Abstract
Although serrated polyps were historically considered to pose little risk, it is now understood that progression down the serrated pathway could account for as many as 15%–35% of colorectal cancers. The sessile serrated adenoma/polyp (SSA/P) is the most prevalent pre-invasive serrated lesion. Our objective was to identify the CpG loci that are persistently hyper-methylated during serrated carcinogenesis, from the early SSA/P lesion through the later cancer phases of neoplasia development. We queried the loci hyper-methylated in serrated cancers within our right-sided SSA/Ps from the New Hampshire Colonoscopy Registry, using the Illumina Infinium Human Methylation 450 k panel to comprehensively assess the DNA methylation status. We identified CpG loci and regions consistently hyper-methylated throughout the serrated carcinogenesis spectrum, in both our SSA/P specimens and in serrated cancers. Hyper-methylated CpG loci included the known the tumor suppressor gene RET (p = 5.72 × 10−10), as well as loci in differentially methylated regions for GSG1L, MIR4493, NTNG1, MCIDAS, ZNF568, and RERG. The hyper-methylated loci that we identified help characterize the biology of SSA/P development, and could be useful as therapeutic targets, or for future identification of patients who may benefit from shorter surveillance intervals.
Highlights
Colorectal cancer (CRC) is the second leading cause of cancer death in the U.S [1], but is preventable with colonoscopic screening and polypectomy [2]
The characteristics of patients assessed for methylation were similar to those of right-sided sessile serrated adenoma/polyp (SSA/P) patients in the overall 2005–2008 registry population, with a slightly larger proportion of females (57%) and a mean age of 57 ± 6.9
We identified loci hyper-methylated in right-sided SSA/Ps that persist into serrated cancers using epigenome-wide, locus specific assessment
Summary
Colorectal cancer (CRC) is the second leading cause of cancer death in the U.S [1], but is preventable with colonoscopic screening and polypectomy [2]. Current recommendations for the interval between screening or surveillance examinations are based on the risks of cancer or adenomas after polypectomy. Serrated polyps, when previously all characterized as hyperplastic polyps, were not considered to have malignant potential. More than 70% of serrated lesions are hyperplastic polyps (HPs), while 4%–25% are sessile serrated adenomas/polyps (SSA/Ps), which are the main pre-invasive serrated lesion. These are predominantly found in the proximal colon [4,5]. Current models depict a major pathway for progression via the serrated pathway involving extensive DNA methylation [6]
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