Fission yeast Rnf4 homologs are required for DNA repair

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Abstract

We describe two RING finger proteins in the fission yeast Schizosaccharomyces pombe, Rfp1 and Rfp2. We show that these proteins function redundantly in DNA repair. Rfp1 was isolated as a Chk1-interacting protein in a two-hybrid screen and has high amino acid sequence similarity to Rfp2. Deletion of either gene does not cause a phenotype, but a double deletion (rfp1Δrfp2Δ) showed poor viability and defects in cell cycle progression. These cells are also sensitive to DNA-damaging agents, although they maintained normal checkpoint signaling to Chk1. Rfp1 and Rfp2 are most closely related to human Rnf4, and we showed that Rnf4 can substitute functionally for Rfp1 and/or Rfp2. The double mutants also showed significantly increased levels of protein SUMOylation, and we identified an S. pombe Ulp2/Smt4 homolog that, when overexpressed, reduced SUMO levels and suppressed the DNA damage sensitivity of rfp1Δ rfp2Δ cells. © 2007 by The American Society for Biochemistry and Molecular Biology, Inc.

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Kosoy, A., Calonge, T. M., Outwin, E. A., & O’Connell, M. J. (2007). Fission yeast Rnf4 homologs are required for DNA repair. Journal of Biological Chemistry, 282(28), 20388–20394. https://doi.org/10.1074/jbc.M702652200

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