PLoS ONE (Jan 2011)

Next-generation sequencing of apoptotic DNA breakpoints reveals association with actively transcribed genes and gene translocations.

  • Melissa J Fullwood,
  • Joanne Lee,
  • Lifang Lin,
  • Guoliang Li,
  • Mikael Huss,
  • Patrick Ng,
  • Wing-Kin Sung,
  • Shirish Shenolikar

DOI
https://doi.org/10.1371/journal.pone.0026054
Journal volume & issue
Vol. 6, no. 11
p. e26054

Abstract

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DNA fragmentation is a well-recognized hallmark of apoptosis. However, the precise DNA sequences cleaved during apoptosis triggered by distinct mechanisms remain unclear. We used next-generation sequencing of DNA fragments generated in Actinomycin D-treated human HL-60 leukemic cells to generate a high-throughput, global map of apoptotic DNA breakpoints. These data highlighted that DNA breaks are non-random and show a significant association with active genes and open chromatin regions. We noted that transcription factor binding sites were also enriched within a fraction of the apoptotic breakpoints. Interestingly, extensive apoptotic cleavage was noted within genes that are frequently translocated in human cancers. We speculate that the non-random fragmentation of DNA during apoptosis may contribute to gene translocations and the development of human cancers.