Magnitude of Urine Albumin and KIM-1 Changes Can be Used to Differentiate Glomerular Injury From Tubular Injury in Rats

Author:

Gu Yi-Zhong1ORCID,Paul Erina1,Vlasakova Katerina1ORCID,Troth Sean P.1ORCID,Sistare Frank D.1ORCID,Ramaiah Lila2,Potz Oliver34,Sutradhar Santosh1,Glaab Warren E.1

Affiliation:

1. Merck & Co., Inc., Rahway, New Jersey, USA

2. Janssen Research & Development, Spring House, Pennsylvania, USA

3. Signatope GmbH, Reutlingen, Germany

4. University of Tubingen, Reutlingen, Germany

Abstract

Emerging urinary kidney safety biomarkers have been evaluated in recent years and have been shown to be superior to the serum parameters blood urea nitrogen (BUN) and creatinine (sCr) for monitoring kidney injury in the proximal tubule. However, their potential application in differentiating the location of the initial kidney injury (eg, glomerulus vs tubule) has not been fully explored. Here, we assessed the performance of two algorithms that were constructed using either an empirical or a mathematical model to predict the site of kidney injury using a data set consisting of 22 rat kidney toxicity studies with known urine biomarker and histopathologic outcomes. Two kidney safety biomarkers used in both models, kidney injury molecule 1 (KIM-1) and albumin (ALB), were the best performers to differentiate glomerular injury from tubular injury. The performance of algorithms using these two biomarkers against the gold standard of kidney histopathologic examination showed high sensitivity in differentiating the location of the kidney damage to either the glomerulus or the proximal tubules. These data support the exploration of such an approach for use in clinical settings, leveraging urinary biomarker data to aid in the diagnosis of either glomerular or tubular injury where histopathologic assessments are not conducted.

Publisher

SAGE Publications

Reference16 articles.

1. C-Path Predictive Safety Testing Consortium. DDT-BMQ-000014: safety biomarker panel to aid in the detection of kidney tubular injury in phase 1 trials in healthy volunteers; full qualification package 2018. Accessed April 18, 2024. https://force-dsc.my.site.com/ddt/s/.

2. Renal biomarker qualification submission: a dialog between the FDA-EMEA and Predictive Safety Testing Consortium

3. Polyethlyene Glycol 200 Can Protect Rats Against Drug-Induced Kidney Toxicity Through Inhibition of the Renal Organic Anion Transporter 3

4. Early-Onset albuminuria and Associated Renal Pathology in Leucine-Rich Repeat Kinase 2 Knockout Rats

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