Cyclin A2 Mutagenesis Analysis: A New Insight into CDK Activation and Cellular Localization Requirements

A Philips; BA Schulman; Bénédicte Lemmers; C Lukas; CH Yam; CS Sorensen; DO Morgan; EA Nigg; G Maridor; I Barlat; I Kalaszczynska; Jean-Marc Vanacker; Jean-Marie Blanchard; L Fajas; M Coisy; M Coisy-Quivy; M Jackman; M Murphy; Nawal Bendris; Nikola Arsic; NR Brown; P Gallant; P Meraldi; PD Jeffrey; T Goda; TK Fung; WY Tsang; X Huet

Cyclin A2 Mutagenesis Analysis: A New Insight into CDK Activation and Cellular Localization Requirements

Authors: A Philips
BA Schulman
Bénédicte Lemmers
C Lukas
CH Yam
CS Sorensen
DO Morgan
EA Nigg
G Maridor
I Barlat
I Kalaszczynska
Jean-Marc Vanacker
Jean-Marie Blanchard
L Fajas
M Coisy
M Coisy-Quivy
M Jackman
M Murphy
Nawal Bendris
Nikola Arsic
NR Brown
P Gallant
P Meraldi
PD Jeffrey
T Goda
TK Fung
WY Tsang
X Huet
Publication date: 1 January 2011
Publisher: Public Library of Science
Doi

Abstract

Cyclin A2 is essential at two critical points in the somatic cell cycle: during S phase, when it activates CDK2, and during the G2 to M transition when it activates CDK1. Based on the crystal structure of Cyclin A2 in association with CDKs, we generated a panel of mutants to characterize the specific amino acids required for partner binding, CDK activation and subcellular localization. We find that CDK1, CDK2, p21, p27 and p107 have overlapping but distinct requirements for association with this protein. Our data highlight the crucial importance of the N-terminal α helix, in conjunction with the α3 helix within the cyclin box, in activating CDK. Several Cyclin A2 mutants selectively bind to either CDK1 or CDK2. We demonstrate that association of Cyclin A2 to proteins such as CDK2 that was previously suggested as crucial is not a prerequisite for its nuclear localization, and we propose that the whole protein structure is involved