Absence of full-length Brca1 sensitizes mice to oxidative stress and carcinogen-induced tumorigenesis in the esophagus and forestomach

doi:10.1093/carcin/bgm060

Carcinogenesis Advance Access originally published online on March 15, 2007
Carcinogenesis 2007 28(7):1401-1407; doi:10.1093/carcin/bgm060

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Absence of full-length Brca1 sensitizes mice to oxidative stress and carcinogen-induced tumorigenesis in the esophagus and forestomach

Liu Cao, Xiaoling Xu, Longyue L. Cao, Rui-Hong Wang, Xavier Coumoul, Sang S. Kim¹ and Chu-Xia Deng^*

Genetics of Development and Diseases Branch, National Institutes of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, 10/9N105, 10 Center Drive, Bethesda, MD 20892, USA
¹ Present address: Division of Radiation and Nuclear Medicine, National Cancer Center, Goyang, Gyeonggi 411-769, South Korea

^* To whom correspondence should be addressed. Tel: +301 402 7225; Fax: +301 480 1135; Email: chuxiad{at}bdg10.niddk.nih.gov

Environmental and genetic factors are important both in affectinglife span and neoplastic transformation. We have shown previouslythat mice, which are homozygous for full-length breast cancer-associatedgene-1 (Brca1) deletion and heterozygous for a p53-null mutation(Brca1^11/11p53^+/–), display premature aging and high frequencyof spontaneous lymphoma and mammary tumor formation. To investigatethe role of Brca1 in regulation of organ homeostasis and susceptibilityof Brca1 deficiency to environmental carcinogens, we examinedbiological function of Brca1 in maintaining organ homeostasisand carcinogen-induced tumorigenesis. Brca1^11/11p53^+/–mice showed altered gastrointestinal tract homeostasis, includinghyperkeratosis in the esophagus and forestomach. At 6 monthsof age, most mutant mice displayed hyperplasia in their forestomachand esophagus, leading to dysplasia and carcinoma formationin older animals. Brca1 mutant mice exhibited increased expressionof Redd1, elevated reactive oxygen species and are more sensitiveto oxidative stress induced lethality. Upon methyl-N-amylnitrosamine(MNAN) treatment, 70% Brca1 mutant mice developed tumors within4 months whereas only 14% control animals developed tumor atthe same period of the time. Our further analysis revealed thatthe tumorigenesis is accompanied by the loss of p53 and increasedexpression of a number of oncogenes, including Cyclin D1, phosphorylatedform of Akt, ß-catenin, Runx-2 and c-Myc. These resultssuggest that Brca1 is involved in renewable organ homeostasis,linking the environmental and genetic factors in carcinogenesisand aging, and providing new insights into genomic instabilityin organism maintenance and tumorigenesis.

Abbreviations: BRCA1, breast cancer-associated gene-1; DDR, DNA damage response; LOH, loss of heterozygosity; MEF, mouse embryonic fibroblast; ROS, reactive oxygen species; WT, wild type

Received January 3, 2007; revised March 1, 2007; accepted March 2, 2007.

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