Journal article icon

Journal article

ATR activation and replication fork restart are defective in FANCM-deficient cells

Abstract:
Fanconi anaemia is a chromosomal instability disorder associated with cancer predisposition and bone marrow failure. Among the 13 identified FA gene products only one, the DNA translocase FANCM, has homologues in lower organisms, suggesting a conserved function in DNA metabolism. However, a precise role for FANCM in DNA repair remains elusive. Here, we show a novel function for FANCM that is distinct from its role in the FA pathway: promoting replication fork restart and simultaneously limiting the accumulation of RPA-ssDNA. We show that in DT40 cells this process is controlled by ATR and PLK1, and that in the absence of FANCM, stalled replication forks are unable to resume DNA synthesis and genome duplication is ensured by excess origin firing. Unexpectedly, we also uncover an early role for FANCM in ATR-mediated checkpoint signalling by promoting chromatin retention of TopBP1. Failure to retain TopBP1 on chromatin impacts on the ability of ATR to phosphorylate downstream molecular targets, including Chk1 and SMC1. Our data therefore indicate a fundamental role for FANCM in the maintenance of genome integrity during S phase. © 2010 European Molecular Biology Organization.

Actions

Access Document

Publisher copy:
10.1038/emboj.2009.385

Authors


Journal:
EMBO Journal More from this journal
Volume:
29
Issue:
4
Pages:
806-818
Publication date:
2010-02-01
DOI:
EISSN:
1460-2075
ISSN:
0261-4189


Language:
English
Keywords:
Pubs id:
pubs:178946
UUID:
uuid:1b73267e-af8a-4b9d-9179-91f7a8599611
Local pid:
pubs:178946
Source identifiers:
178946
Deposit date:
2012-12-19
ARK identifier:

Terms of use


Views and Downloads






If you are the owner of this record, you can report an update to it here: Report update to this record

TO TOP