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Machine learning enables pan-cancer identification of mutational hotspots at persistent CTCF binding sites. | LitMetric

AI Article Synopsis

  • CTCF is an important protein that helps control the 3D structure of DNA and gene expression, and its binding sites (CTCF-BSs) often mutate in cancer.
  • Researchers discovered a unique group of CTCF-BSs called persistent CTCF binding sites (P-CTCF-BSs) that resist changes and are highly conserved, potentially influencing cell structure.
  • The study found that P-CTCF-BSs have a higher mutation rate in breast and prostate cancer, and developed a machine learning tool (CTCF-INSITE) to predict mutations across various cancer types, confirming that these mutations can disrupt CTCF binding and affect genome organization.

Article Abstract

CCCTC-binding factor (CTCF) is an insulator protein that binds to a highly conserved DNA motif and facilitates regulation of three-dimensional (3D) nuclear architecture and transcription. CTCF binding sites (CTCF-BSs) reside in non-coding DNA and are frequently mutated in cancer. Our previous study identified a small subclass of CTCF-BSs that are resistant to CTCF knock down, termed persistent CTCF binding sites (P-CTCF-BSs). P-CTCF-BSs show high binding conservation and potentially regulate cell-type constitutive 3D chromatin architecture. Here, using ICGC sequencing data we made the striking observation that P-CTCF-BSs display a highly elevated mutation rate in breast and prostate cancer when compared to all CTCF-BSs. To address whether P-CTCF-BS mutations are also enriched in other cell-types, we developed CTCF-INSITE-a tool utilising machine learning to predict persistence based on genetic and epigenetic features of experimentally-determined P-CTCF-BSs. Notably, predicted P-CTCF-BSs also show a significantly elevated mutational burden in all 12 cancer-types tested. Enrichment was even stronger for P-CTCF-BS mutations with predicted functional impact to CTCF binding and chromatin looping. Using in vitro binding assays we validated that P-CTCF-BS cancer mutations, predicted to be disruptive, indeed reduced CTCF binding. Together this study reveals a new subclass of cancer specific CTCF-BS DNA mutations and provides insights into their importance in genome organization in a pan-cancer setting.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11317138PMC
http://dx.doi.org/10.1093/nar/gkae530DOI Listing

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