• Title of article

    Genome-wide Loss-of-Function Screen Reveals an Important Role for the Proteasome in HDAC Inhibitor-Induced Apoptosis

  • Author/Authors

    Fotheringham، نويسنده , , Susan and Epping، نويسنده , , Mirjam T. and Stimson، نويسنده , , Lindsay and Khan، نويسنده , , Omar and Wood، نويسنده , , Victoria and Pezzella، نويسنده , , Francesco and Bernards، نويسنده , , René and La Thangue، نويسنده , , Nicholas B.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2009
  • Pages
    10
  • From page
    57
  • To page
    66
  • Abstract
    Summary nt acetylation has been strongly linked to tumorigenesis, and the modulation of acetylation through targeting histone deacetylases (HDACs) is gathering increasing pace as a viable therapeutic strategy. A genome-wide loss-of-function screen identified HR23B, which shuttles ubiquitinated cargo proteins to the proteasome, as a sensitivity determinant for HDAC inhibitor-induced apoptosis. HR23B also governs tumor cell sensitivity to drugs that act directly on the proteasome. The level of HR23B influences the response of tumor cells to HDAC inhibitors, and HR23B is found at high levels in cutaneous T cell lymphoma in situ, a malignancy that responds favorably to HDAC inhibitor-based therapy. These results suggest that deregulated proteasome activity contributes to the anticancer activity of HDAC inhibitors.
  • Keywords
    CELLBIO , HUMDISEASE , Signaling
  • Journal title
    Cancer Cell
  • Serial Year
    2009
  • Journal title
    Cancer Cell
  • Record number

    1336907