Folate transport gene inactivation in mice increases sensitivity to colon carcinogenesis. Academic Article

abstract

• Low dietary folate intake is associated with an increased risk for colon cancer; however, relevant genetic animal models are lacking. We therefore investigated the effect of targeted ablation of two folate transport genes, folate binding protein 1 (Folbp1) and reduced folate carrier 1 (RFC1), on folate homeostasis to elucidate the molecular mechanisms of folate action on colonocyte cell proliferation, gene expression, and colon carcinogenesis. Targeted deletion of Folbp1 (Folbp1(+/-) and Folbp1(-/-)) significantly reduced (P < 0.05) colonic Folbp1 mRNA, colonic mucosa, and plasma folate concentration. In contrast, subtle changes in folate homeostasis resulted from targeted deletion of RFC1 (RFC1(+/-)). These animals had reduced (P < 0.05) colonic RFC1 mRNA and exhibited a 2-fold reduction in the plasma S-adenosylmethionine/S-adenosylhomocysteine. Folbp1(+/-) and Folbp1(-/-) mice had larger crypts expressed as greater (P < 0.05) numbers of cells per crypt column relative to Folbp1(+/+) mice. Colonic cell proliferation was increased in RFC1(+/-) mice relative to RFC1(+/+) mice. Microarray analysis of colonic mucosa showed distinct changes in gene expression specific to Folbp1 or RFC1 ablation. The effect of folate transporter gene ablation on colon carcinogenesis was evaluated 8 and 38 weeks post-azoxymethane injection in wild-type and heterozygous mice. Relative to RFC1(+/+) mice, RFC1(+/-) mice developed increased (P < 0.05) numbers of aberrant crypt foci at 8 weeks. At 38 weeks, RFC1(+/-) mice developed local inflammatory lesions with or without epithelial dysplasia as well as adenocarcinomas, which were larger relative to RFC1(+/+) mice. In contrast, Folbp1(+/-) mice developed 4-fold (P < 0.05) more lesions relative to Folbp1(+/+) mice. In conclusion, Folbp1 and RFC1 genetically modified mice exhibit distinct changes in colonocyte phenotype and therefore have utility as models to examine the role of folate homeostasis in colon cancer development.

authors

• Chapkin, Robert
• Weeks, Bradley

published proceedings

• Cancer Res

author list (cited authors)

• Ma, D., Finnell, R. H., Davidson, L. A., Callaway, E. S., Spiegelstein, O., Piedrahita, J. A., ... Chapkin, R. S.

citation count

• 51

complete list of authors

• Ma, David WL||Finnell, Richard H||Davidson, Laurie A||Callaway, Evelyn S||Spiegelstein, Ofer||Piedrahita, Jorge A||Salbaum, J Michael||Kappen, Claudia||Weeks, Brad R||James, Jill||Bozinov, Daniel||Lupton, Joanne R||Chapkin, Robert S

publication date

• February 2005

publisher

• American Association for Cancer Research (AACR)  Publisher

published in

• Cancer Research  Journal

keywords

• Animals
• Azoxymethane
• Carcinogens
• Carrier Proteins
• Cell Cycle
• Cell Transformation, Neoplastic
• Colon
• Colonic Neoplasms
• Folate Receptors, GPI-Anchored
• Gene Expression Profiling
• Gene Silencing
• Genetic Predisposition To Disease
• Kidney
• Male
• Membrane Transport Modulators
• Membrane Transport Proteins
• Mice
• Mice, Inbred C57BL
• Mice, Knockout
• Non-programmatic
• Oligonucleotide Array Sequence Analysis
• Precancerous Conditions
• Receptors, Cell Surface
• Reduced Folate Carrier Protein
• Reverse Transcriptase Polymerase Chain Reaction
• S-adenosylhomocysteine
• S-adenosylmethionine

PubMed Central ID

• 15705887

Digital Object Identifier (DOI)

• 10.1158/0008-5472.887.65.3

start page

• 887

end page

• 897

volume

• 65

issue

• 3

URL

• http://dx.doi.org/10.1158/0008-5472.887.65.3