)和罗氏研究所(巴黎,法国)的支持。
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