Saccharomyces cerevisiae Checkpoint Genes MEC1, RAD17 and RAD24 Are Required for Normal Meiotic Recombination Partner Choice

Saccharomyces cerevisiae Checkpoint Genes MEC1, RAD17 and RAD24 Are Required for Normal Meiotic Recombination Partner Choice

Jeremy M. Grushcow^a, Teresa M. Holzen^a, Ken J. Park^a, Ted Weinert^b, Michael Lichten^c, and Douglas K. Bishop^a
^a Departments of Radiation and Cellular Oncology and Molecular Genetics and Cell Biology, University of Chicago, Chicago, Illinois 60637,
^b Department of Molecular and Cellular Biology, University of Arizona, Tucson, Arizona 85721
^c Laboratory of Biochemistry, Division of Cancer Biology, Diagnosis and Centers, National Cancer Institute, Bethesda, Maryland 20892

Corresponding author: Douglas K. Bishop, Department of Radiation and Cellular Oncology, University of Chicago Medical Center, 5841 S. Maryland Ave., MC1105, Chicago, IL 60637., dbishop{at}midway.uchicago.edu (E-mail)

Communicating editor: L. S. SYMINGTON

Checkpoint gene function prevents meiotic progression when recombinationis blocked by mutations in the recA homologue DMC1. Bypass ofdmc1 arrest by mutation of the DNA damage checkpoint genes MEC1,RAD17, or RAD24 results in a dramatic loss of spore viability,suggesting that these genes play an important role in monitoringthe progression of recombination. We show here that the roleof mitotic checkpoint genes in meiosis is not limited to maintainingarrest in abnormal meioses; mec1-1, rad24, and rad17 singlemutants have additional meiotic defects. All three mutants displayZip1 polycomplexes in two- to threefold more nuclei than observedin wild-type controls, suggesting that synapsis may be aberrant.Additionally, all three mutants exhibit elevated levels of ectopicrecombination in a novel physical assay. rad17 mutants alsoalter the fraction of recombination events that are accompaniedby an exchange of flanking markers. Crossovers are associatedwith up to 90% of recombination events for one pair of allelesin rad17, as compared with 65% in wild type. Meiotic progressionis not required to allow ectopic recombination in rad17 mutants,as it still occurs at elevated levels in ndt80 mutants thatarrest in prophase regardless of checkpoint signaling. Theseobservations support the suggestion that MEC1, RAD17, and RAD24,in addition to their proposed monitoring function, act to promotenormal meiotic recombination.

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				G. S. Brush, D. M. Clifford, S. M. Marinco, and A. J. Bartrand Replication protein A is sequentially phosphorylated during meiosis Nucleic Acids Res., December 1, 2001; 29(23): 4808 - 4817. [Abstract] [Full Text] [PDF]

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				V. Paciotti, M. Clerici, M. Scotti, G. Lucchini, and M. P. Longhese Characterization of mec1 Kinase-Deficient Mutants and of New Hypomorphic mec1 Alleles Impairing Subsets of the DNA Damage Response Pathway Mol. Cell. Biol., June 15, 2001; 21(12): 3913 - 3925. [Abstract] [Full Text]

				F. Hu, A. A. Alcasabas, and S. J. Elledge Asf1 links Rad53 to control of chromatin assembly Genes & Dev., May 1, 2001; 15(9): 1061 - 1066. [Abstract] [Full Text]

				H. Scherthan, M. Jerratsch, S. Dhar, Y. A. Wang, S. P. Goff, and T. K. Pandita Meiotic Telomere Distribution and Sertoli Cell Nuclear Architecture Are Altered in Atm- and Atm-p53-Deficient Mice Mol. Cell. Biol., October 15, 2000; 20(20): 7773 - 7783. [Abstract] [Full Text]

				E. Trelles-Sticken, M. E. Dresser, and H. Scherthan Meiotic Telomere Protein Ndj1p Is Required for Meiosis-specific Telomere Distribution, Bouquet Formation and Efficient Homologue Pairing J. Cell Biol., October 3, 2000; 151(1): 95 - 106. [Abstract] [Full Text] [PDF]

				P. A. San-Segundo and G. S. Roeder Role for the Silencing Protein Dot1 in Meiotic Checkpoint Control Mol. Biol. Cell, October 1, 2000; 11(10): 3601 - 3615. [Abstract] [Full Text]

				A. S. H. Goldman and M. Lichten Restriction of ectopic recombination by interhomolog interactions during Saccharomyces cerevisiae meiosis PNAS, August 15, 2000; 97(17): 9537 - 9542. [Abstract] [Full Text] [PDF]

				V. Paciotti, M. Clerici, G. Lucchini, and M. P. Longhese The checkpoint protein Ddc2, functionally related to S. pombe Rad26, interacts with Mec1 and is regulated by Mec1-dependent phosphorylation in budding yeast Genes & Dev., August 15, 2000; 14(16): 2046 - 2059. [Abstract] [Full Text]

				V. I. Bashkirov, J. S. King, E. V. Bashkirova, J. Schmuckli-Maurer, and W.-D. Heyer DNA Repair Protein Rad55 Is a Terminal Substrate of the DNA Damage Checkpoints Mol. Cell. Biol., June 15, 2000; 20(12): 4393 - 4404. [Abstract] [Full Text]

				D. A. Thompson and F. W. Stahl Genetic Control of Recombination Partner Preference in Yeast Meiosis: Isolation and Characterization of Mutants Elevated for Meiotic Unequal Sister-Chromatid Recombination Genetics, October 1, 1999; 153(2): 621 - 641. [Abstract] [Full Text] [PDF]