Cell cycle-dependent gene transcription is tightly controlled by the retinoblastoma (RB): E2F
and DREAM complexes, which repress all cell cycle genes during quiescence. Cyclin …

The precise timing of cell cycle gene expression is critical for the control of cell proliferation;
de-regulation of this timing promotes the formation of cancer and leads to defects during …

The canonical model of RB-mediated tumour suppression developed over the past 30 years
is based on the regulation of E2F transcription factors to restrict cell cycle progression …

Most human cancers acquire mutations causing defects in the p53 signaling pathway. The
tumor suppressor p53 becomes activated in response to genotoxic stress and is essential for …

Perfectly orchestrated periodic gene expression during cell cycle progression is essential for
maintaining genome integrity and ensuring that cell proliferation can be stopped by …

Background Previous studies report that miR-1-3p, a member of the microRNA-1 family (miR-
1), and functions as a tumor suppressor in several different cancers. However, little is known …

The retinoblastoma Rb protein is an important factor controlling the cell cycle. Yet,
mammalian cells carrying Rb deletions are still able to arrest under growth-limiting …

Ordered cell cycle progression is coordinated by cyclin dependent kinases (CDKs). CDKs
often phosphorylate substrates at multiple sites clustered within disordered regions …

Pocket proteins retinoblastoma (pRb), p107 and p130 are negative regulators of cellular
proliferation and multifunctional proteins regulating development, differentiation and …

The DREAM (Dp/Retinoblastoma (Rb)-like/E2F/MuvB) transcriptional repressor complex
acts as a gatekeeper of the mammalian cell cycle by establishing and maintaining cellular …