Publication | Open Access
FANCJ Is a Structure-specific DNA Helicase Associated with the Maintenance of Genomic G/C Tracts
243
Citations
27
References
2008
Year
GeneticsGenomic MechanismMolecular BiologyMolecular GeneticsGenomic G/c TractsFanconi AnemiaGene StructureGenome InstabilityGenome StructureDna ReplicationNuclear OrganizationChromosomal RearrangementCell BiologyStructural BiologyChromatinG4 DnaChromatin RemodelingNatural SciencesFancj G4Medicine
Fanconi anemia (FA) is a heritable human cancer-susceptibility disorder, delineating a genetically heterogenous pathway for the repair of replication-blocking lesions such as interstrand DNA cross-links. Here we demonstrate that one component of this pathway, FANCJ, is a structure-specific DNA helicase that dissociates guanine quadruplex DNA (G4 DNA) in vitro. Moreover, in contrast with previously identified G4 DNA helicases, such as the Bloom's helicase (BLM), FANCJ unwinds G4 substrates with 5'-3' polarity. In the FA-J human patient cell line EUFA0030 the loss of FANCJ G4 unwinding function correlates with the accumulation of large genomic deletions in the vicinity of sequences, which match the G4 DNA signature. Together these findings support a role for FANCJ in the maintenance of potentially unstable genomic G/C tracts during replication.
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