Health & Environmental Research Online (HERO)


Print Feedback Export to File
635847 
Journal Article 
Review 
A reexamination of the PPAR-alpha activation mode of action as a basis for assessing human cancer risks of environmental contaminants 
Guyton, KZ; Chiu, WA; Bateson, TF; Jinot, J; Scott, CS; Brown, RC; Caldwell, JC 
2009 
Yes 
Environmental Health Perspectives
ISSN: 0091-6765
EISSN: 1552-9924 
117 
11 
1664-1672 
English 
20049115 
WOS:000271399300020 
BACKGROUND: Diverse environmental contaminants, including the plasticizer di(2-ethylhexyl)phthalate (DEHP), are hepatocarcinogenic peroxisome proliferators in rodents. Peroxisome proliferator-activated receptor-alpha (PPAR-alpha) activation and its sequelae have been proposed to constitute a mode of action (MOA) for hepatocarcinogenesis by such agents as a sole causative factor. Further, based on a hypothesized lower sensitivity of humans to this MOA, prior reviews have concluded that rodent hepatocarcinogenesis by PPAR-alpha agonists is irrelevant to human carcinogenic risk. DATA SYNTHESIS: Herein, we review recent studies that experimentally challenge the PPAR-alpha activation MOA hypothesis, providing evidence that DEHP is hepatocarcinogenic in PPAR-alpha-null mice and that the MOA but not hepatocarcinogenesis is evoked by PPAR-alpha activation in a transgenic mouse model. We further examine whether relative potency for PPAR-alpha activation or other steps in the MOA correlates with tumorigenic potency. In addition, for most PPAR-alpha agonists of environmental concern, available data are insufficient to characterize relative human sensitivity to this rodent MOA or to induction of hepatocarcinogenesis. CONCLUSIONS: Our review and analyses raise questions about the hypothesized PPAR-alpha activation MOA as a sole explanation for rodent hepatocarcinogenesis by PPAR-alpha agonists and therefore its utility as a primary basis for assessing human carcinogenic risk from the diverse compounds that activate PPAR-alpha. These findings have broad implications for how MOA hypotheses are developed, tested, and applied in human health risk assessment. We discuss alternatives to the current approaches to these key aspects of mechanistic data evaluation. 
Animals; Diethylhexyl Phthalate/toxicity; Environmental Pollutants/*toxicity; Humans; Liver Neoplasms/*chemically induced; Liver Neoplasms, Experimental/chemically induced; Mice; Mice, Knockout; PPAR alpha/*agonists/metabolism; Peroxisome Proliferators/toxicity; Risk Assessment/methods; Species Specificity 
IRIS
• Biphenyl
     Cited References
          Other studies
               Studies Supporting Mode-of-Action
• tert-Butanol
     Cited in Document
• ETBE
     Cited in Document
     Not in Lit Search
• Phthalates – Targeted Search for Epidemiological Studies
     Source – all searches
          Pubmed
          WOS
          Toxnet
     Excluded
     Source – no date limit through June 2013 (Private)
          Pubmed
          WOS
          ToxNet
• Tetrachloroethylene (Perc) (Final, 2012)
     Hazard
          Liver
• Trichloroacetic acid (TCA) (Final, 2011)
• Trichloroethylene (TCE) (Final, 2011)
     All References
     Hazard
     Liver
     Liver Issues
• OPPT_Perchloroethylene (Perc)_C. Engineering
     Total – title/abstract screening
          Off topic
• OPPT_Perchloroethylene (Perc)_D. Exposure
     Total – title/abstract screening
          Off topic
• OPPT_Perchloroethylene (Perc)_E. Fate
     Total – title/abstract screening
          Off topic
• OPPT_Perchloroethylene (Perc)_F. Human Health
     Total – title/abstract screening
          Off topic
• OPPT_Trichloroethylene (TCE)_F. Human Health
     Total – title/abstract screening
          On topic
               Peer review
                    Secondary source/ Review
               Cited in IRIS document or IRIS HERO page
     On topic - additional tags for titles/abstracts
          MOA
PFAS
• PFBA
     Protocol References