Genetic control of susceptibility to carcinogen-induced colorectal cancer in mice: TheCcs3andCcs5loci regulate different aspects of tumorigenesis
Autor: | Nicole Beauchemin, Philippe Gros, Charles Meunier, Tony Kwan, Claire Turbide |
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Rok vydání: | 2011 |
Předmět: |
Congenic
Chromosome 9 Locus (genetics) Quantitative trait locus Biology medicine.disease_cause Chromosomes Mice Genetic linkage medicine Animals Genetic Predisposition to Disease Allele Molecular Biology Genetics Homozygote Cell Biology Cell Transformation Neoplastic Phenotype Chromosome 3 Genetic Loci Carcinogens Colorectal Neoplasms Carcinogenesis Molecular Chaperones Developmental Biology |
Zdroj: | Cell Cycle. 10:1739-1749 |
ISSN: | 1551-4005 1538-4101 |
Popis: | Colorectal cancer (CRC) is a multistep disease that involves a two-way interaction between a complex genetic pre-disposition component, and a set of poorly understood extrinsic environmental factors. In mice, CRC can be induced by treatment with azoxymethane (AOM). Using a set of AcB/BcA recombinant congenic strains derived from CRC-susceptible A/J and CRC-resistant C57Bl/6J (B6) progenitors, we previously detected the Ccs3 locus (colon cancer susceptibility locus 3) as a major regulator of CRC susceptibility. Phenotyping of additional AcB/BcA strains for susceptibility to AOM-induced CRC has refined the Ccs3 interval to a 6.7 Mb segment on chromosome 3. In addition, the presence of intermediate susceptibility phenotypes in individual AcB/BcA strains suggested additional gene effects regulating CRC susceptibility in A/J and B6 strains. Those were investigated by linkage analysis and whole genome scanning in a set of 208 informative (B6 x A/J)F2 progeny, using tumor multiplicity as a quantitative measure of susceptibility. This analysis validated the important role of Ccs3 in regulating this trait, and additionally detected contribution from a second locus on the distal portion of chromosome 9 (LOD = 3.76), that was given the temporary designation of Ccs5. Ccs5 modulates tumor multiplicity in F2 animals bearing at least one A/J-derived susceptibility allele at Ccs3, with A/J-derived Ccs5 susceptibility alleles being inherited in a recessive manner. There is a strong additive effect of Ccs3 and Ccs5 on tumor multiplicity in F2 mice: mice doubly homozygotes for A/J or B6 alleles at Ccs3 and Ccs5 show tumor numbers similar to those of parental A/J and B6, respectively. Interestingly, the Ccs5 region overlaps several quantitative trait loci previously reported to regulate intestinal homeostasis and susceptibility to intestinal colitis in mice and humans. Our findings identify a novel two-locus system regulating CRC susceptibility in mice, of which the relevance to human CRC can now be tested experimentally. |
Databáze: | OpenAIRE |
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