AI Article Synopsis

  • Research indicates that chromosome 8q24.21 is linked to an increased risk of colorectal cancer (CRC) based on studies involving both genome-wide associations and specific gene candidates.
  • A study involving over 5,400 individuals (2,713 CRC patients and 2,718 controls) identified significant associations with two SNPs (rs10505477 and rs6983267), showing an odds ratio of 1.50 for susceptibility to CRC.
  • The analysis highlighted a specific 17 kb genetic region as a key area of interest for CRC risk, particularly in tumors that are microsatellite instability-stable, where the odds ratio increased to 1.71.

Article Abstract

Human chromosome 8q24.21 has been implicated as a susceptibility region for colorectal cancer (CRC) as a result of genome-wide association and candidate gene studies. To assess the impact of molecular variants at 8q24.21 upon the CRC risk of German individuals and to refine the disease-associated region, a total of 2,713 patients with operated CRC (median age at diagnosis: 63 years) were compared with 2,718 sex-matched control individuals (median age at inclusion: 65 years). Information on microsatellite instability in tumors was available for 901 patients. Association analysis of SNPs rs10505477 and rs6983267 yielded allelic p-values of 1.42 x 10(-7) and 2.57 x 10(-7), respectively. For both polymorphisms, the odds ratio was estimated to be 1.50 (95% CI: 1.29-1.75) under a recessive disease model. The strongest candidate interval, outside of which significance dropped by more than 4 orders of magnitude, was delineated by SNPs rs10505477 and rs7014346 and comprised 17 kb. In a subgroup analysis, the disease association was found to be more pronounced in MSI-stable tumors (odds ratio: 1.71). Our study confirms the role of genetic variation at 8q24.21 as a risk factor for CRC and localizes the corresponding susceptibility gene to a 17 kb candidate region.

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Source
http://dx.doi.org/10.1002/ijc.23872DOI Listing

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