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    The genomic landscape of 2,023 colorectal cancers

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    Authors
    Cornish, A. J.
    Gruber, Andreas J
    Kinnersley, B.
    Chubb, D.
    Frangou, A.
    Caravagna, G.
    Noyvert, B.
    Lakatos, E.
    Wood, H. M.
    Thorn, S.
    Culliford, R.
    Arnedo-Pac, C.
    Househam, J.
    Cross, W.
    Sud, A.
    Law, P.
    Leathlobhair, M. N.
    Hawari, Aliah
    Woolley, C.
    Sherwood, K.
    Feeley, N.
    Gül, G.
    Fernandez-Tajes, J.
    Zapata, L.
    Alexandrov, L. B.
    Murugaesu, N.
    Sosinsky, A.
    Mitchell, J.
    Lopez-Bigas, N.
    Quirke, P.
    Church, D. N.
    Tomlinson, I. P. M.
    Sottoriva, A.
    Graham, T. A.
    Wedge, David C
    Houlston, R. S.
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    Affiliation
    Manchester Cancer Research Centre, Division of Cancer Sciences, University of Manchester, Manchester, UK.
    Issue Date
    2024
    
    Metadata
    Show full item record
    Abstract
    Colorectal carcinoma (CRC) is a common cause of mortality(1), but a comprehensive description of its genomic landscape is lacking(2-9). Here we perform whole-genome sequencing of 2,023 CRC samples from participants in the UK 100,000 Genomes Project, thereby providing a highly detailed somatic mutational landscape of this cancer. Integrated analyses identify more than 250 putative CRC driver genes, many not previously implicated in CRC or other cancers, including several recurrent changes outside the coding genome. We extend the molecular pathways involved in CRC development, define four new common subgroups of microsatellite-stable CRC based on genomic features and show that these groups have independent prognostic associations. We also characterize several rare molecular CRC subgroups, some with potential clinical relevance, including cancers with both microsatellite and chromosomal instability. We demonstrate a spectrum of mutational profiles across the colorectum, which reflect aetiological differences. These include the role of Escherichia coli(pks+) colibactin in rectal cancers(10) and the importance of the SBS93 signature(11-13), which suggests that diet or smoking is a risk factor. Immune-escape driver mutations(14) are near-ubiquitous in hypermutant tumours and occur in about half of microsatellite-stable CRCs, often in the form of HLA copy number changes. Many driver mutations are actionable, including those associated with rare subgroups (for example, BRCA1 and IDH1), highlighting the role of whole-genome sequencing in optimizing patient care.
    Citation
    Cornish AJ, Gruber AJ, Kinnersley B, Chubb D, Frangou A, Caravagna G, et al. The genomic landscape of 2,023 colorectal cancers. Nature. 2024 Sep;633(8028):127-36. PubMed PMID: 39112709. Pubmed Central PMCID: PMC11374690 an employee of Biotheranostics. L.B.A. is also an inventor of a US Patent 10,776,718 for source identification by non-negative matrix factorization. L.B.A. declares US provisional applications with the following serial numbers: 63/289,601; 63/269,033; 63/366,392; 63/367,846; 63/412,835. A.J.C. is an employee of Owkin UK Ltd. All other authors declare they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper. Epub 2024/08/08. eng.
    Journal
    Nature
    URI
    http://hdl.handle.net/10541/627183
    DOI
    10.1038/s41586-024-07747-9
    PubMed ID
    39112709
    Additional Links
    https://dx.doi.org/10.1038/s41586-024-07747-9
    Type
    Article
    Language
    en
    ae974a485f413a2113503eed53cd6c53
    10.1038/s41586-024-07747-9
    Scopus Count
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