Cutting edge: heat shock protein 60 is a putative endogenous ligand of the toll-like receptor-4 complex
K Ohashi, V Burkart, S Flohé, H Kolb - The Journal of Immunology, 2000 - journals.aai.org
K Ohashi, V Burkart, S Flohé, H Kolb
The Journal of Immunology, 2000•journals.aai.orgHuman heat shock protein 60 (hsp60) elicits a potent proinflammatory response in cells of
the innate immune system and therefore has been proposed as a danger signal of stressed
or damaged cells. We report here that macrophages of C3H/HeJ mice, carrying a mutant Toll-
like-receptor (Tlr) 4 are nonresponsive to hsp60. Both the induction of TNF-α and NO
formation were found dependent on a functional Tlr4 whereas stimulation of macrophages
by CpG DNA was Tlr4 independent. We conclude that Tlr4 mediates hsp60 signaling. This is …
the innate immune system and therefore has been proposed as a danger signal of stressed
or damaged cells. We report here that macrophages of C3H/HeJ mice, carrying a mutant Toll-
like-receptor (Tlr) 4 are nonresponsive to hsp60. Both the induction of TNF-α and NO
formation were found dependent on a functional Tlr4 whereas stimulation of macrophages
by CpG DNA was Tlr4 independent. We conclude that Tlr4 mediates hsp60 signaling. This is …
Abstract
Human heat shock protein 60 (hsp60) elicits a potent proinflammatory response in cells of the innate immune system and therefore has been proposed as a danger signal of stressed or damaged cells. We report here that macrophages of C3H/HeJ mice, carrying a mutant Toll-like-receptor (Tlr) 4 are nonresponsive to hsp60. Both the induction of TNF-α and NO formation were found dependent on a functional Tlr4 whereas stimulation of macrophages by CpG DNA was Tlr4 independent. We conclude that Tlr4 mediates hsp60 signaling. This is the first report of a putative endogenous ligand of the Tlr4 complex.
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