Acceleration of the G1/S phase transition by expression of cyclins D1 and E with an inducible system.

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Mol Cell Biol. 1994 March; 14(3): 1669-1679

Acceleration of the G1/S phase transition by expression of cyclins D1 and E with an inducible system.

D Resnitzky, M Gossen, H Bujard and S I Reed

Department of Molecular Biology, Scripps Research Institute, La Jolla, California 92037.

ABSTRACT

Conditional overexpression of human cyclins B1, D1, and E wasaccomplished by using a synthetic cDNA expression system basedon the Escherichia coli tetracycline repressor. After inductionof these cyclins in asynchronous Rat-1 fibroblasts, a decreasein the length of the G1 interval was observed for cyclins D1and E, consistent with an acceleration of the G1/S phase transition.We observed, in addition, a compensatory lengthening of S phaseand G2 so that the mean cell cycle length in populations constitutivelyexpressing these cyclins was unchanged relative to those oftheir uninduced counterparts. We found that expression of cyclinB1 had no effect on cell cycle dynamics, despite elevated levelsof cyclin B-associated histone H1 kinase activity. Inductionof cyclins D1 and E also accelerated entry into S phase forsynchronized cultures emerging from quiescence. However, whereascyclin E exerted a greater effect than cyclin D1 in asynchronouscycling cells, cyclin D1 conferred a greater effect upon stimulationfrom quiescence, suggesting a specific role for cyclin D1 inthe G0-to-G1 transition. Overexpression of cyclins did not preventcells from entering into quiescence upon serum starvation, althougha slight delay in attainment of quiescence was observed forcells expressing either cyclin D1 or cyclin E. These resultssuggest that cyclins D1 and E are rate-limiting activators ofthe G1-to-S phase transition and that cyclin D1 might play aspecialized role in facilitating emergence from quiescence.

Mol Cell Biol. 1994 March; 14(3): 1669-1679

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