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Title: TLR1- and TLR6-independent recognition of bacterial lipopeptides.
Author(s): Buwitt-Beckmann, U.
Heine, H.
Wiesmuller, K.H.
Jung, G.
Brock, R.E. (314277129)
Akira, S.
Ulmer, A.J.
Publication year: 2006
Document type: Article / Letter to editor
Journal: Journal of Biological Chemistry
ISSN: 0021-9258
Volume: vol. 281
Issue: iss. 14
Start page: p. 9049
End page: p. 9057
Abstract: Bacterial cell walls contain lipoproteins/peptides, which are strong modulators of the innate immune system. Triacylated lipopeptides are assumed to be recognized by TLR2/TLR1-, whereas diacylated lipopeptides use TLR2/TLR6 heteromers for signaling. Following our initial discovery of TLR6-independent diacylated lipopeptides, we could now characterize di- and triacylated lipopeptides (e.g. Pam(2)C-SK(4), Pam(3)C-GNNDESNISFKEK), which have stimulatory activity in TLR1- and in TLR6-deficient mice. Furthermore, for the first time, we present triacylated lipopeptides with short length ester-bound fatty acids (like PamOct(2)C-SSNASK(4)), which induce no response in TLR1-deficient cells. No differences in the phosphorylation of MAP kinases by lipopeptide analogs having different TLR2-coreceptor usage were observed. Blocking experiments indicated that different TLR2 heteromers recognize their specific lipopeptide ligands independently from each other. In summary, a triacylation pattern is necessary but not sufficient to render a lipopeptide TLR1-dependent, and a diacylation pattern is necessary but not sufficient to render a lipopeptide TLR6-dependent. Contrary to the current model, distinct lipopeptides are recognized by TLR2 in a TLR1- and TLR6-independent manner.
Subject: UMCN 4.2: Chronic inflammation and autoimmunity
Organization: UMCN Extern
Biochemistry (UMCN)
Appears in Collections:Academic bibliography

Please use this identifier to cite or link to this item: http://hdl.handle.net/2066/51407

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