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Toxicologic Pathology
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Article

The Liver Toxicity Biomarker Study: Phase I Design and Preliminary Results

Robert N. McBurney*, Wade M. Hines, Linda S. von Tungeln, Laura K. Schnackenberg, Richard D. Beger, Carrie L. Moland, Tao Han, James C. Fuscoe, Ching-Wei Chang, James J. Chen, Zhenqiang Su, Xiao-hui Fan, Weida Tong, Shelagh A. Booth, Raji Balasubramanian, Paul L. Courchesne, Jennifer M. Campbell, Armin Graber, Yu Guo, Peter J. Juhasz, Tricin Y. Li, Moira D. Lynch, Nicole M. Morel, Thomas N. Plasterer, Edward J. Takach, Chenhui Zeng, and Frederick A. Beland

* To whom correspondence should be addressed. E-mail: rmcburney{at}bg-medicine.com.


  Abstract
ABSTRACT

Drug-induced liver injury (DILI) is the primary adverse event that results in withdrawal of drugs from the market and a frequent reason for the failure of drug candidates in development. The Liver Toxicity Biomarker Study (LTBS) is an innovative approach to investigate DILI because it compares molecular events produced in vivo by compound pairs that (a) are similar in structure and mechanism of action, (b) are associated with few or no signs of liver toxicity in preclinical studies, and (c) show marked differences in hepatotoxic potential. The LTBS is a collaborative preclinical research effort in molecular systems toxicology between the National Center for Toxicological Research and BG Medicine, Inc., and is supported by seven pharmaceutical companies and three technology providers. In phase I of the LTBS, entacapone and tolcapone were studied in rats to provide results and information that will form the foundation for the design and implementation of phase II. Molecular analysis of the rat liver and plasma samples combined with statistical analyses of the resulting datasets yielded marker analytes, illustrating the value of the broad-spectrum, molecular systems analysis approach to studying pharmacological or toxicological effects.

First published on January 26, 2009, doi:10.1177/0192623308329287

Toxicologic Pathology 2009;37:52.

A more recent version of this article appeared on January 1, 2009

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