Interaction of the S phase regulator Cdc18 with cyclin-dependent kinase in fission yeast

  1. Grant W. Brown,
  2. Prasad V. Jallepalli,
  3. Brenda J. Huneycutt, and
  4. Thomas J. Kelly*
  1. Department of Molecular Biology and Genetics, Johns Hopkins University School of Medicine, Baltimore, MD 21205

Abstract

The fission yeast gene cdc18 + is required for entry into S phase and for coupling mitosis to the successful completion of S phase. Cdc18 is a highly unstable protein that is expressed only once per cell cycle at the G1/S boundary. Overexpression of Cdc18 causes a mitotic delay and reinitiation of DNA replication, suggesting that the inactivation of Cdc18 plays a role in preventing rereplication within a given cell cycle. In this paper, we present evidence that Cdc18 is associated with active cyclin-dependent kinase in vivo. We have expressed Cdc18 as a glutathione S-transferase fusion in fission yeast and demonstrated that the fusion protein is functional in vivo. We find that the Cdc18 fusion protein copurifies with a kinase activity capable of phosphorylating histone H1 and Cdc18. The activity was identified by a variety of methods as the cyclin-dependent kinase containing the product of the cdc2 + gene. The amino terminus of Cdc18 is required for association with cyclin-dependent kinase, but the association does not require the consensus cyclin-dependent kinase phosphorylation sites in this region. Additionally, both G1/S and mitotic forms of cyclin-dependent kinase phosphorylate and interact with Cdc18. These interactions between Cdc18 and cyclin-dependent kinases suggest mechanisms by which cyclin-dependent kinases could activate the initiation of DNA replication and could prevent rereplication.

Footnotes

  • * To whom reprint requests should be addressed. e-mail: tom_kelly{at}qmail.bs.jhu.edu.

  • Thomas J. Kelly

  • ABBREVIATIONS:
    cdk,
    cyclin-dependent kinase;
    GST,
    glutathione S-transferase;
    HA,
    hemaglutinin;
    NLS,
    nuclear localization sequence
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