D-type cyclin-dependent kinase activity in mammalian cells.

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Mol Cell Biol. 1994 March; 14(3): 2066-2076

D-type cyclin-dependent kinase activity in mammalian cells.

H Matsushime, D E Quelle, S A Shurtleff, M Shibuya, C J Sherr and J Y Kato

Department of Genetics, University of Tokyo, Japan.

ABSTRACT

D-type cyclin-dependent kinase activities have not so far beendetected in mammalian cells. Lysis of rodent fibroblasts, mousemacrophages, or myeloid cells with Tween 20 followed by precipitationwith antibodies to cyclins D1, D2, and D3 or to their majorcatalytic partner, cyclin-dependent kinase 4 (cdk4), yieldedkinase activities in immune complexes which readily phosphorylatedthe retinoblastoma protein (pRb) but not histone H1 or casein.Virtually all cyclin D1-dependent kinase activity in proliferatingmacrophages and fibroblasts could be attributed to cdk4. Whenquiescent cells were stimulated by growth factors to enter thecell cycle, cyclin D1-dependent kinase activity was first detectedin mid G1, reached a maximum near the G1/S transition, and remainedelevated in proliferating cells. The rate of appearance of kinaseactivity during G1 phase lagged significantly behind cyclininduction and correlated with the more delayed accumulationof cdk4 and formation of cyclin D1-cdk4 complexes. Thus, cyclinD1-associated kinase activity was not detected during the G0-to-G1transition, which occurs within the first few hours followinggrowth factor stimulation. Rodent fibroblasts engineered toconstitutively overexpress either cyclin D1 alone or cyclinD3 together with cdk4 exhibited greatly elevated cyclin D-dependentkinase activity, which remained absent in quiescent cells butrose to supraphysiologic levels as cells progressed throughG1. Therefore, despite continued enforced overproduction ofcyclins and cdk4, the assembly of cyclin D-cdk4 complexes andthe appearance of their kinase activities remained dependentupon serum stimulation, indicating that upstream regulatorsmust govern formation of the active enzymes.

Mol Cell Biol. 1994 March; 14(3): 2066-2076

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Jensen, S. S., Madsen, M. W., Lukas, J., Binderup, L., Bartek, J. (2001). Inhibitory Effects of 1{alpha},25-Dihydroxyvitamin D3 on the G1-S Phase-Controlling Machinery. Mol. Endocrinol. 15: 1370-1380 [Abstract] [Full Text]
Ezhevsky, S. A., Ho, A., Becker-Hapak, M., Davis, P. K., Dowdy, S. F. (2001). Differential Regulation of Retinoblastoma Tumor Suppressor Protein by G1 Cyclin-Dependent Kinase Complexes In Vivo. Mol. Cell. Biol. 21: 4773-4784 [Abstract] [Full Text]
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