1. Identification of five novel modifier loci of ApcMin harbored in the BXH14 recombinant inbred strain
- Author
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Julie Innocent, Rayneisha Watson, Stephanie C. Nnadi, Arthur M. Buchberg, Gregory E. Gonye, and Linda D. Siracusa
- Subjects
Male ,Cancer Research ,Genes, APC ,Colon ,Adenomatous polyposis coli ,Mice, Inbred Strains ,Genome-wide association study ,Familial adenomatous polyposis ,Mice ,Germline mutation ,Inbred strain ,Gene interaction ,Intestine, Small ,medicine ,Animals ,Allele ,Germ-Line Mutation ,Genetics ,Original Paper ,biology ,Intestinal Polyps ,Recombinant inbred strain ,General Medicine ,medicine.disease ,biology.protein ,Female - Abstract
Every year thousands of people in the USA are diagnosed with small intestine and colorectal cancers (CRC). Although environmental factors affect disease etiology, uncovering underlying genetic factors is imperative for risk assessment and developing preventative therapies. Familial adenomatous polyposis is a heritable genetic disorder in which individuals carry germ-line mutations in the adenomatous polyposis coli (APC) gene that predisposes them to CRC. The Apc ( Min ) mouse model carries a point mutation in the Apc gene and develops polyps along the intestinal tract. Inbred strain background influences polyp phenotypes in Apc ( Min ) mice. Several Modifier of Min (Mom) loci that alter tumor phenotypes associated with the Apc ( Min ) mutation have been identified to date. We screened BXH recombinant inbred (RI) strains by crossing BXH RI females with C57BL/6J (B6) Apc ( Min ) males and quantitating tumor phenotypes in backcross progeny. We found that the BXH14 RI strain harbors five modifier loci that decrease polyp multiplicity. Furthermore, we show that resistance is determined by varying combinations of these modifier loci. Gene interaction network analysis shows that there are multiple networks with proven gene-gene interactions, which contain genes from all five modifier loci. We discuss the implications of this result for studies that define susceptibility loci, namely that multiple networks may be acting concurrently to alter tumor phenotypes. Thus, the significance of this work resides not only with the modifier loci we identified but also with the combinations of loci needed to get maximal protection against polyposis and the impact of this finding on human disease studies.
- Published
- 2012