Chimeric Saccharomyces cerevisiae Msh6 protein with an Msh3 mispair-binding domain combines properties of both proteins

  1. Scarlet S. Shell*,,,§,
  2. Christopher D. Putnam*, and
  3. Richard D. Kolodner*,,,§,
  1. *Ludwig Institute for Cancer Research,
  2. Departments of Medicine and
  3. Cellular and Molecular Medicine, and
  4. §Cancer Center, University of California at San Diego, 9500 Gilman Drive, La Jolla, CA 92093-0669

  1. Contributed by Richard D. Kolodner, May 10, 2007 (received for review March 30, 2007)

Abstract

Msh2–Msh3 and Msh2–Msh6 are two partially redundant mispair-recognition complexes that initiate mismatch repair in eukaryotes. Crystal structures of the prokaryotic homolog MutS suggest the mechanism by which Msh6 interacts with mispairs because key mispair-contacting residues are conserved in these two proteins. Because Msh3 lacks these conserved residues, we constructed a series of mutants to investigate the requirements for mispair interaction by Msh3. We found that a chimeric protein in which the mispair-binding domain (MBD) of Msh6 was replaced by the equivalent domain of Msh3 was functional for mismatch repair. This chimera possessed the mispair-binding specificity of Msh3 and revealed that communication between the MBD and the ATPase domain is conserved between Msh2–Msh3 and Msh2–Msh6. Further, the chimeric protein retained Msh6-like properties with respect to genetic interactions with the MutL homologs and an Msh2 MBD deletion mutant, indicating that Msh3-like behaviors beyond mispair specificity are not features controlled by the MBD.

Footnotes

  • To whom correspondence should be addressed. E-mail: rkolodner{at}ucsd.edu

  • Author contributions: S.S.S., C.D.P., and R.D.K. designed research; S.S.S. and C.D.P. performed research; S.S.S., C.D.P., and R.D.K. analyzed data; and S.S.S., C.D.P., and R.D.K. wrote the paper.

  • The authors declare no conflict of interest.

  • This article contains supporting information online at www.pnas.org/cgi/content/full/0704148104/DC1.

  • Abbreviations:
    CSM,
    complete supplement mixture;
    MBD,
    mispair-binding domain;
    MMR,
    mismatch repair;
    MSH,
    MutS homolog;
    SPR,
    surface plasma resonance;
    YPD,
    yeast extract/peptone/dextrose.
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  1. Published online before print June 15, 2007, doi: 10.1073/pnas.0704148104 PNAS June 26, 2007 vol. 104 no. 26 10956-10961
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