| Literature DB >> 22573522 |
Robert N McBurney1, Wade M Hines, Linda S VonTungeln, 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 Juhasz, Tricia Y Li, Moira D Lynch, Nicole M Morel, Thomas N Plasterer, Edward J Takach, Chenhui Zeng, Frederick A Beland.
Abstract
The Liver Toxicity Biomarker Study is a systems toxicology approach to discover biomarkers that are indicative of a drug's potential to cause human idiosyncratic drug-induced liver injury. In phase I, the molecular effects in rat liver and blood plasma induced by tolcapone (a "toxic" drug) were compared with the molecular effects in the same tissues by dosing with entacapone (a "clean" drug, similar to tolcapone in chemical structure and primary pharmacological mechanism). Two durations of drug exposure, 3 and 28 days, were employed. Comprehensive molecular analysis of rat liver and plasma samples yielded marker analytes for various drug-vehicle or drug-drug comparisons. An important finding was that the marker analytes associated with tolcapone only partially overlapped with marker analytes associated with entacapone, despite the fact that both drugs have similar chemical structures and the same primary pharmacological mechanism of action. This result indicates that the molecular analyses employed in the study are detecting substantial "off-target" markers for the two drugs. An additional interesting finding was the modest overlap of the marker data sets for 3-day exposure and 28-day exposure, indicating that the molecular changes in liver and plasma caused by short- and long-term drug treatments do not share common characteristics.Entities:
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Year: 2012 PMID: 22573522 DOI: 10.1177/0192623312444026
Source DB: PubMed Journal: Toxicol Pathol ISSN: 0192-6233 Impact factor: 1.902