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


ABSTRACT: 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 ?M?2, 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 ?I domain, and our structure of the C3d:?I domain complex rationalizes the CR3 selectivity for iC3b. Based on extensive structural analysis, we suggest that the choice between a ligand glutamate or aspartate for coordination of a receptor metal ion-dependent adhesion site-bound metal ion is governed by the secondary structure of the ligand. Comparison of our structure to the CR2:C3d complex and the in vitro formation of a stable CR3:C3d:CR2 complex suggests a molecular mechanism for the hand-over of CR3-bound immune complexes from macrophages to CR2-presenting cells in lymph nodes.

SUBMITTER: Bajic G 

PROVIDER: S-EPMC3799375 | biostudies-literature | 2013 Oct

REPOSITORIES: biostudies-literature

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

Bajic Goran G   Yatime Laure L   Sim Robert B RB   Vorup-Jensen Thomas T   Andersen Gregers R GR  

Proceedings of the National Academy of Sciences of the United States of America 20130924 41


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  ...[more]

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