PLoS Pathogens (Jun 2011)

Pathogen recognition receptor signaling accelerates phosphorylation-dependent degradation of IFNAR1.

  • Juan Qian,
  • Hui Zheng,
  • Wei-Chun Huangfu,
  • Jianghuai Liu,
  • Christopher J Carbone,
  • N Adrian Leu,
  • Darren P Baker,
  • Serge Y Fuchs

DOI
https://doi.org/10.1371/journal.ppat.1002065
Journal volume & issue
Vol. 7, no. 6
p. e1002065

Abstract

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An ability to sense pathogens by a number of specialized cell types including the dendritic cells plays a central role in host's defenses. Activation of these cells through the stimulation of the pathogen-recognition receptors induces the production of a number of cytokines including Type I interferons (IFNs) that mediate the diverse mechanisms of innate immunity. Type I IFNs interact with the Type I IFN receptor, composed of IFNAR1 and IFNAR2 chains, to mount the host defense responses. However, at the same time, Type I IFNs elicit potent anti-proliferative and pro-apoptotic effects that could be detrimental for IFN-producing cells. Here, we report that the activation of p38 kinase in response to pathogen-recognition receptors stimulation results in a series of phosphorylation events within the IFNAR1 chain of the Type I IFN receptor. This phosphorylation promotes IFNAR1 ubiquitination and accelerates the proteolytic turnover of this receptor leading to an attenuation of Type I IFN signaling and the protection of activated dendritic cells from the cytotoxic effects of autocrine or paracrine Type I IFN. In this paper we discuss a potential role of this mechanism in regulating the processes of innate immunity.