Contribution of pks+E. coli mutations to colorectal carcinogenesis

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Bingjie Chen
Daniele Ramazzotti
Timon Heide
Inmaculada Spiteri
Javier Fernandez-Mateos
Chela James
Luca Magnani
Trevor A. Graham
Andrea Sottoriva
机构
[1] The Institute of Cancer Research,Centre for Evolution and Cancer
[2] Guangzhou Medical University,GMU
[3] University of Milano-Bicocca,GIBH Joint School of Life Sciences, The Guangdong
[4] Human Technopole,Hong Kong
[5] The Institute of Cancer Research,Macau Joint Laboratory for Cell Fate Regulation and Diseases
[6] Imperial College London,Department of Medicine and Surgery
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The dominant mutational signature in colorectal cancer genomes is C > T deamination (COSMIC Signature 1) and, in a small subgroup, mismatch repair signature (COSMIC signatures 6 and 44). Mutations in common colorectal cancer driver genes are often not consistent with those signatures. Here we perform whole-genome sequencing of normal colon crypts from cancer patients, matched to a previous multi-omic tumour dataset. We analyse normal crypts that were distant vs adjacent to the cancer. In contrast to healthy individuals, normal crypts of colon cancer patients have a high incidence of pks + (polyketide synthases) E.coli (Escherichia coli) mutational and indel signatures, and this is confirmed by metagenomics. These signatures are compatible with many clonal driver mutations detected in the corresponding cancer samples, including in chromatin modifier genes, supporting their role in early tumourigenesis. These results provide evidence that pks + E.coli is a potential driver of carcinogenesis in the human gut.
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