c-Myc regulates cyclin D-Cdk4 and-Cdk6 activity but affects cell cycle progression at multiple independent points

MK Mateyak, AJ Obaya, JM Sedivy - Molecular and cellular biology, 1999 - Taylor & Francis
MK Mateyak, AJ Obaya, JM Sedivy
Molecular and cellular biology, 1999Taylor & Francis
c-myc is a cellular proto-oncogene associated with a variety of human cancers and is
strongly implicated in the control of cellular proliferation, programmed cell death, and
differentiation. We have previously reported the first isolation of a c-myc-null cell line. Loss of
c-Myc causes a profound growth defect manifested by the lengthening of both the G1and G2
phases of the cell cycle. To gain a clearer understanding of the role of c-Myc in cellular
proliferation, we have performed a comprehensive analysis of the components that regulate …
c-myc is a cellular proto-oncogene associated with a variety of human cancers and is strongly implicated in the control of cellular proliferation, programmed cell death, and differentiation. We have previously reported the first isolation of a c-myc-null cell line. Loss of c-Myc causes a profound growth defect manifested by the lengthening of both the G1and G2 phases of the cell cycle. To gain a clearer understanding of the role of c-Myc in cellular proliferation, we have performed a comprehensive analysis of the components that regulate cell cycle progression. The largest defect observed in c-myc−/− cells is a 12-fold reduction in the activity of cyclin D1-Cdk4 and -Cdk6 complexes during the G0-to-S transition. Downstream events, such as activation of cyclin E-Cdk2 and cyclin A-Cdk2 complexes, are delayed and reduced in magnitude. However, it is clear that c-Myc affects the cell cycle at multiple independent points, because restoration of the Cdk4 and -6 defect does not significantly increase growth rate. In exponentially cycling cells the absence of c-Myc reduces coordinately the activities of all cyclin–cyclin-dependent kinase complexes. An analysis of cyclin-dependent kinase complex regulators revealed increased expression of p27KIP1 and decreased expression of Cdk7 in c-myc−/− cells. We propose that c-Myc functions as a crucial link in the coordinate adjustment of growth rate to environmental conditions.
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