PLoS ONE (Jan 2014)

ATRX dysfunction induces replication defects in primary mouse cells.

  • David Clynes,
  • Clare Jelinska,
  • Barbara Xella,
  • Helena Ayyub,
  • Stephen Taylor,
  • Matthew Mitson,
  • Csanád Z Bachrati,
  • Douglas R Higgs,
  • Richard J Gibbons

DOI
https://doi.org/10.1371/journal.pone.0092915
Journal volume & issue
Vol. 9, no. 3
p. e92915

Abstract

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The chromatin remodeling protein ATRX, which targets tandem repetitive DNA, has been shown to be required for expression of the alpha globin genes, for proliferation of a variety of cellular progenitors, for chromosome congression and for the maintenance of telomeres. Mutations in ATRX have recently been identified in tumours which maintain their telomeres by a telomerase independent pathway involving homologous recombination thought to be triggered by DNA damage. It is as yet unknown whether there is a central underlying mechanism associated with ATRX dysfunction which can explain the numerous cellular phenomena observed. There is, however, growing evidence for its role in the replication of various repetitive DNA templates which are thought to have a propensity to form secondary structures. Using a mouse knockout model we demonstrate that ATRX plays a direct role in facilitating DNA replication. Ablation of ATRX alone, although leading to a DNA damage response at telomeres, is not sufficient to trigger the alternative lengthening of telomere pathway in mouse embryonic stem cells.