Suppression of the p53- or pRB-mediated G1 checkpoint is required for E2F-induced S-phase entry.

Marina Lomazzi, M Cristina Moroni, Michael R Jensen, Emanuela Frittoli, Kristian Helin

    72 Citations (Scopus)

    Abstract

    Deregulation of the retinoblastoma protein (pRB) pathway is a hallmark of cancer. In the absence of other genetic alterations, this deregulation results in lack of differentiation, hyperproliferation and apoptosis. The pRB protein acts as a transcriptional repressor by targeting the E2F transcription factors, whose functions are required for entry into S phase. Increased E2F activity can induce S phase in quiescent cells--this is a central element of most models for the development of cancer. We show that although E2F1 alone is not sufficient to induce S phase in diploid mouse and human fibroblasts, increased E2F1 activity can result in S-phase entry in diploid fibroblasts in which the p53-mediated G1 checkpoint is suppressed. In addition, we show that E2F1 can induce S phase in primary mouse fibroblasts lacking pRB. These results indicate that, in addition to acting as an E2F-dependent transcriptional repressor, pRB is also required for the cells to retain the G1 checkpoint in response to unprogrammed proliferative signals.
    Original languageEnglish
    JournalNature Genetics
    Volume31
    Issue number2
    Pages (from-to)190-4
    Number of pages4
    ISSN1061-4036
    DOIs
    Publication statusPublished - 2002

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