Monitoring liver safety in drug development: The GSK experience

To promptly identify and evaluate liver safety events, an evidence-based liver safety system was created for global Phase I–III clinical trials. The goals of this system included improving clinical trial subject safety, expanding information on liver safety events, and improving data quality across...

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Veröffentlicht in:	Regulatory toxicology and pharmacology 2007-11, Vol.49 (2), p.90-100
Hauptverfasser:	Hunt, Christine M., Papay, Julie I., Edwards, Rita I., Theodore, Dickens, Alpers, David H., Dollery, Colin, DeBruin, Tjerk W., Adkison, Kimberly K., Stirnadel, Heide A., Gibbs, Trevor G.
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Sprache:	eng
Schlagworte:	Algorithms Chemical and Drug Induced Liver Injury Clinical Trials as Topic Drug Monitoring - methods Drug-Related Side Effects and Adverse Reactions Endpoint Determination Evidence-Based Medicine Hepatitis B screening Hepatitis C screening Humans Hy’s Law Liver - drug effects Liver chemistries Liver Function Tests Liver safety Safety systems Transaminase elevation Withholding Treatment
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container_title	Regulatory toxicology and pharmacology
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creator	Hunt, Christine M. Papay, Julie I. Edwards, Rita I. Theodore, Dickens Alpers, David H. Dollery, Colin DeBruin, Tjerk W. Adkison, Kimberly K. Stirnadel, Heide A. Gibbs, Trevor G.
description	To promptly identify and evaluate liver safety events, an evidence-based liver safety system was created for global Phase I–III clinical trials. The goals of this system included improving clinical trial subject safety, expanding information on liver safety events, and improving data quality across studies by establishing and communicating: • Liver chemistry subject stopping criteria. • Hepatitis B and C screening and exclusion criteria. • Close monitoring and follow-up of subjects to determine the etiology of the liver event. Two different algorithms for liver stopping criteria were developed. The most stringent criteria were selected for healthy volunteers in Phase I studies, where no treatment benefit is anticipated and clinical safety data are limited. With an interest in assessing potential liver “tolerance” or adaptation with accruing safety information, slightly higher liver chemistry thresholds were set for Phase II–III studies. This paper will describe the importance of liver safety in drug development, laboratory tests used to monitor liver safety, the rationale for selected liver chemistry subject stopping criteria, and implementation of this safety system.
doi_str_mv	10.1016/j.yrtph.2007.06.002
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subjects	Algorithms Chemical and Drug Induced Liver Injury Clinical Trials as Topic Drug Monitoring - methods Drug-Related Side Effects and Adverse Reactions Endpoint Determination Evidence-Based Medicine Hepatitis B screening Hepatitis C screening Humans Hy’s Law Liver - drug effects Liver chemistries Liver Function Tests Liver safety Safety systems Transaminase elevation Withholding Treatment
title	Monitoring liver safety in drug development: The GSK experience
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