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Soluble collectin-12 mediates C3-independent docking of properdin that activates the alternative pathway of complement

Permanent lenke
https://hdl.handle.net/10037/21316
DOI
https://doi.org/10.7554/ELIFE.60908
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article.pdf (2.556Mb)
Publisert versjon (PDF)
Dato
2020-09-10
Type
Journal article
Tidsskriftartikkel
Peer reviewed

Forfatter
Zhang, Jie; Song, Lihong; Pedersen, Dennis V.; Li, Anna; Lambris, John D.; Andersen, Gregers Rom; Mollnes, Tom Eirik; Ma, Ying Jie; Garred, Peter
Sammendrag
Properdin stabilizes the alternative C3 convertase (C3bBb), whereas its role as pattern-recognition molecule mediating complement activation is disputed for decades. Previously, we have found that soluble collectin-12 (sCL-12) synergizes complement alternative pathway (AP) activation. However, whether this observation is C3 dependent is unknown. By application of the C3-inhibitor Cp40, we found that properdin in normal human serum bound to Aspergillus fumigatus solely in a C3b-dependent manner. Cp40 also prevented properdin binding when properdin-depleted serum reconstituted with purified properdin was applied, in analogy with the findings achieved by C3-depleted serum. However, when opsonized with sCL-12, properdin bound in a C3-independent manner exclusively via its tetrameric structure and directed in situ C3bBb assembly. In conclusion, a prerequisite for properdin binding and in situ C3bBb assembly was the initial docking of sCL-12. This implies a new important function of properdin in host defense bridging pattern recognition and specific AP activation.
Forlag
eLife Sciences Publications
Sitering
Zhang, Song, Pedersen, Li, Lambris, Andersen, Mollnes, Ma, Garred. Soluble collectin-12 mediates C3-independent docking of properdin that activates the alternative pathway of complement. eLIFE. 2020;9:e60908:1-19
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  • Artikler, rapporter og annet (UB) [3260]
Copyright 2020 The Author(s)

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