Investigation of Correlation Among Safety Biomarkers in Serum, Histopathological Examination, and Toxicogenomics

Author:

Wang Tao1,Papoutsi Maria2,Wiesmann Marion3,DeCristofaro Marc1,Keselica M. Craig1,Skuba Elizabeth1,Spaet Robert1,Markovits Judit1,Wolf Armin2,Moulin Pierre2,Pognan Francois2,Vancutsem Paul1,Petryk Lew4,Sutton James1,Chibout Salah-Dine2,Kluwe William1

Affiliation:

1. Translational Sciences, Novartis Institute of Biomedical Research, Emeryville, CA, USA

2. Translational Sciences, Novartis Institute of Biomedical Research, Basel, Switzerland

3. Oncology, Novartis Institute of Biomedical Research, Basel, Switzerland

4. Oncology, Novartis Pharma, Emeryville, CA, USA

Abstract

This article addresses the issue of miscorrelation between hepatic injury biomarkers and histopathological findings in the drug development context. Our studies indicate that the use of toxicogenomics can aid in the drug development decision-making process associated with such miscorrelated data. BLZ945 was developed as a Colony-Stimulating Factor 1 Receptor (CSF-1R) inhibitor. Treatment of BLZ945 in rats and monkeys increased serum alanine aminotransferase (ALT) and aspartate transaminase (AST). However, liver hypertrophy was the only histopathological liver finding in rats, and there was no change in the livers of monkeys. Longer treatment of BLZ945 in rats for 6 weeks caused up to 6-fold elevation of ALT, yet hepatocyte necrosis was not detected microscopically. Toxicogenomic profiling of liver samples demonstrated that the genes associated with early response to liver injury, apoptosis/necrosis, inflammation, oxidative stress, and metabolic enzymes were upregulated. Studies are ongoing to evaluate the mechanisms underlying BL945-induced ALT and AST elevations.

Publisher

SAGE Publications

Subject

Toxicology

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