Literature DB >> 16329147

The role of NO synthases in arginine-dependent small intestinal and colonic carcinogenesis.

Hagit F Yerushalmi1, David G Besselsen, Natalia A Ignatenko, Karen A Blohm-Mangone, Jose L Padilla-Torres, David E Stringer, Haiyan Cui, Hana Holubec, Claire M Payne, Eugene W Gerner.   

Abstract

Arginine is catabolized by NOS2 and other nitric oxide synthases to form nitric oxide. We evaluated the roles of dietary arginine and Nos2 in Apc-dependent intestinal tumorigenesis in Min mice with and without a functional Nos2 gene. NOS2 protein was expressed only in intestinal tissues of Apc(Min/+) Nos2+/+ mice. NOS3 expression was higher in intestinal tissues of mice lacking Nos2, mainly in the small intestine. When diet was supplemented with arginine (0.2% and 2% in drinking water), lack of Nos2 results in decreased tumorigenesis in both small intestine and colon. In Nos2 knockout mice, supplemental arginine (up to 2%) caused a decrease in small intestinal tumor number and size. The arginine-dependent decrease was associated with an increase in nitrotyrosine formation and apoptosis in the region of intestinal stem cells. Mice expressing Nos2 did not show these changes. These mice did, however, show an arginine-dependent increase in colon tumor number and incidence, while no effect on apoptosis was seen. These changes were associated with increased nitrotyrosine formation in epithelial cells. Mice lacking Nos2 did not show changes in tumorigenesis or nitrotyrosine formation, while demonstrating an arginine-dependent increase in apoptosis. These data suggest that Nos2 and dietary arginine have significant effects on intestinal and colonic tumorigenesis in Min mice. In both tissues, loss of Nos2 is associated with decreased tumorigenesis when mice are supplemented with dietary arginine. In the small intestine, Nos2 prevents the arginine-induced decrease in tumor number and size, which is associated with NOS3 expression and increased apoptosis. In the colon, Nos2 is required for the arginine-induced increase in tumor number and incidence. Copyright 2005 Wiley-Liss, Inc.

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Year:  2006        PMID: 16329147     DOI: 10.1002/mc.20168

Source DB:  PubMed          Journal:  Mol Carcinog        ISSN: 0899-1987            Impact factor:   4.784


  15 in total

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Review 5.  Targeting polyamines and inflammation for cancer prevention.

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Review 7.  Combination chemoprevention for colon cancer targeting polyamine synthesis and inflammation.

Authors:  Eugene W Gerner; Frank L Meyskens
Journal:  Clin Cancer Res       Date:  2009-02-01       Impact factor: 12.531

8.  Differential effects of reactive nitrogen species on DNA base excision repair initiated by the alkyladenine DNA glycosylase.

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Review 9.  Current concepts in colorectal cancer prevention.

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10.  Transitions at CpG dinucleotides, geographic clustering of TP53 mutations and food availability patterns in colorectal cancer.

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