Surfactant Protein D (Sp-D) Binds to Membrane-proximal Domain (D3) of Signal Regulatory Protein α (SIRPα), a Site Distant from Binding Domain of CD47, while Also Binding to Analogous Region on Signal Regulatory Protein β (SIRPβ)
| Autor: | Alexander Z. Robin, Dominique A. Weber, Oskar Laur, Charles A. Parkos, Winston Y. Lee, Rakieb Andargachew, Dennis R. Voelker, Bénédicte Fournier |
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| Rok vydání: | 2012 |
| Předmět: |
Glycosylation
Neutrophils Immunology Amino Acid Motifs CD47 Antigen HL-60 Cells CHO Cells Plasma protein binding Immunoglobulin domain Biology Biochemistry Cricetulus Protein structure Cricetinae Animals Humans Amino Acid Sequence Receptors Immunologic Molecular Biology Sequence Deletion Surfactant protein D Cell Biology Pulmonary Surfactant-Associated Protein D Ligand (biochemistry) Antigens Differentiation Transmembrane protein Protein Structure Tertiary Cell biology A-site HEK293 Cells Calcium Protein Binding Binding domain |
| Zdroj: | Journal of Biological Chemistry. 287:19386-19398 |
| ISSN: | 0021-9258 |
| Popis: | Signal regulatory protein α (SIRPα), a highly glycosylated type-1 transmembrane protein, is composed of three immunoglobulin-like extracellular loops as well as a cytoplasmic tail containing three classical tyrosine-based inhibitory motifs. Previous reports indicate that SIRPα binds to humoral pattern recognition molecules in the collectin family, namely surfactant proteins D and A (Sp-D and Sp-A, respectively), which are heavily expressed in the lung and constitute one of the first lines of innate immune defense against pathogens. However, little is known about molecular details of the structural interaction of Sp-D with SIRPs. In the present work, we examined the molecular basis of Sp-D binding to SIRPα using domain-deleted mutant proteins. We report that Sp-D binds to the membrane-proximal Ig domain (D3) of SIRPα in a calcium- and carbohydrate-dependent manner. Mutation of predicted N-glycosylation sites on SIRPα indicates that Sp-D binding is dependent on interactions with specific N-glycosylated residues on the membrane-proximal D3 domain of SIRPα. Given the remarkable sequence similarity of SIRPα to SIRPβ and the lack of known ligands for the latter, we examined Sp-D binding to SIRPβ. Here, we report specific binding of Sp-D to the membrane-proximal D3 domain of SIRPβ. Further studies confirmed that Sp-D binds to SIRPα expressed on human neutrophils and differentiated neutrophil-like cells. Because the other known ligand of SIRPα, CD47, binds to the membrane-distal domain D1, these findings indicate that multiple, distinct, functional ligand binding sites are present on SIRPα that may afford differential regulation of receptor function. |
| Databáze: | OpenAIRE |
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