PLoS ONE (Jan 2016)

Interaction of Toll-Like Receptors with the Molecular Chaperone Gp96 Is Essential for Its Activation of Cytotoxic T Lymphocyte Response.

  • Weiwei Liu,
  • Mi Chen,
  • Xinghui Li,
  • Bao Zhao,
  • Junwei Hou,
  • Huaguo Zheng,
  • Lipeng Qiu,
  • Zihai Li,
  • Songdong Meng

DOI
https://doi.org/10.1371/journal.pone.0155202
Journal volume & issue
Vol. 11, no. 5
p. e0155202

Abstract

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The heat shock protein gp96 elicits specific T cell responses to its chaperoned peptides against cancer and infectious diseases in both rodent models and clinical trials. Although gp96-induced innate immunity, via a subset of Toll like receptors (TLRs), and adaptive immunity, through antigen presentation, are both believed to be important for priming potent T cell responses, direct evidence for the role of gp96-mediated TLR activation related to its functional T cell activation is lacking. Here, we report that gp96 containing mutations in its TLR-binding domain failed to activate macrophages, but peptide presentation was unaffected. Moreover, we found that peptide-specific T cell responses, as well as antitumor T cell immunity induced by gp96, are severely impaired when the TLR-binding domain is mutated. These data demonstrate the essential role of the gp96-TLR interaction in priming T cell immunity and provide further molecular basis for the coupling of gp96-mediated innate with adaptive immunity.