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Open Access 01-11-2014 | Review Article

Causality Assessment for Suspected DILI During Clinical Phases of Drug Development

Authors: Arie Regev, Leonard B. Seeff, Michael Merz, Sif Ormarsdottir, Guruprasad P. Aithal, Jim Gallivan, Paul B. Watkins

Published in: Drug Safety | Special Issue 1/2014

Abstract

Causality assessment is a critical step in establishing the diagnosis of drug induced liver injury (DILI) during drug development. DILI may resemble almost any type of liver disease, and often presents a serious challenge to clinical investigators and drug makers. The diagnosis of DILI is largely based upon a combination of a compatible clinical course, exclusion of all other reasonable causes, resemblance of clinical and pathological features to known features of liver injury due to the drug (i.e., “drug’s signature”), and incidence of liver injury among patients treated with the drug compared to placebo or comparator. Causality assessment for suspected DILI is currently performed using either evaluation by physicians with expertise in liver disorders (i.e., expert opinion) or standardized scoring instruments such as the Roussel Uclaf Causality Assessment Method (RUCAM). Both approaches are widely used in the post marketing setting. Causality assessment based on expert opinion is considered superior to standardized instruments such as RUCAM, in the setting of drug development, and is currently the preferred approach during clinical trials. There is a need for a systematic revision of RUCAM that will render it more suitable for the setting of clinical trials and drug development. Careful monitoring and meticulous data collection during clinical trials are essential in all cases with established liver injury to allow for a proper causality assessment. A workshop was convened to discuss best practices for the assessment of drug-induced liver injury (DILI) in clinical trials. This publication is based on the conclusions of this workshop.

Clinical chemistry criteria for DILI, based on the definition of the DILI Expert Working Group [4] include any one of the following: (1) More than or equal to 5X elevation above the ULN for ALT. (2) More than or equal to 2X elevation above the ULN for ALP (particularly with accompanying elevations in concentrations of gamma-glutamyl transpeptidase) in the absence of known bone pathology driving the rise in ALP level. (3) More than or equal to 3X elevation in ALT concentration and simultaneous elevation of TBL concentration exceeding 2X ULN.

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Title: Causality Assessment for Suspected DILI During Clinical Phases of Drug Development
Authors: Arie Regev
Leonard B. Seeff
Michael Merz
Sif Ormarsdottir
Guruprasad P. Aithal
Jim Gallivan
Paul B. Watkins
Publication date: 01-11-2014
Publisher: Springer International Publishing
Published in: Drug Safety / Issue Special Issue 1/2014
Print ISSN: 0114-5916
Electronic ISSN: 1179-1942
DOI: https://doi.org/10.1007/s40264-014-0185-4

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Causality Assessment for Suspected DILI During Clinical Phases of Drug Development

Abstract

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Abstract

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