1. The Ets transcription factor GABP is required for cell-cycle progression.
- Author
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Zhong-Fa Yang, Mott, Stephanie, and Rosmarin, Alan G.
- Subjects
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CYCLINS , *GROWTH factors , *MITOGENS , *PROTEIN kinases , *PHOSPHORYLATION , *TRANSCRIPTION factors , *CELL proliferation - Abstract
The transition from cellular quiescence (G0) into S phase is regulated by the mitogenic-activation of D-type cyclins and cyclin-dependent kinases (Cdks), the sequestration of the Cdk inhibitors (CDKIs), p21 and p27, and the hyperphosphorylation of Rb with release of E2F transcription factors. However, fibroblasts that lack all D-type cyclins can still undergo serum-induced proliferation and key E2F targets are expressed at stable levels despite cyclical Rb–E2F activity. Here, we show that serum induces expression of the Ets transcription factor, Gabpα, and that its ectopic expression induces quiescent cells to re-enter the cell cycle. Genetic disruption of Gabpα prevents entry into S phase, and selectively reduces expression of genes that are required for DNA synthesis and degradation of CDKIs, yet does not alter expression of D-type cyclins, Cdks, Rb or E2Fs. Thus, GABP is necessary and sufficient for re-entry into the cell cycle and it regulates a pathway that is distinct from that of D-type cyclins and CDKs. [ABSTRACT FROM AUTHOR]
- Published
- 2007
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