Systematic analysis of functional genetic and epigenetic variants in colorectal cancer.
1/5 보강
Colorectal cancer (CRC) is a leading cause of cancer-related mortality worldwide, yet the functional impact of noncoding variants on enhancer activity remains largely unexplored.
APA
Chen E, Yang Q, et al. (2026). Systematic analysis of functional genetic and epigenetic variants in colorectal cancer.. Science advances, 12(8), eaeb2473. https://doi.org/10.1126/sciadv.aeb2473
MLA
Chen E, et al.. "Systematic analysis of functional genetic and epigenetic variants in colorectal cancer.." Science advances, vol. 12, no. 8, 2026, pp. eaeb2473.
PMID
41719390 ↗
Abstract 한글 요약
Colorectal cancer (CRC) is a leading cause of cancer-related mortality worldwide, yet the functional impact of noncoding variants on enhancer activity remains largely unexplored. In this study, we adapted and applied two high-throughput techniques, SNP-STARR-seq and Methyl-STARR-seq, to systematically evaluate the influence of 30,790 noncoding SNPs and more than 134,000 CpG sites on enhancer activity in primary and metastatic CRC cells. We identified 922 SNPs and 487 CpG-containing elements modulating enhancer activity in primary cells and found 3136 SNPs and 3008 methylation-sensitive elements with metastasis-specific regulatory effects. Multi-omics integration linked these variants to target genes, and CRISPR editing validated their roles in driving tumorigenic and metastatic phenotypes. Furthermore, we identified two CRC-specific hypermethylated loci, cg08640619 and cg25982657, as exceptional tissue-based early detection biomarkers (AUC > 0.96). Mechanistically, hypermethylation at cg08640619 disrupts RUNX2 binding, leading to inhibition of and . Our study provides a comprehensive platform for understanding how genetic and epigenetic variants disrupt transcriptional programs in CRC, offering insights into disease susceptibility and identifying potential diagnostic and therapeutic targets.
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