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Surveillance of Barrett’s oesophagus allows us to study the evolutionary dynamics of a human neoplasm over time. Here we use multicolour fluorescence in situ hybridization on brush cytology specimens, from two time points with a median interval of 37 months

Surveillance of Barrett’s oesophagus allows us to study the evolutionary dynamics of a human neoplasm over time. Here we use multicolour fluorescence in situ hybridization on brush cytology specimens, from two time points with a median interval of 37 months in 195 non-dysplastic Barrett's patients, and a third time point in a subset of 90 patients at a median interval of 36 months, to study clonal evolution at single-cell resolution. Baseline genetic diversity predicts progression and remains in a stable dynamic equilibrium over time. Clonal expansions are rare, being detected once every 36.8 patient years, and growing at an average rate of 1.58 cm[superscript 2] (95% CI: 0.09–4.06) per year, often involving the p16 locus. This suggests a lack of strong clonal selection in Barrett’s and that the malignant potential of ‘benign’ Barrett’s lesions is predetermined, with important implications for surveillance programs.

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    Title
    • Dynamic Clonal Equilibrium and Predetermined Cancer Risk in Barrett’s Oesophagus
    Date Created
    2016-08-19
    Resource Type
  • Text
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    Identifier
    • Digital object identifier: 10.1038/ncomms12158
    • Identifier Type
      International standard serial number
      Identifier Value
      2041-1723
    Note
    • The final version of this article, as published in Nature Communications, can be viewed online at: https://www.nature.com/articles/ncomms12158

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    Martinez, P., Timmer, M. R., Lau, C. T., Calpe, S., Sancho-Serra, M. D., Straub, D., . . . Krishnadath, K. K. (2016). Dynamic clonal equilibrium and predetermined cancer risk in Barrett’s oesophagus. Nature Communications, 7, 12158. doi:10.1038/ncomms12158

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