Cell cycle regulation of the yeast Cdc7 protein kinase by association with the Dbf4 protein.

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Mol Cell Biol. 1993 May; 13(5): 2899-2908

Cell cycle regulation of the yeast Cdc7 protein kinase by association with the Dbf4 protein.

A L Jackson, P M Pahl, K Harrison, J Rosamond and R A Sclafani

Department of Biochemistry, Biophysics, and Genetics, University of Colorado Health Sciences Center, Denver 80262.

ABSTRACT

Yeast Cdc7 protein kinase and Dbf4 protein are both requiredfor the initiation of DNA replication at the G1/S phase boundaryof the mitotic cell cycle. Cdc7 kinase function is stage-specificin the cell cycle, but total Cdc7 protein levels remained unchanged.Therefore, regulation of Cdc7 function appears to be the resultof posttranslational modification. In this study, we have attemptedto elucidate the mechanism responsible for achieving this specificexecution point of Cdc7. Cdc7 kinase activity was shown to bemaximal at the G1/S boundary by using either cultures synchronizedwith alpha factor or Cdc- mutants or with inhibitors of DNAsynthesis or mitosis. Therefore, Cdc7 kinase is regulated bya posttranslational mechanism that ensures maximal Cdc7 activityat the G1/S boundary, which is consistent with Cdc7 functionin the cell cycle. This cell cycle-dependent regulation couldbe the result of association with the Dbf4 protein. In thisstudy, the Dbf4 protein was shown to be required for Cdc7 kinaseactivity in that Cdc7 kinase activity is thermolabile in vitrowhen extracts prepared from a temperature-sensitive dbf4 mutantgrown under permissive conditions are used. In vitro reconstitutionassays, in addition to employment of the two-hybrid system forprotein-protein interactions, have demonstrated that the Cdc7and Dbf4 proteins interact both in vitro and in vivo. A suppressormutation, bob1-1, which can bypass deletion mutations in bothcdc7 and dbf4 was isolated. However, the bob1-1 mutation cannotbypass all events in G1 phase because it fails to suppress temperature-sensitivecdc4 or cdc28 mutations. This indicates that the Cdc7 and Dbf4proteins act at a common point in the cell cycle. Therefore,because of the common point of function for the two proteinsand the fact that the Dbf4 protein is essential for Cdc7 function,we propose that Dbf4 may represent a cyclin-like molecule specificfor the activation of Cdc7 kinase.

Mol Cell Biol. 1993 May; 13(5): 2899-2908

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