ERK Activity and G1 Phase Progression: Identifying Dispensable Versus Essential Activities and Primary Versus Secondary Targets

Jessie Villanueva,* Yuval Yung,* Janice L. Walker, and Richard K. Assoian

Department of Pharmacology, University of Pennsylvania School of Medicine, Philadelphia, PA 19104-6084

Monitoring Editor: Jean Schwarzbauer

The ERK subfamily of MAPkinases is a critical regulator of S phase entry. ERK activityregulates the induction of cyclin D1, and a sustained ERK signalis thought to be required for this effect, at least in fibroblasts.We now show that early G1 phase ERK activity is dispensablefor the induction of cyclin D1, and that the critical ERK signalingperiod is restricted to 3-6 h after mitogenic stimulation ofquiescent fibroblasts. Similarly, early G1 phase ERK activityis dispensable for entry into S phase. Moreover, if cyclin D1is expressed ectopically, ERK activity becomes dispensable throughoutG1 phase. In addition to its effect on cyclin D1, ERK activityis thought to contribute to the down-regulation of p27^kip1.We found that this effect is restricted to late G1/S phase.Mechanistic analysis showed that the ERK effect on p27^kip1 ismediated by Skp2 and secondary to its effect on cyclin D1. Ourresults emphasize the importance of midG1 phase ERK activityand resolve primary versus secondary ERK targets within theG1 phase cyclin-dependent kinases.

^*These authors contributed equally to this work.

Address correspondence to: Richard K. Assoian (rka{at}pharm.med.upenn.edu)

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