| Literature DB >> 28533443 |
Ádám I Csincsi1, Zsóka Szabó1, Zsófia Bánlaki1, Barbara Uzonyi2, Marcell Cserhalmi1, Éva Kárpáti1, Agustín Tortajada3,4, Joseph J E Caesar5, Zoltán Prohászka6, T Sakari Jokiranta7, Susan M Lea5, Santiago Rodríguez de Córdoba3,4, Mihály Józsi8.
Abstract
Factor H-related protein (FHR) 1 is one of the five human FHRs that share sequence and structural homology with the alternative pathway complement inhibitor FH. Genetic studies on disease associations and functional analyses indicate that FHR-1 enhances complement activation by competitive inhibition of FH binding to some surfaces and immune proteins. We have recently shown that FHR-1 binds to pentraxin 3. In this study, our aim was to investigate whether FHR-1 binds to another pentraxin, C-reactive protein (CRP), analyze the functional relevance of this interaction, and study the role of FHR-1 in complement activation and regulation. FHR-1 did not bind to native, pentameric CRP, but it bound strongly to monomeric CRP via its C-terminal domains. FHR-1 at high concentration competed with FH for CRP binding, indicating possible complement deregulation also on this ligand. FHR-1 did not inhibit regulation of solid-phase C3 convertase by FH and did not inhibit terminal complement complex formation induced by zymosan. On the contrary, by binding C3b, FHR-1 allowed C3 convertase formation and thereby enhanced complement activation. FHR-1/CRP interactions increased complement activation via the classical and alternative pathways on surfaces such as the extracellular matrix and necrotic cells. Altogether, these results identify CRP as a ligand for FHR-1 and suggest that FHR-1 enhances, rather than inhibits, complement activation, which may explain the protective effect of FHR-1 deficiency in age-related macular degeneration.Entities:
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Year: 2017 PMID: 28533443 DOI: 10.4049/jimmunol.1600483
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422