Article

  • The EMBO Journal (2007) 26, 3397 - 3409
  • doi:10.1038/sj.emboj.7601777

Published online: 28 June 2007

BLM is required for faithful chromosome segregation and its localization defines a class of ultrafine anaphase bridges

Kok-Lung Chan1, Phillip S North1 and Ian D Hickson1

  1. Cancer Research UK Laboratories, Weatherall Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, Oxford, UK

Correspondence to:

Ian D Hickson, Cancer Research UK Oxford Cancer Centre, Weatherall Institute of Molecular Medicine, University of Oxford, John Radcliffe Hospital, Oxford OX3 9DS, UK. Tel.: +44 1865 222 417; Fax: +44 1865 222 431; E-mail: ian.hickson@cancer.org.uk

Received 15 January 2007; Accepted 31 May 2007


Mutations in BLM cause Bloom's syndrome, a disorder associated with cancer predisposition and chromosomal instability. We investigated whether BLM plays a role in ensuring the faithful chromosome segregation in human cells. We show that BLM-defective cells display a higher frequency of anaphase bridges and lagging chromatin than do isogenic corrected derivatives that eptopically express the BLM protein. In normal cells undergoing mitosis, BLM protein localizes to anaphase bridges, where it colocalizes with its cellular partners, topoisomerase IIIalpha and hRMI1 (BLAP75). Using BLM staining as a marker, we have identified a class of ultrafine DNA bridges in anaphase that are surprisingly prevalent in the anaphase population of normal human cells. These so-called BLM–DNA bridges, which also stain for the PICH protein, frequently link centromeric loci, and are present at an elevated frequency in cells lacking BLM. On the basis of these results, we propose that sister-chromatid disjunction is often incomplete in human cells even after the onset of anaphase. We present a model for the action of BLM in ensuring complete sister chromatid decatenation in anaphase.

  • Keywords:

    • anaphase bridges,
    • Bloom's syndrome,
    • centromeres,
    • chromosome segregation,
    • PICH helicase
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