Article
- The EMBO Journal (2006) 25, 1987 - 1996
- doi:10.1038/sj.emboj.7601075
Published online: 13 April 2006
Subject Categories:
A CDK-catalysed regulatory phosphorylation for formation of the DNA replication complex Sld2–Dpb11
Yon-Soo Tak1,2,a, Yoshimi Tanaka1,3, Shizuko Endo1, Yoichiro Kamimura1,2,3,b and Hiroyuki Araki1,2,3
- Division of Microbial Genetics, National Institute of Genetics, Research Organization of Information and Systems, Mishima, Shizuoka, Japan
- Department of Genetics, SOKENDAI, Mishima, Shizuoka, Japan
- CREST, Kawaguchi, Saitama, Japan
Correspondence to:
Hiroyuki Araki, Division of Microbial Genetics, National Institute of Genetics, Research Organization of Information and Systems, Yata 1111, Mishima, Shizuoka 411-8540, Japan. Tel.: +81 55 981 6754; Fax: +81 55 981 6762; E-mail: hiaraki@lab.nig.ac.jp
aPresent address: Department of Biological Sciences, KAIST, Daejeon 305-701, Korea
bPresent address: Department of Cell Biology, Johns Hopkins University School of Medicine, Baltimore, MD 21205, USA
Received 8 November 2005; Accepted 9 March 2006
Abstract
Phosphorylation often regulates protein–protein interactions to control biological reactions. The Sld2 and Dpb11 proteins of budding yeast form a phosphorylation-dependent complex that is essential for chromosomal DNA replication. The Sld2 protein has a cluster of 11 cyclin-dependent kinase (CDK) phosphorylation motifs (Ser/Thr–Pro), six of which match the canonical sequences Ser/Thr–Pro–X–Lys/Arg, Lys/Arg–Ser/Thr–Pro and Ser/Thr–Pro–Lys/Arg. Simultaneous alanine substitution for serine or threonine in all the canonical CDK-phosphorylation motifs severely reduces complex formation between Sld2 and Dpb11, and inhibits DNA replication. Here we show that phosphorylation of these canonical motifs does not play a direct role in complex formation, but rather regulates phosphorylation of another residue, Thr84. This constitutes a non-canonical CDK-phosphorylation motif within a 28-amino-acid sequence that is responsible, after phosphorylation, for binding of Sld2–Dpb11. We further suggest that CDK-catalysed phosphorylation of sites other than Thr84 renders Thr84 accessible to CDK. Finally, we argue that this novel mechanism sets a threshold of CDK activity for formation of the essential Sld2 to Dpb11 complex and therefore prevents premature DNA replication.
Keywords:
- BRCT,
- CDK,
- DNA replication,
- phosphorylation,
- S phase
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