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Caspase-1 processes IFN-γ-inducing factor and regulates LPS-induced IFN- γ production

Author

Listed:
  • Tariq Ghayur

    (BASF Bioresearch Corporation)

  • Subhashis Banerjee

    (BASF Bioresearch Corporation)

  • Margaret Hugunin

    (BASF Bioresearch Corporation)

  • Deborah Butler

    (BASF Bioresearch Corporation)

  • Linda Herzog

    (BASF Bioresearch Corporation)

  • Adam Carter

    (BASF Bioresearch Corporation)

  • Lucia Quintal

    (BASF Bioresearch Corporation)

  • Les Sekut

    (BASF Bioresearch Corporation)

  • Robert Talanian

    (BASF Bioresearch Corporation)

  • Michael Paskind

    (BASF Bioresearch Corporation)

  • Winnie Wong

    (BASF Bioresearch Corporation)

  • Robert Kamen

    (BASF Bioresearch Corporation)

  • Daniel Tracey

    (BASF Bioresearch Corporation)

  • Hamish Alien

    (BASF Bioresearch Corporation)

Abstract

Interferon-γ-inducing factor (IGIF, interleukin-18) is a recently described cytokine that shares structural features with the inter-leukin-1 (IL-1) family of proteins and functional properties with IL-121–4. Like IL-12, IGIF is a potent inducer of interferon (IFN)-γ from T cells and natural killer cells1–3,5,6. IGIF is synthesized as a biologically inactive precursor molecule (proIGIF). The cellular production of IL-lβ, a cytokine implicated in a variety of inflammatory diseases, requires cleavage of its precursor (proIL-lβ) at an Asp-X site by interleukin-lβ-converting enzyme7,8 (ICE, recently termed caspase-19). The Asp-X sequence at the putative processing site in proIGIF2,3 suggests that a protease such as caspase-1 might be involved in the maturation of IGIF4. Here we demonstrate that caspase-1 processes proIGIF and proIL-lβ with equivalent efficiencies in vitro. A selective caspase-1 inhibitor blocks both lipopolysaccharide-induced IL-1β and IFN-γ production from human mononuclear cells. Furthermore, caspase-1-deficient mice are defective in lipopolysaccharide-induced IFN-γ production. Our results thus implicate caspase-1 in the physiological production of IGIF and demonstrate that it plays a critical role in the regulation of multiple proinflammatory cytokines. Specific caspase-1 inhibitors would provide a new class of anti-inflammatory drugs with multipotent action.

Suggested Citation

  • Tariq Ghayur & Subhashis Banerjee & Margaret Hugunin & Deborah Butler & Linda Herzog & Adam Carter & Lucia Quintal & Les Sekut & Robert Talanian & Michael Paskind & Winnie Wong & Robert Kamen & Daniel, 1997. "Caspase-1 processes IFN-γ-inducing factor and regulates LPS-induced IFN- γ production," Nature, Nature, vol. 386(6625), pages 619-623, April.
  • Handle: RePEc:nat:nature:v:386:y:1997:i:6625:d:10.1038_386619a0
    DOI: 10.1038/386619a0
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