• Title of article

    ROCK and JAK1 Signaling Cooperate to Control Actomyosin Contractility in Tumor Cells and Stroma

  • Author/Authors

    Victoria Sanz-Moreno، نويسنده , , Victoria and Gaggioli، نويسنده , , Cedric and Yeo، نويسنده , , Maggie and Albrengues، نويسنده , , Jean and Wallberg، نويسنده , , Fredrik and Viros، نويسنده , , Amaya and Hooper، نويسنده , , Steven and Mitter، نويسنده , , Richard and Féral، نويسنده , , Chloé C. and Cook، نويسنده , , Martin and Larkin، نويسنده , , James and Marais، نويسنده , , Richard and Meneguzzi، نويسنده , , Guerrino and Sahai، نويسنده , , Erik S. Marshall، نويسنده , , Chris J.، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2011
  • Pages
    17
  • From page
    229
  • To page
    245
  • Abstract
    Summary lammatory cytokines are frequently observed in the tumor microenvironment, and chronic inflammation is involved in cancer initiation and progression. We show that cytokine signaling through the receptor subunit GP130-IL6ST and the kinase JAK1 generates actomyosin contractility through Rho-kinase dependent signaling. This pathway generates contractile force in stromal fibroblasts to remodel the extracellular matrix to create tracks for collective migration of squamous carcinoma cells and provides the high levels of actomyosin contractility required for migration of individual melanoma cells in the rounded, “amoeboid” mode. Thus, cytokine signaling can generate actomyosin contractility in both stroma and tumor cells. Strikingly, actomyosin contractility itself positively modulates activity of the transcription factor STAT3 downstream of JAK1, demonstrating positive feedback within the signaling network.
  • Journal title
    Cancer Cell
  • Serial Year
    2011
  • Journal title
    Cancer Cell
  • Record number

    1337594