Inhibition of vinyl carbamate-induced lung tumors and Kras2 mutations by the garlic derivative diallyl sulfone

T transversions (31%) and A-->G transitions (25%) in the second base, and A-->T transversions (12%) in the third base. All of these mutations were significantly reduced by DASO2 pretreatment. The number of tumors containing Kras2 mutations was highest (38%) in the large papillary tumors. Hence, mice treated with DASO2/VC had decreased frequencies of Kras2 mutations and reduced numbers of small and large papillary tumors, suggesting that activation of the Kras2 gene may be implicated in lung tumor formation and progression. -->

ISSN:	0027-5107
DOI:	10.1016/j.mrfmmm.2008.11.013
Přístupová URL adresa:	https://explore.openaire.eu/search/publication?articleId=doi_dedup___::59a93f5dbfcc3939a57155ded1d27981 https://doi.org/10.1016/j.mrfmmm.2008.11.013
Rights:	CLOSED
Přírůstkové číslo:	edsair.doi.dedup.....59a93f5dbfcc3939a57155ded1d27981
Autor:	Lya G. Hernandez, Poh-Gek Forkert
Rok vydání:	2009
Předmět:	Lung Neoplasms Health Toxicology and Mutagenesis Mutant Urethane Proto-Oncogene Proteins p21(ras) Mice chemistry.chemical_compound Exon Vinyl carbamate Genetics medicine Animals Sulfones Garlic Molecular Biology Malignant phenotype Lung Molecular biology Allyl Compounds medicine.anatomical_structure Amino Acid Substitution chemistry Biochemistry Mutation Ethyl carbamate Lung tumor Diallyl sulfone
Zdroj:	Mutation Research/Fundamental and Molecular Mechanisms of Mutagenesis. 662:16-21
ISSN:	0027-5107
DOI:	10.1016/j.mrfmmm.2008.11.013
Popis:	Vinyl carbamate (VC) is derived from ethyl carbamate (EC), a chemical found in alcoholic beverages and fermented foods. The objectives of this study were to characterize the formation of lung tumors induced by VC in F1 (Big BluexA/J) mice, and to identify the mutations formed in the Kras2 gene. In addition, we have tested the hypothesis that pretreatment with diallyl sulfone (DASO2) inhibits the adverse effects of VC. Mice were treated with VC (60 mg/kg, i.p.) or DASO2 (50 mg/kg, p.o.) 2 h prior to VC (DASO2/VC). Lung tumor multiplicity was significantly lower (21%) in mice treated with DASO2/VC than with VC. Lung tumors induced by VC are manifested as solid or papillary tumors, with the latter being regarded as a more malignant phenotype as they demonstrate no growth restrictions. Solid (42%) and papillary tumors (58%) were found in similar proportions in VC-treated mice. The number of papillary tumors was significantly decreased (44.5%) in mice treated with DASO2/VC, while there was a proportional increase (44.5%) in the number of solid tumors. The number of tumors with mutations in the first and second exon of Kras2 was significantly lower after treatment with DASO2/VC (7%) than after treatment with VC (61%). The mutations were mainly found in codon 61, and were identified as A-->T transversions (31%) and A-->G transitions (25%) in the second base, and A-->T transversions (12%) in the third base. All of these mutations were significantly reduced by DASO2 pretreatment. The number of tumors containing Kras2 mutations was highest (38%) in the large papillary tumors. Hence, mice treated with DASO2/VC had decreased frequencies of Kras2 mutations and reduced numbers of small and large papillary tumors, suggesting that activation of the Kras2 gene may be implicated in lung tumor formation and progression.
Databáze:	OpenAIRE
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