Inflammatory Stress and Idiosyncratic Hepatotoxicity: Hints from Animal Models
Adverse drug reactions (ADRs) present a serious human health problem. They are major contributors to hospitalization and mortality throughout the world ( Lazarou et al., 1998 ; Pirmohamed et al., 2004 ). A small fraction (less than 5%) of ADRs can be classified as âidiosyncratic.â Idiosyncratic...
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Veröffentlicht in: | Pharmacological reviews 2009-09, Vol.61 (3), p.262-282 |
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Sprache: | eng |
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Zusammenfassung: | Adverse drug reactions (ADRs) present a serious human health problem. They are major contributors to hospitalization and mortality
throughout the world ( Lazarou et al., 1998 ; Pirmohamed et al., 2004 ). A small fraction (less than 5%) of ADRs can be classified as âidiosyncratic.â Idiosyncratic ADRs (IADRs) are caused by
drugs with diverse pharmacological effects and occur at various times during drug therapy. Although IADRs affect a number
of organs, liver toxicity occurs frequently and is the primary focus of this review. Because of the inconsistency of clinical
data and the lack of experimental animal models, how IADRs arise is largely undefined. Generation of toxic drug metabolites
and induction of specific immunity are frequently cited as causes of IADRs, but definitive evidence supporting either mechanism
is lacking for most drugs. Among the more recent hypotheses for causation of IADRs is that inflammatory stress induced by
exogenous or endogenous inflammagens is a susceptibility factor. In this review, we give a brief overview of idiosyncratic
hepatotoxicity and the inflammatory response induced by bacterial lipopolysaccharide. We discuss the inflammatory stress hypothesis
and use as examples two drugs that have caused IADRs in human patients: ranitidine and diclofenac. The review focuses on experimental
animal models that support the inflammatory stress hypothesis and on the mechanisms of hepatotoxic response in these models.
The need for design of epidemiological studies and the potential for implementation of inflammation interaction studies in
preclinical toxicity screening are also discussed briefly. |
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ISSN: | 0031-6997 1521-0081 |
DOI: | 10.1124/pr.109.001727 |