4.8 Article

Quantitative evidence for early metastatic seeding in colorectal cancer

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NATURE GENETICS
卷 51, 期 7, 页码 1113-+

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NATURE PORTFOLIO
DOI: 10.1038/s41588-019-0423-x

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资金

  1. National Institutes of Health through the NIH Director's Pioneer Award [DP1-CA238296]
  2. NCI Cancer Target Discovery and Development Network [CA217851]
  3. American Cancer Society [IRG-58-007-54]
  4. Emerson Collective Cancer Research Fund
  5. Innovative Genomics Initiative (IGI) Postdoctoral Fellowship
  6. Cancer Center Support Grants from the National Cancer Institute [P30CA124435]
  7. University of Southern California Norris Comprehensive Cancer Center [P30CA014089]

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Both the timing and molecular determinants of metastasis are unknown, hindering treatment and prevention efforts. Here we characterize the evolutionary dynamics of this lethal process by analyzing exome-sequencing data from 118 biopsies from 23 patients with colorectal cancer with metastases to the liver or brain. The data show that the genomic divergence between the primary tumor and metastasis is low and that canonical driver genes were acquired early. Analysis within a spatial tumor growth model and statistical inference framework indicates that early disseminated cells commonly (81%07 out of 21evaluable patients) seed metastases while the carcinoma is clinically undetectable (typically, less than 0.01cm(3)). We validated the association between early drivers and metastasis in an independent cohort of 2,751 colorectal cancers, demonstrating their utility as biomarkers of metastasis. This conceptual and analytical framework provides quantitative in vivo evidence that systemic spread can occur early in colorectal cancer and illuminates strategies for patient stratification and therapeutic targeting of the canonical drivers of tumorigenesis.

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