Human RECQ1 interacts with Ku70/80 and modulates DNA end-joining of double-strand breaks.

[werner syndrome]

Genomic instability is a known precursor to cancer and aging . The RecQ helicases are a highly conserved family of DNA-unwinding enzymes that play key roles in maintaining genome stability in all living organisms . Human RecQ homologs include RECQ 1 , BLM , WRN , RECQ 4 , and RECQ 5 Î² , three of which have been linked to diseases with elevated risk of cancer and growth defects (Bloom Syndrome and Rothmund-Thomson Syndrome ) or premature aging (Werner Syndrome ). RECQ 1 , the first RecQ helicase discovered and the most abundant in human cells , is the least well understood of the five human RecQ homologs . We have previously described that knockout of RECQ 1 in mice or knockdown of its expression in human cells results in elevated frequency of spontaneous sister chromatid exchanges , chromosomal instability , increased load of DNA damage and heightened sensitivity to ionizing radiation . We have now obtained evidence implicating RECQ 1 in the nonhomologous end-joining pathway of DNA double -strand break repair . We show that RECQ 1 interacts directly with the Ku 70 /80 subunit of the DNA-PK complex , and depletion of RECQ 1 results in reduced end-joining in cell free extracts . In vitro , RECQ 1 binds and unwinds the Ku 70 /80 -bound partial duplex DNA substrate efficiently . Linear DNA is co -bound by RECQ 1 and Ku 70 /80 , and DNA binding by Ku 70 /80 is modulated by RECQ 1 . Collectively , these results provide the first evidence for an interaction of RECQ 1 with Ku 70 /80 and a role of the human RecQ helicase in double -strand break repair through nonhomologous end-joining .

Diseases
Validation

Diseases presenting "bound partial duplex dna substrate" symptom

werner syndrome

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