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Structural insight on the recognition of surface-bound opsonins by the integrin I domain of complement receptor 3.

Proc Natl Acad Sci U S A.. 2013-09; 
Bajic G, Yatime L, Sim RB, Vorup-Jensen T, Andersen GR. Departments of Molecular Biology and Genetics and Biomedicine, Aarhus University, DK-8000 Aarhus, Denmark.
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摘要

Complement receptors (CRs), expressed notably on myeloid and lymphoid cells, play an essential function in the elimination of complement-opsonized pathogens and apoptotic/necrotic cells. In addition, these receptors are crucial for the cross-talk between the innate and adaptive branches of the immune system. CR3 (also known as Mac-1, integrin αMβ2, or CD11b/CD18) is expressed on all macrophages and recognizes iC3b on complement-opsonized objects, enabling their phagocytosis. We demonstrate that the C3d moiety of iC3b harbors the binding site for the CR3 αI domain, and our structure of the C3d:αI domain complex rationalizes the CR3 selectivity for iC3b. Based on extensive structural analys... More

关键词

innate immunity; integrin receptor; phagocytosis; structural biology