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Publication : Hyaluronan fragments act as an endogenous danger signal by engaging TLR2.

First Author  Scheibner KA Year  2006
Journal  J Immunol Volume  177
Issue  2 Pages  1272-81
PubMed ID  16818787 Mgi Jnum  J:135038
Mgi Id  MGI:3790279 Doi  10.4049/jimmunol.177.2.1272
Citation  Scheibner KA, et al. (2006) Hyaluronan fragments act as an endogenous danger signal by engaging TLR2. J Immunol 177(2):1272-81
abstractText  Upon tissue injury, high m.w. hyaluronan (HA), a ubiquitously distributed extracellular matrix component, is broken down into lower m.w. (LMW) fragments, which in turn activate an innate immune response. In doing so, LMW HA acts as an endogenous danger signal alerting the immune system of a breach in tissue integrity. In this report, we demonstrate that LMW HA activates the innate immune response via TLR-2 in a MyD88-, IL-1R-associated kinase-, TNFR-associated factor-6-, protein kinase Czeta-, and NF-kappaB-dependent pathway. Furthermore, we show that intact high m.w. HA can inhibit TLR-2 signaling. Finally, we demonstrate that LMW HA can act as an adjuvant promoting Ag-specific T cell responses in vivo in wild-type but not TLR-2(null) mice.
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