par Paternot, Sabine 
;Bockstaele, Laurence ;Bisteau, Xavier ;Kooken, Hugues ;Coulonval, Katia ;Roger, Pierre P.
Référence Cell cycle (Georgetown, Tex.), 9, 4, page (689-699)
Publication Publié, 2010-02
;Bockstaele, Laurence ;Bisteau, Xavier ;Kooken, Hugues ;Coulonval, Katia ;Roger, Pierre P. Référence Cell cycle (Georgetown, Tex.), 9, 4, page (689-699)
Publication Publié, 2010-02
Article révisé par les pairs
| Résumé : | Cyclin-dependent kinase (CDK) 4 is a master integrator that couples mitogenic/oncogenic signalling cascades with the inactivation of the central oncosuppressor Rb and the cell cycle. Its activation requires binding to a D-type cyclin and then T-loop phosphorylation at T172 by the only identified CDK-activating kinase in animal cells, cyclin H-CDK7. In contrast with the observed constitutive activity of cyclin H-CDK7, we have recently identified the T172-phosphorylation of cyclin D-bound CDK4 as a crucial cell cycle regulatory target. Intriguingly, the homologous T177-phosphorylation of CDK6 is weak in several systems and does not present this regulation. In this Perspective, we review the recent advances and debates on the multistep mechanism leading to activation of D-type cyclin-CDK4 complexes. This involves a re-evaluation of the implication of Cip/Kip CDK "inhibitors" and CDK7 in this process. |
