Cancer Research Annual Meeting 2010  Protein Translation and Cancer
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[Cancer Research 63, 7136-7146, November 1, 2003]
© 2003 American Association for Cancer Research


Regular Articles

Werner Protein Stimulates Topoisomerase I DNA Relaxation Activity

Jean-Philippe Laine1, Patricia L. Opresko1, Fred E. Indig, Jeanine A. Harrigan, Cayetano von Kobbe and Vilhelm A. Bohr2

Laboratory of Molecular Gerontology, National Institute on Aging, NIH, Baltimore, Maryland 21224 [J-P. L., P. L. O., F. E. I., J. A. H., C. v. K., V. A. B.], and Institut de Genetique et de Biologie Moleculaire et Cellulaire, Illkirch, France [J-P. L.]

Werner syndrome (WS) is a human premature aging disorder characterized by the early onset of age-related clinical features and an elevated incidence of cancer. The Werner protein (WRN) belongs to the RecQ family of DNA helicases and is required for the maintenance of genomic stability in human cells. Potential cooperation between RecQ helicases and topoisomerases in many aspects of DNA metabolism, such as the progression of replication forks, transcription, recombination, and repair, has been reported. Here, we show a physical and functional interaction between WRN and topoisomerase I (topo I). WRN colocalizes and interacts directly with topo I. WRN stimulates the ability of topo I to relax negatively supercoiled DNA and specifically stimulates the religation step of the relaxation reaction. Moreover, cell extracts from WS fibroblasts exhibit a decrease in the relaxation activity of negatively supercoiled DNA. We have identified two regions of WRN that mediate functional interaction with topo I, and they are located at the NH2 and COOH termini of the WRN protein. In a reciprocal functional interaction, topo I inhibits the ATPase activity of WRN. Our data provide new insight into the interrelationship between RecQ helicases and topoisomerases in the maintenance of genomic integrity and prevention of tumorigenesis.




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