2020
DOI: 10.1016/j.str.2020.05.010
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Structural Basis for the Activation and Target Site Specificity of CDC7 Kinase

Abstract: Summary CDC7 is an essential Ser/Thr kinase that acts upon the replicative helicase throughout the S phase of the cell cycle and is activated by DBF4. Here, we present crystal structures of a highly active human CDC7-DBF4 construct. The structures reveal a zinc-finger domain at the end of the kinase insert 2 that pins the CDC7 activation loop to motif M of DBF4 and the C lobe of CDC7. These interactions lead to ordering of the substrate-binding platform and full opening of the kinase active site. In… Show more

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Cited by 15 publications
(19 citation statements)
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“…3d ). The zinc-binding site formed by yeast and human Dbf4 proteins is highly conserved and helps to keep the Cdc7 αC helix and kinase insert 2 in their “kinase active” state, as described in the context of human Cdc7 41 (Fig. 3e, f ).…”
Section: Resultsmentioning
confidence: 96%
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“…3d ). The zinc-binding site formed by yeast and human Dbf4 proteins is highly conserved and helps to keep the Cdc7 αC helix and kinase insert 2 in their “kinase active” state, as described in the context of human Cdc7 41 (Fig. 3e, f ).…”
Section: Resultsmentioning
confidence: 96%
“…3e, f ). Even though residues forming a second zinc-binding site are not conserved between human and yeast Cdc7, a zinc ion is observed in a nearby alternative location relative to the structure of the human Cdc7, and may therefore stabilise a similar section of the kinase 41 .…”
Section: Resultsmentioning
confidence: 99%
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“…Dbf4 contains three evolutionarily conserved sequence motifs, termed N, M, and C that constitute parts of distinct domains separated by flexible linkers ( Hughes et al, 2012 ; Masai and Arai, 2000 ). The M and C domains embrace the Cdc7 kinase to mediate Cdc7 activation, while the N motif forms part of an N-terminal BRCT domain that is dispensable for Cdc7 activation ( Almawi et al, 2016 ; Dick et al, 2020 ; Hughes et al, 2012 ). Intriguingly, an N-terminal fragment encompassing the BRCT and M domains is required and sufficient to target Dbf4 to MCM complexes loaded at replication origins ( Dowell et al, 1994 ; Francis et al, 2009 ), while a physical interaction between Rad53 and the Dbf4 BRCT domain has been proposed to contribute to checkpoint-dependent origin control ( Chen et al, 2013 ; Duncker et al, 2002 ; Matthews et al, 2012 ; Matthews et al, 2014 ).…”
Section: Discussionmentioning
confidence: 99%