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Epigenetically driven and early immune evasion in colorectal cancer evolution.

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Nature genetics 2025 Vol.57(12) p. 3039-3049
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Lakatos E, Gunasri V, Zapata L, Househam J, Heide T, Trahearn N, Swinyard O, Cisneros L, Lynn C, Mossner M, Kimberley C, Spiteri I, Cresswell GD, Llibre-Palomar G, Mitchison M, Maley CC, Jansen M, Rodriguez-Justo M, Bridgewater J, Baker AM, Sottoriva A, Graham TA

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Immune system control is a principal hurdle in cancer evolution.

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APA Lakatos E, Gunasri V, et al. (2025). Epigenetically driven and early immune evasion in colorectal cancer evolution.. Nature genetics, 57(12), 3039-3049. https://doi.org/10.1038/s41588-025-02349-1
MLA Lakatos E, et al.. "Epigenetically driven and early immune evasion in colorectal cancer evolution.." Nature genetics, vol. 57, no. 12, 2025, pp. 3039-3049.
PMID 41193656

Abstract

Immune system control is a principal hurdle in cancer evolution. The temporal dynamics of immune evasion remain incompletely characterized, and how immune-mediated selection interrelates with epigenome alteration is unclear. Here we infer the genome- and epigenome-driven evolutionary dynamics of tumor-immune coevolution within primary colorectal cancers (CRCs). We utilize a multiregion multiomic dataset of matched genome, transcriptome and chromatin accessibility profiling from 495 single glands (from 29 CRCs) supplemented with high-resolution spatially resolved neoantigen sequencing data and multiplexed imaging of the tumor microenvironment from 82 microbiopsies within 11 CRCs. Somatic chromatin accessibility alterations contribute to accessibility loss of antigen-presenting genes and silencing of neoantigens. Immune escape and exclusion occur at the outset of CRC formation, and later intratumoral differences in immuno-editing are negligible or exclusive to sites of invasion. Collectively, immune evasion in CRC follows a 'Big Bang' evolutionary pattern, whereby it is acquired close to transformation and defines subsequent cancer-immune evolution.

MeSH Terms

Epigenesis, Genetic; Tumor Escape; Colorectal Neoplasms; Humans; Datasets as Topic; Multiomics; Neoplasm Invasiveness; Antigen Presentation; Transcription, Genetic