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Arrest of the cell cycle by the tumour-suppressor BRCA1 requires the CDK-inhibitor p21WAF1/CiPl

Author

Listed:
  • Kumaravel Somasundaram

    (Laboratory of Molecular Oncology and Cell Cycle Regulation, Howard Hughes Medical Institute, University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine)

  • Hongbing Zhang

    (University of Pennsylvania School of Medicine)

  • Yi-Xin Zeng

    (Laboratory of Molecular Oncology and Cell Cycle Regulation, Howard Hughes Medical Institute, University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine)

  • Yariv Houvras

    (The Mount Sinai School of Medicine)

  • Yi Peng

    (University of Pennsylvania School of Medicine)

  • Hongxiang Zhang

    (University of Pennsylvania School of Medicine)

  • Gen Sheng Wu

    (Laboratory of Molecular Oncology and Cell Cycle Regulation, Howard Hughes Medical Institute, University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine)

  • Jonathan D. Licht

    (The Mount Sinai School of Medicine)

  • Barbara L. Weber

    (University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine)

  • Wafik S. El-Deiry

    (Laboratory of Molecular Oncology and Cell Cycle Regulation, Howard Hughes Medical Institute, University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine
    University of Pennsylvania School of Medicine)

Abstract

Much of the predisposition to hereditary breast and ovarian cancer has been attributed to inherited defects in the BRCA1 tumour-suppressor gene1,2,3. The nuclear protein BRCA1 has the properties of a transcription factor4,5,6,7, and can interact with the recombination and repair protein RAD51 (ref. 8). Young women with germline alterations in BRCA1 develop breast cancer at rates 100-fold higher than the general population3, and BRCA1-null mice die before day 8 of development9,10. However, the mechanisms of BRCA1-mediated growth regulation and tumour suppression remain unknown. Here we show that BRCA1 transactivates expression of the cyclin-dependent kinase inhibitor p21WAF1/CIP1 in a p53-independent manner, and that BRCA1 inhibits cell-cycle progression into the S-phase following its transfection into human cancer cells. BRCA1 does not inhibit S-phase progression in p21−/− cells, unlike p21+/+ cells, and tumour-associated, transactivation-deficient mutants of BRCA1 are defective in both transactivation of p21 and cell-cycle inhibition. These data suggest that one mechanism by which BRCA1 contributes to cell-cycle arrest and growth suppression is through the induction of p21.

Suggested Citation

  • Kumaravel Somasundaram & Hongbing Zhang & Yi-Xin Zeng & Yariv Houvras & Yi Peng & Hongxiang Zhang & Gen Sheng Wu & Jonathan D. Licht & Barbara L. Weber & Wafik S. El-Deiry, 1997. "Arrest of the cell cycle by the tumour-suppressor BRCA1 requires the CDK-inhibitor p21WAF1/CiPl," Nature, Nature, vol. 389(6647), pages 187-190, September.
  • Handle: RePEc:nat:nature:v:389:y:1997:i:6647:d:10.1038_38291
    DOI: 10.1038/38291
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