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
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