4.7 Article

Toxicogenomic biomarkers for renal papillary injury in rats

Journal

TOXICOLOGY
Volume 303, Issue 1, Pages 1-8

Publisher

ELSEVIER IRELAND LTD
DOI: 10.1016/j.tox.2012.09.012

Keywords

Toxicogenomics; Rat; Papillary injury; Timp1; Igf1; Lamc2

Funding

  1. Ministry of Health, Labor and Welfare of Japan [H14-001-Toxico, H19-001-Toxico]

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Renal papillary injury is a common side effect observed during nonclinical and clinical investigations in drug development. The present study aimed to identify genomic biomarkers for early and sensitive detection of renal papillary injury in rats. We hypothesized that previously identified genomic biomarkers for tubular injury might be applicable for the sensitive detection of papillary injury in rats. We selected 18 genes as candidate biomarkers for papillary injury based on previously published studies and analyzed their expression profiles by RT-PCR in each kidney region, namely the cortex, cortico-medullary junction, and papilla in various nephrotoxicity models. Comparative analysis of gene expression profiles revealed that some genes were commonly upregulated or downregulated in the renal papilla, reflecting papillary injuries induced by 2-bromoethylamine hydrobromide, phenylbutazone, or n-phenylanthranilic acid. By applying receiver operator characteristics analysis, six candidate biomarkers were identified and their usefulness was confirmed by using an independent data set. The three top-ranked genes, Timp1, Igf1, and Lamc2, exhibited the best prediction performance in an external data set with area under the curve (AUC) values of greater than 0.91. An optimized support vector machine model consisting of three genes achieved the highest AUC value of 0.99. In conclusion, even though definitive validation studies are required for the establishment of their usefulness and reliability, these identified genes may prove to be the most promising candidate genomic biomarkers of renal papillary injury in rats. (C) 2012 Elsevier Ireland Ltd. All rights reserved.

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