Schultz et al. (1998) Proc. Natl. Acad. Sci. USA 95, 5857-5864
Letunic et al. (2012) Nucleic Acids Res , doi:10.1093/nar/gkr931

• HOME
• SETUP
• FAQ
• ABOUT
• GLOSSARY
• WHAT'S NEW
• FEEDBACK

CDT1 DNA replication factor CDT1 like

SMART accession number:	SM01075
Description:	CDT1 is a component of the replication licensing system and promotes the loading of the mini-chromosome maintenance complex onto chromatin. Geminin is an inhibitor of CDT1 and prevents inappropriate re-initiation of replication on an already fired origin. This region of CDT1 binds to Geminin (PUBMED:15286659).
Interpro abstract (IPR014939):	This entry represents the geminin-binding domain of the DNA replication factor CDT1 and related domains whose functions are not known [(PUBMED:15286659)].
Family alignment:	View or CHROMA formatCLUSTALW formatMSF formatFASTA formatPIR format

There are 144 CDT1 domains in 144 proteins in SMART's nrdb database.

Click on the following links for more information.

• Evolution (species in which this domain is found)

• Click on to expand nodes. To display all proteins with a CDT1 domain in a specific node, click on it.

  This tree shows only several representative species. The complete taxonomic breakdown of all proteins with CDT1 domain is also avaliable.

  Useful shortcuts: Expand all nodes or Collapse tree
  Go to specific node: Anopheles gambiae, Arabidopsis thaliana, Caenorhabditis elegans, Drosophila melanogaster, Homo sapiens, Mus musculus, Rattus norvegicus, Takifugu rubripes

• Cellular role (predicted cellular role)

• Cellular role: chromatin
  Binding / catalysis: binds to Geminin

• Literature (relevant references for this domain)

• Primary literature is listed below; Automatically-derived, secondary literature is also avaliable.

  • Lee C et al.
  • Structural basis for inhibition of the replication licensing factor Cdt1by geminin.
  • Nature. 2004; 430: 913-7
  • Display abstract

  • To maintain chromosome stability in eukaryotic cells, replication originsmust be licensed by loading mini-chromosome maintenance (MCM2-7) complexesonce and only once per cell cycle. This licensing control is achievedthrough the activities of geminin and cyclin-dependent kinases. Gemininbinds tightly to Cdt1, an essential component of the replication licensingsystem, and prevents the inappropriate reinitiation of replication on analready fired origin. The inhibitory effect of geminin is thought toprevent the interaction between Cdt1 and the MCM helicase. Here wedescribe the crystal structure of the mouse geminin-Cdt1 complex usingtGeminin (residues 79-157, truncated geminin) and tCdt1 (residues 172-368,truncated Cdt1). The amino-terminal region of a coiled-coil dimer oftGeminin interacts with both N-terminal and carboxy-terminal parts oftCdt1. The primary interface relies on the steric complementarity betweenthe tGeminin dimer and the hydrophobic face of the two short N-terminalhelices of tCdt1 and, in particular, Pro 181, Ala 182, Tyr 183, Phe 186and Leu 189. The crystal structure, in conjunction with our biochemicaldata, indicates that the N-terminal region of tGeminin might be requiredto anchor tCdt1, and the C-terminal region of tGeminin prevents access ofthe MCM complex to tCdt1 through steric hindrance.

• Structure (3D structures containing this domain)

• 3D Structures of CDT1 domains in PDB

  PDB code	Main view	Title
  2wvr		Human cdt1:geminin complex
  2zxx		Crystal structure of cdt1/geminin complex

• Links (links to other resources describing this domain)

• PFAM	CDT1
  INTERPRO	IPR014939

Send comments to Ivica Letunic