Mms22p protects Saccharomyces cerevisiae from DNA damage induced by topoisomerase II

E. L. Baldwin¹, A. C. Berger³, A. H. Corbett³ and N. Osheroff¹^,2^,*

¹ Department of Biochemistry, Vanderbilt University School of Medicine Nashville, TN 37232-0146, USA ² Department of Medicine (Hematology/Oncology), Vanderbilt University School of Medicine Nashville, TN 37232-0146, USA ³ Department of Biochemistry, Emory University School of Medicine Atlanta, GA 30322, USA

^*To whom correspondence should be addressed at Department of Biochemistry, 654 Robinson Research Building, Vanderbilt University School of Medicine, Nashville, TN 37232-0146, USA. Tel: +615 322 4338; Fax: +615 343 1166; Email: neil.osheroff{at}vanderbilt.edu

Received November 19, 2004. Accepted January 24, 2005.

The cleavage reaction of topoisomerase II, which creates double-strandedDNA breaks, plays a central role in both the cure and initiationof cancer. Therefore, it is important to understand the cellularprocesses that repair topoisomerase II-generated DNA damage.Using a genome-wide approach with Saccharomyces cerevisiae,we found that ${Delta}$ mre11, ${Delta}$ xrs2, ${Delta}$ rad50, ${Delta}$ rad51, ${Delta}$ rad52, ${Delta}$ rad54, ${Delta}$ rad55, ${Delta}$ rad57 and ${Delta}$ mms22 strains were hypersensitive to etoposide, adrug that specifically increases levels of topoisomerase II-mediatedDNA breaks. These results confirm that the single-strand invasionpathway of homologous recombination is the major pathway thatrepairs topoisomerase II-induced DNA damage in yeast and alsoindicate an important role for Mms22p. Although ${Delta}$ mms22 strainsare sensitive to several DNA-damaging agents, little is knownabout the function of Mms22p. ${Delta}$ mms22 cultures accumulate in G₂/M,and display an abnormal cell cycle response to topoisomeraseII-mediated DNA damage. MMS22 appears to function outside ofthe single-strand invasion pathway, but levels of etoposide-inducedhomologous recombination in ${Delta}$ mms22 cells are lower than wild-type.MMS22 is epistatic with RTT101 and RTT107, genes that encodeits protein binding partners. Finally, consistent with a rolein DNA processes, Mms22p localizes to discrete nuclear foci,even in the absence of etoposide or its binding partners.

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Mms22p protects Saccharomyces cerevisiae from DNA damage induced by topoisomerase II