Your search keyword '"Monnot, Andrew D."' showing total 2 results

1. A critical review of the acetaminophen preclinical carcinogenicity and tumor promotion data and their implications for its carcinogenic hazard potential.

Author

Murray, F. Jay, Monnot, Andrew D., Jacobson-Kram, David, Cohen, Samuel M., Hardisty, Jerry F., Bandara, Suren B., Kovochich, Michael, Deore, Milind, Pitchaiyan, Suresh Kumar, Gelotte, Cathy K., Lai, John C.K., Atillasoy, Evren, Hermanowski-Vosatka, Anne, Kuffner, Edwin, Unice, Kenneth M., Yang, Kyunghee, Gebremichael, Yeshitila, Howell, Brett A., and Eichenbaum, Gary

Subjects

*CARCINOGENS, *CARCINOGENICITY, *ENVIRONMENTAL risk assessment, *HEALTH risk assessment, *ACETAMINOPHEN, *HAZARDS

Abstract

In 2019 the California Office of Environmental Health Hazard Assessment (OEHHA) initiated a review of the carcinogenic hazard potential of acetaminophen, including an assessment of the long-term rodent carcinogenicity and tumor initiation/promotion studies. The objective of the analysis herein was to inform this review process with a weight-of-evidence assessment of these studies and an assessment of the relevance of these models to humans. In most of the 14 studies, there were no increases in the incidences of tumors in any organ system. In the few studies in which an increase in tumor incidence was observed, there were factors such as absence of a dose response and a rodent-specific tumor supporting that these findings are not relevant to human hazard identification. In addition, we performed qualitative analysis and quantitative simulations of the exposures to acetaminophen and its metabolites and its toxicity profile; the data support that the rodent models are toxicologically relevant to humans. The preclinical carcinogenicity results are consistent with the broader weight of evidence assessment and evaluations of multiple international health authorities supporting that acetaminophen is not a carcinogenic hazard. • A weight-of-evidence assessment of long-term rodent carcinogenicity and tumor initiation/promotion studies was performed. • No increases in tumor incidence were observed or responses were not relevant to human hazard identification. • Qualitative assessment and quantitative simulations confirm relevance of rodent model data to humans. • Results demonstrate that acetaminophen is not a carcinogenicity hazard. [ABSTRACT FROM AUTHOR]

Published

2020

2. A comprehensive weight of evidence assessment of published acetaminophen genotoxicity data: Implications for its carcinogenic hazard potential.

Author

Kirkland, David, Kovochich, Michael, More, Sharlee L., Murray, F. Jay, Monnot, Andrew D., Miller, Julie V., Jaeschke, Hartmut, Jacobson-Kram, David, Deore, Milind, Pitchaiyan, Suresh Kumar, Unice, Kenneth, and Eichenbaum, Gary

Subjects

*GENETIC toxicology, *ENVIRONMENTAL risk assessment, *HEALTH risk assessment, *ACETAMINOPHEN, *GENETIC mutation, *BACTERIAL mutation

Abstract

In 2019, the California Office of Environmental Health Hazard Assessment initiated a review of the carcinogenic hazard potential of acetaminophen, including an assessment of its genotoxicity. The objective of this analysis was to inform this review process with a weight-of-evidence assessment of more than 65 acetaminophen genetic toxicology studies that are of widely varying quality and conformance to accepted standards and relevance to humans. In these studies, acetaminophen showed no evidence of induction of point or gene mutations in bacterial and mammalian cell systems or in in vivo studies. In reliable, well-controlled test systems, clastogenic effects were only observed in unstable, p53-deficient cell systems or at toxic and/or excessively high concentrations that adversely affect cellular processes (e.g., mitochondrial respiration) and cause cytotoxicity. Across the studies, there was no clear evidence that acetaminophen causes DNA damage in the absence of toxicity. In well-controlled clinical studies, there was no meaningful evidence of chromosomal damage. Based on this weight-of-evidence assessment, acetaminophen overwhelmingly produces negative results (i.e., is not a genotoxic hazard) in reliable, robust high-weight studies. Its mode of action produces cytotoxic effects before it can induce the stable, genetic damage that would be indicative of a genotoxic or carcinogenic hazard. • Acetaminophen genotoxicity reviewed using weight of evidence approaches. • No induction of gene mutations in bacteria or mammalian cells in vitro or in vivo. • No clastogenicity in robust systems at non-cytotoxic concentrations up to 1 mM in vitro. • No evidence of clastogenicity in well-controlled human studies even at acute overdose. • Does not induce genetic damage indicative of a genotoxic or carcinogenic hazard. [ABSTRACT FROM AUTHOR]

Published

2021