The crystal structure of iC3b-CR3 αI reveals a modular recognition of the main opsonin iC3b by the CR3 integrin receptor

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作者
Francisco J. Fernández
Jorge Santos-López
Rubén Martínez-Barricarte
Javier Querol-García
Héctor Martín-Merinero
Sergio Navas-Yuste
Martin Savko
William E. Shepard
Santiago Rodríguez de Córdoba
M. Cristina Vega
机构
[1] Agencia Estatal Consejo Superior de Investigaciones Científicas,Centro de Investigaciones Biológicas Margarita Salas
[2] Abvance Biotech srl,Synchrotron SOLEIL
[3] Centro de Investigación Biomédica en Enfermedades Raras,Division of Genetic Medicine, Department of Medicine
[4] L’Orme des Merisiers Saint-Aubin,undefined
[5] Vanderbilt University Medical Center,undefined
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Complement activation on cell surfaces leads to the massive deposition of C3b, iC3b, and C3dg, the main complement opsonins. Recognition of iC3b by complement receptor type 3 (CR3) fosters pathogen opsonophagocytosis by macrophages and the stimulation of adaptive immunity by complement-opsonized antigens. Here, we present the crystallographic structure of the complex between human iC3b and the von Willebrand A inserted domain of the α chain of CR3 (αI). The crystal contains two composite interfaces for CR3 αI, encompassing distinct sets of contiguous macroglobulin (MG) domains on the C3c moiety, MG1-MG2 and MG6-MG7 domains. These composite binding sites define two iC3b-CR3 αI complexes characterized by specific rearrangements of the two semi-independent modules, C3c moiety and TED domain. Furthermore, we show the structure of iC3b in a physiologically-relevant extended conformation. Based on previously available data and novel insights reported herein, we propose an integrative model that reconciles conflicting facts about iC3b structure and function and explains the molecular basis for iC3b selective recognition by CR3 on opsonized surfaces.
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