• Title of article

    PI3Kγ Mediates Kaposiʹs Sarcoma-Associated Herpesvirus vGPCR-Induced Sarcomagenesis

  • Author/Authors

    Martin، نويسنده , , Daniel and Galisteo، نويسنده , , Rebeca and Molinolo، نويسنده , , Alfredo A. and Wetzker، نويسنده , , Reinhard and Hirsch، نويسنده , , Emilio and Gutkind، نويسنده , , J. Silvio، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2011
  • Pages
    9
  • From page
    805
  • To page
    813
  • Abstract
    Summary roliferative tumors induced by the Kaposiʹs sarcoma-associated herpesvirus (KSHV) have been successfully treated with rapamycin, which provided direct evidence of the clinical activity of mTOR inhibitors in human malignancies. However, prolonged mTOR inhibition may raise concerns in immunocompromised patients, including AIDS-Kaposiʹs sarcoma (KS). Here, we explored whether KSHV oncogenes deploy cell type-specific signaling pathways activating mTOR, which could be exploited to halt KS development while minimizing immune suppressive effects. We found that PI3Kγ, a PI3K isoform exhibiting restricted tissue distribution, is strictly required for signaling from the KSHV-encoded vGPCR oncogene to Akt/mTOR. Indeed, by using an endothelial-specific gene delivery system modeling KS development, we provide genetic and pharmacological evidence that PI3Kγ may represent a suitable molecular target for therapeutic intervention in KS.
  • Journal title
    Cancer Cell
  • Serial Year
    2011
  • Journal title
    Cancer Cell
  • Record number

    1337537