Abstract:BackgroundThere is an increasing demand for accurate biomarkers for early non-invasive colorectal cancer detection. We employed a genome-scale marker discovery method to identify and verify candidate DNA methylation biomarkers for blood-based detection of colorectal cancer.Methodology/Principal FindingsWe used DNA methylation data from 711 colorectal tumors, 53 matched adjacent-normal colonic tissue samples, 286 healthy blood samples and 4,201 tumor samples of 15 different cancer types. DNA methylation data we… Show more
“…[13][14][15] Considerable effort has also been devoted to investigate mutational events that could explain cancer-related aberrant methylation through their effect on the epigenetic machinery. 16,17 Recently, the development of clinically relevant diagnostic tests for cancer based on methylation biomarkers measured in blood, urine, and other body fluids [18][19][20][21][22] have provided a glimpse into the biomedical applications that may become mainstream in the near future. 23 DNA methylation experiments performed by individual laboratories provide evidence for the identification of shared signatures of differential methylation that can separate tumors from normal controls.…”
(2013) Recurrent patterns of DNA methylation in the ZNF154, CASP8, and VHL promoters across a wide spectrum of human solid epithelial tumors and cancer cell lines, Epigenetics, 8:12, 1355Epigenetics, 8:12, -1372
“…[13][14][15] Considerable effort has also been devoted to investigate mutational events that could explain cancer-related aberrant methylation through their effect on the epigenetic machinery. 16,17 Recently, the development of clinically relevant diagnostic tests for cancer based on methylation biomarkers measured in blood, urine, and other body fluids [18][19][20][21][22] have provided a glimpse into the biomedical applications that may become mainstream in the near future. 23 DNA methylation experiments performed by individual laboratories provide evidence for the identification of shared signatures of differential methylation that can separate tumors from normal controls.…”
(2013) Recurrent patterns of DNA methylation in the ZNF154, CASP8, and VHL promoters across a wide spectrum of human solid epithelial tumors and cancer cell lines, Epigenetics, 8:12, 1355Epigenetics, 8:12, -1372
“…A number of methylation biomarkers have been found in circulating cell-free DNA (ccfDNA) in blood and are promising avenues to address this clinical need (10,(12)(13)(14)(15)(16)(17). Among those that have been rigorously studied, methylated SEPT9 6 (septin 9) is the most well characterized (18,19 ).…”
BACKGROUND: Epi proColon® is a new blood-based colorectal cancer (CRC) screening test designed to determine the methylation status of a promoter region of the SEPT9 (septin 9) gene in cell-free DNA isolated from plasma. We describe the analytical and clinical performance of the test.
“…However, there is definitive evidence suggesting the existence of epigenetic drivers, such as MLH1 CpG island promoter hypermethylation in colorectal cancer, which occur at high frequency and can stably propagate within cancer cells [45,48]. Accordingly, aberrant patterns of DNA methylation have been identified as cancer-specific biomarkers, and their clinical utility is actively being established [26,46,[49][50][51]. The most encouraging example is a multi-target stool DNA test developed by a company called Exact Science for colorectal cancer (CRC) early screening.…”
Section: Epigeneticsmentioning
confidence: 99%
“…Targeted sequencing of specific CpG island promoter regions is the most clinically relevant because many cancer-associated promoter hypermethylation patterns have been identified and used as cancer biomarkers [46,[49][50][51]. For example, by analyzing a panel of 10 selected cancer hypermethylation markers through methylation-specific PCR on cfDNA, a sensitivity of 91% was reached among recurrent stage IV breast cancer patients [51].…”
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