FHIT, at a constitutively active chromosome fragile site, is often a target of chromosomal aberrations and deletion in a large fraction of human tumors. Inactivation of murine Fhit allelessignificantly increases susceptibility of mice to spontaneous and carcinogen-induced tumorigenesis. In this study, transgenic mice, carrying a human FHIT cDNA under control of the endogenous promoter, were produced to determine the effect of Fhit expression, from a nonfragile cDNA transgene outside the fragile region, on carcinogen-induced tumor susceptibility of wildtype and Fhit heterozygous mice. Mice received sufficient oral doses of N-nitrosomethybenzylamine (NMBA) to cause forestomach tumors in >80% of nontransgenic control mice. Although the level of expression of the FHIT transgene in the recombinant mouse strains was much lower than the level of endogenous Fhit expression, the tumor burden in NMBA-treated male transgenic mice was significantly reduced, while female transgenic mice were not protected. To determine if the difference in protection could be due to differences in epigenetic changes at the transgene loci in male versus female mice, we examined expression, hypermethylation and induced re-expression of FHIT transgenes in male and female mice or cells derived from them. The transgene was methylated in male and female mice and in cell lines established from male and female transgenic kidneys, the FHIT locus was both hypermethylated and deacetylated. It is likely that the FHIT transgene is more tightly silenced in female transgenic mice, leading to a lack of protection from tumor induction. Copyright © 2007 S. Karger AG.

Influence of a nonfragile FHIT transgene on murine tumor susceptibility / K. A., Mccorkell; Mancini, Rita; Z., Siprashvili; B. L., Barnoski; D., Iliopoulos; L. D., Siracusa; N., Zanesi; C. M., Croce; L. Y. Y., Fong; T., Druck; K., Huebner. - In: CYTOGENETIC AND GENOME RESEARCH. - ISSN 1424-8581. - 118:2-4(2007), pp. 196-203. [10.1159/000108301]

Influence of a nonfragile FHIT transgene on murine tumor susceptibility

MANCINI, RITA;
2007

Abstract

FHIT, at a constitutively active chromosome fragile site, is often a target of chromosomal aberrations and deletion in a large fraction of human tumors. Inactivation of murine Fhit allelessignificantly increases susceptibility of mice to spontaneous and carcinogen-induced tumorigenesis. In this study, transgenic mice, carrying a human FHIT cDNA under control of the endogenous promoter, were produced to determine the effect of Fhit expression, from a nonfragile cDNA transgene outside the fragile region, on carcinogen-induced tumor susceptibility of wildtype and Fhit heterozygous mice. Mice received sufficient oral doses of N-nitrosomethybenzylamine (NMBA) to cause forestomach tumors in >80% of nontransgenic control mice. Although the level of expression of the FHIT transgene in the recombinant mouse strains was much lower than the level of endogenous Fhit expression, the tumor burden in NMBA-treated male transgenic mice was significantly reduced, while female transgenic mice were not protected. To determine if the difference in protection could be due to differences in epigenetic changes at the transgene loci in male versus female mice, we examined expression, hypermethylation and induced re-expression of FHIT transgenes in male and female mice or cells derived from them. The transgene was methylated in male and female mice and in cell lines established from male and female transgenic kidneys, the FHIT locus was both hypermethylated and deacetylated. It is likely that the FHIT transgene is more tightly silenced in female transgenic mice, leading to a lack of protection from tumor induction. Copyright © 2007 S. Karger AG.
2007
01 Pubblicazione su rivista::01a Articolo in rivista
Influence of a nonfragile FHIT transgene on murine tumor susceptibility / K. A., Mccorkell; Mancini, Rita; Z., Siprashvili; B. L., Barnoski; D., Iliopoulos; L. D., Siracusa; N., Zanesi; C. M., Croce; L. Y. Y., Fong; T., Druck; K., Huebner. - In: CYTOGENETIC AND GENOME RESEARCH. - ISSN 1424-8581. - 118:2-4(2007), pp. 196-203. [10.1159/000108301]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11573/144839
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