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. 2024 Dec;636(8041):233-240.
doi: 10.1038/s41586-024-08133-1. Epub 2024 Oct 30.

Polyclonal-to-monoclonal transition in colorectal precancerous evolution

Zhaolian Lu #  1   2 Shanlan Mo #  1   2 Duo Xie #  1   3 Xiangwei Zhai #  4 Shanjun Deng #  4 Kantian Zhou  1   2 Kun Wang  1   5   6 Xueling Kang  1   2 Hao Zhang  1   2 Juanzhen Tong  1   2 Liangzhen Hou  1   3 Huijuan Hu  1 Xuefei Li  1 Da Zhou  5   6 Leo Tsz On Lee  3   7 Li Liu  4 Yaxi Zhu  8 Jing Yu  9   10 Ping Lan  9   10 Jiguang Wang  2   11 Zhen He  12   13 Xionglei He  14 Zheng Hu  15   16
Affiliations

Polyclonal-to-monoclonal transition in colorectal precancerous evolution

Zhaolian Lu et al. Nature. 2024 Dec.

Abstract

Unravelling the origin and evolution of precancerous lesions is crucial for effectively preventing malignant transformation, yet our current knowledge remains limited1-3. Here we used a base editor-enabled DNA barcoding system4 to comprehensively map single-cell phylogenies in mouse models of intestinal tumorigenesis induced by inflammation or loss of the Apc gene. Through quantitative analysis of high-resolution phylogenies including 260,922 single cells from normal, inflamed and neoplastic intestinal tissues, we identified tens of independent cell lineages undergoing parallel clonal expansions within each lesion. We also found polyclonal origins of human sporadic colorectal polyps through bulk whole-exome sequencing and single-gland whole-genome sequencing. Genomic and clinical data support a model of polyclonal-to-monoclonal transition, with monoclonal lesions representing a more advanced stage. Single-cell RNA sequencing revealed extensive intercellular interactions in early polyclonal lesions, but there was significant loss of interactions during monoclonal transition. Therefore, our data suggest that colorectal precancer is often founded by many different lineages and highlight their cooperative interactions in the earliest stages of cancer formation. These findings provide insights into opportunities for earlier intervention in colorectal cancer.

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Conflict of interest statement

Competing interests: The authors declare no competing interests.

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