Granzyme B-dependent proteolysis acts as a switch to enhance the proinflammatory activity of IL-1α.

نویسندگان

  • Inna S Afonina
  • Graham A Tynan
  • Susan E Logue
  • Sean P Cullen
  • Michael Bots
  • Alexander U Lüthi
  • Emer P Reeves
  • Noel G McElvaney
  • Jan P Medema
  • Ed C Lavelle
  • Seamus J Martin
چکیده

Granzyme B is a cytotoxic lymphocyte-derived protease that plays a central role in promoting apoptosis of virus-infected target cells, through direct proteolysis and activation of constituents of the cell death machinery. However, previous studies have also implicated granzymes A and B in the production of proinflammatory cytokines, via a mechanism that remains undefined. Here we show that IL-1α is a substrate for granzyme B and that proteolysis potently enhanced the biological activity of this cytokine in vitro as well as in vivo. Consistent with this, compared with full-length IL-1α, granzyme B-processed IL-1α exhibited more potent activity as an immunoadjuvant in vivo. Furthermore, proteolysis of IL-1α within the same region, by proteases such as calpain and elastase, was also found to enhance its biological potency. Thus, IL-1α processing by multiple immune-related proteases, including granzyme B, acts as a switch to enhance the proinflammatory properties of this cytokine.

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عنوان ژورنال:
  • Molecular cell

دوره 44 2  شماره 

صفحات  -

تاریخ انتشار 2011