• Title of article

    Bcl-xL gain of function and p19ARF loss of function cooperate oncogenically with Myc in vivo by distinct mechanisms

  • Author/Authors

    Finch، نويسنده , , Andrew and Prescott، نويسنده , , Julia and Shchors، نويسنده , , Ksenya and Hunt، نويسنده , , Abigail and Soucek، نويسنده , , Laura and Dansen، نويسنده , , Tobias B. and Swigart، نويسنده , , Lamorna Brown and Evan، نويسنده , , Gerard I.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2006
  • Pages
    8
  • From page
    113
  • To page
    120
  • Abstract
    Summary pression of Bcl-xL, loss of p19ARF, and loss of p53 all accelerate Myc oncogenesis. All three lesions are implicated in suppressing Myc-induced apoptosis, suggesting that this is a common mechanism by which they synergize with Myc. However, using an acutely switchable model of Myc-induced tumorigenesis, we demonstrate that each lesion cooperates with Myc in vivo by a distinct mechanism. While Bcl-xL blocks Myc-induced apoptosis, inactivation of p19ARF enhances it. However, this increase in apoptosis is matched by increased Myc-induced proliferation. p53 inactivation shares features of both lesions, partially suppressing apoptosis while augmenting proliferation. Bcl-xL and p19ARF loss together synergize to further accelerate Myc oncogenesis. Thus, differing lesions cooperate oncogenically with Myc by discrete mechanisms that can themselves synergize with each other.
  • Keywords
    CELLCYCLE
  • Journal title
    Cancer Cell
  • Serial Year
    2006
  • Journal title
    Cancer Cell
  • Record number

    1335737