Probing Genome Maintenance Functions of human RECQ1.

[werner syndrome]

The RecQ helicases are a highly conserved family of DNA-unwinding enzymes that play key roles in protecting the genome stability in all kingdoms of life . Human RecQ homologs include RECQ 1 , BLM , WRN , RECQ 4 , and RECQ 5 Î² . Although the individual RecQ-related diseases are characterized by a variety of clinical features encompassing growth defects (Bloom Syndrome and Rothmund Thomson Syndrome ) to premature aging (Werner Syndrome ), all these patients have a high risk of cancer predisposition . Here , we present an overview of recent progress towards elucidating functions of RECQ 1 helicase , the most abundant but poorly characterized RecQ homolog in humans . Consistent with a conserved role in genome stability maintenance , deficiency of RECQ 1 results in elevated frequency of spontaneous sister chromatid exchanges , chromosomal instability , increased DNA damage and greater sensitivity to certain genotoxic stress . Delineating what aspects of RECQ 1 catalytic functions contribute to the observed cellular phenotypes , and how this is regulated is critical to establish its biological functions in DNA metabolism . Recent studies have identified functional specialization of RECQ 1 in DNA repair ; however , identification of fundamental similarities will be just as critical in developing a unifying theme for RecQ actions , allowing the functions revealed from studying one homolog to be extrapolated and generalized to other RecQ homologs .

Diseases
Validation

Diseases presenting "elevated frequency" symptom

cholangiocarcinoma

werner syndrome

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