| Literature DB >> 35473450 |
Suramya Waidyanatha1, Sherry R Black2, Kristine L Witt1, Timothy R Fennell2, Carol Swartz3, Leslie Recio3, Scott L Watson2, Purvi Patel2, Reshan A Fernando2, Cynthia V Rider1.
Abstract
α-Pinene caused a concentration-responsive increase in bladder hyperplasia and decrease in sperm counts in rodents following inhalation exposure. Additionally, it formed a prospective reactive metabolite, α-pinene oxide.To provide human relevant context for data generated in animal models and explore potential mechanism, we undertook studies to investigate the metabolism of α-pinene to α-pinene oxide and mutagenicity of α-pinene and α-pinene oxide.α-Pinene oxide was formed in rat and human microsomes and hepatocytes with some species differences. Based on area under the concentration versus time curves, the formation of α-pinene oxide was up to 4-fold higher in rats than in humans.While rat microsomes cleared α-pinene oxide faster than human microsomes, the clearance of α-pinene oxide in hepatocytes was similar between species.α-Pinene was not mutagenic with or without induced rat liver S9 in Salmonella typhimurium or Escherichia coli when tested up to 10 000 µg/plate while α-pinene oxide was mutagenic at ≥25 µg/plate.α-Pinene was metabolised to α-pinene oxide under the conditions of the bacterial mutation assay although the concentration was approximately 3-fold lower than the lowest α-pinene oxide concentration that was positive in the assay, potentially explaining the lack of mutagenicity observed with α-pinene.Entities:
Keywords: bacterial mutagenicity; hepatocytes; metabolism; monoterpene; α-pinene; α-pinene oxide
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Year: 2022 PMID: 35473450 PMCID: PMC9298155 DOI: 10.1080/00498254.2022.2070047
Source DB: PubMed Journal: Xenobiotica ISSN: 0049-8254 Impact factor: 1.997