![Sample our Bioscience journals, sign in here to start your access, Latest two full volumes FREE to you for 14 days]({"type":"image" , "src" : "/sda/5925/TOC-Subject-Sample-2021-Bioscience.jpg"})
Abstract
Vinyl carbamate (VC) and ethyl carbamate (EC) induce the formation of lung tumors. The mechanism involves a two-step oxidation of EC to VC and VC to an epoxide, both of which are mediated mainly by CYP2E1. Interaction of the epoxide with DNA leads to the formation of DNA adducts, including 1,N6ethenodeoxyadenosine and 1,N4-ethenodeoxycytidine. The production of DNA adducts correlated with capacities for the bioactivation of VC, which are higher in the lungs of A/J than in C57BL/6 mice. Importantly, CYP2E1 is higher in the lungs of A/J than in C57BL/6 mice. Studies using F1 (Big Blue® × A/J) transgenic mice revealed the formation of mutations in the lambda cII gene after treatment with VC. Mutations induced by VC were mainly A:T→G:C transitions and A:T→T:A transversions, while mutations induced by EC were mainly G:C→A:T transitions. An EC dose that was 17-fold higher than that for VC was required to produce a similar level of mutant frequency in the lung. Pretreatment of mice with the CYP2E1 inhibitor, diallyl sulfone, significantly inhibited the mutant frequencies induced by VC. Mutations in the endogeneous Kras2 gene were found in codon 61 of exon 2 and were identified as A:T transversions and A→G transitions in the second base and A→T transversions in the third base. These mutations were reduced by treatment of mice with diallyl sulfone before VC and coincided with a reduction in the number of lung tumors with Kras2 mutations. These findings affirmed that the metabolism of EC and VC is a prerequisite for, or at least substantially contributes to, initiation of the cascade of events leading to lung tumor formation.
Acknowledgements
The author wishes to acknowledge the contributions of graduate students, Lya Hernandez and Martin Kaufmann, to this research work. The contribution of Dr. Raymond Bowers from the Department of Chemistry, Queen’s University (Kingston, Ontario, Canada) is gratefully acknowledged.
Declaration of interest: The research work from the author′s laboratory and the preparation of this report have been supported by the Canadian Cancer Society through Grants 014061 and 011129 from the National Cancer Institute of Canada (Toronto, Ontario, Canada). The author reports no conflicts of interest. The author alone is responsible for the content and writing of the paper.