Mode of action and human relevance analysis for nuclear receptor-mediated liver toxicity: A case study with phenobarbital as a model constitutive androstane receptor (CAR) activator
Clifford R. Elcombe,Richard C. Peffer,Douglas C. Wolf,Jason Bailey,Remi Bars,David R. Bell,Russell C. Cattley,Stephen S. Ferguson,David R. Geter,Amber K. Goetz,Jay I. Goodman,Susan D. Hester,Abigail Jacobs,Curtis J. Omiecinski,Rita Schoeny,Wen Xie,Brian G. Lake +16 more
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The MOA for PB-induced rodent liver tumor formation was considered to be qualitatively not plausible for humans, supported by data from a number of epidemiological studies conducted in human populations chronically exposed to PB in which there is no clear evidence for increased liver tumor risk.Abstract:
The constitutive androstane receptor (CAR) and pregnane X receptor (PXR) are important nuclear receptors involved in the regulation of cellular responses from exposure to many xenobiotics and various physiological processes. Phenobarbital (PB) is a non-genotoxic indirect CAR activator, which induces cytochrome P450 (CYP) and other xenobiotic metabolizing enzymes and is known to produce liver foci/tumors in mice and rats. From literature data, a mode of action (MOA) for PB-induced rodent liver tumor formation was developed. A MOA for PXR activators was not established owing to a lack of suitable data. The key events in the PB-induced liver tumor MOA comprise activation of CAR followed by altered gene expression specific to CAR activation, increased cell proliferation, formation of altered hepatic foci and ultimately the development of liver tumors. Associative events in the MOA include altered epigenetic changes, induction of hepatic CYP2B enzymes, liver hypertrophy and decreased apoptosis; with inhibition of gap junctional intercellular communication being an associative event or modulating factor. The MOA was evaluated using the modified Bradford Hill criteria for causality and other possible MOAs were excluded. While PB produces liver tumors in rodents, important species differences were identified including a lack of cell proliferation in cultured human hepatocytes. The MOA for PB-induced rodent liver tumor formation was considered to be qualitatively not plausible for humans. This conclusion is supported by data from a number of epidemiological studies conducted in human populations chronically exposed to PB in which there is no clear evidence for increased liver tumor risk.read more
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References
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Journal ArticleDOI
The environment and disease: association or causation?
TL;DR: The criteria outlined in "The Environment and Disease: Association or Causation?" help identify the causes of many diseases, including cancers of the reproductive system.
Journal Article
The environment and disease: association or causation?
TL;DR: This paper contrasts Bradford Hill’s approach with a currently fashionable framework for reasoning about statistical associations – the Common Task Framework – and suggests why following Bradford Hill, 50+ years on, is still extraordinarily reasonable.
Journal ArticleDOI
Libri Ricevuti: IARC Monographs on the Evaluation of Carcinogenic Risks to Humans
Journal ArticleDOI
Species differences between mouse, rat, dog, monkey and human CYP-mediated drug metabolism, inhibition and induction.
TL;DR: The authors conclude that CYP2E1 shows no large differences between species, and extrapolation between species appears to hold quite well, and the species-specific isoforms of CYP1A, -2C, -1D and -3A show appreciable interspecies differences in terms of catalytic activity and some caution should be applied when extrapolating metabolism data from animal models to humans.
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Drug-Related Hepatotoxicity
Victor J. Navarro,John R. Senior +1 more
TL;DR: Clinical guidance is provided with regard to the detection, evaluation, and possible prevention of drug-related hepatotoxicity in patients exposed to hepatotoxic effects of new medication.