• Title of article

    Interleukin-1β impairs brain derived neurotrophic factor-induced signal transduction

  • Author/Authors

    Liqi Tong، نويسنده , , Robert Balazs، نويسنده , , Rungtip Soiampornkul، نويسنده , , Wipawan Thangnipon، نويسنده , , Carl W. Cotman، نويسنده ,

  • Issue Information
    روزنامه با شماره پیاپی سال 2008
  • Pages
    14
  • From page
    1380
  • To page
    1393
  • Abstract
    The expression of IL-1 is elevated in the CNS in diverse neurodegenerative disorders, including Alzheimerʹs disease. The hypothesis was tested that IL-1β renders neurons vulnerable to degeneration by interfering with BDNF-induced neuroprotection. In trophic support-deprived neurons, IL-1β compromised the PI3-K/Akt pathway-mediated protection by BDNF and suppressed Akt activation. The effect was specific as in addition to Akt, the activation of MAPK/ERK, but not PLCγ, was decreased. Activation of CREB, a target of these signaling pathways, was severely depressed by IL-1β. As the cytokine did not influence TrkB receptor and PLCγ activation, IL-1β might have interfered with BDNF signaling at the docking step conveying activation to the PI3-K/Akt and Ras/MAPK pathways. Indeed, IL-1β suppressed the activation of the respective scaffolding proteins IRS-1 and Shc; this effect might involve ceramide generation. IL-1-induced interference with BDNF neuroprotection and signal transduction was corrected, in part, by ceramide production inhibitors and mimicked by the cell-permeable C2-ceramide. These results suggest that IL-1β places neurons at risk by interfering with BDNF signaling involving a ceramide-associated mechanism.
  • Keywords
    signal transduction , BDNF , IL-1 , Cortical neurons
  • Journal title
    Neurobiology of Aging
  • Serial Year
    2008
  • Journal title
    Neurobiology of Aging
  • Record number

    821245