The complement receptors on macrophage are responsible for their binding and ingestion of opsonized targets. The two established receptors are CR1, which recognizes C3b, and CR3, which recognizes iC3b, the natural product of C3b from cleavage by the complement control protein factor I and its cofactors. CR1 belongs to a group of proteins that contain a structural element characterized by its size of 60–65 amino acids, and four conservatively positioned cysteines, which engage in a self-contained 1–3, 2–4 disulphide arrangement. This structural unit is called SCR (short consensus repeat) and is found in the complement proteins Clr, Cls, C2, factor B, factor H, C4BP, DAF, MCP and CR2, each of which interacts with some cleavage products of C3 and/or C4. CR1 has 30 SCR units accounting for its entire extracellular structure. It has a transmembrane segment and a small cytoplasmic domain. CR3 is a heterodimer containing an α and β subunit held together by non-covalent forces. The β subunit is also found in the two leukocyte antigens, LFA-1 and p150,95, which have α subunits distinct from that of CR3. The β subunit contains 56 cysteine residues, 42 of which lie in a span of 256 residues immediately adjacent to the transmembrane segment. It shares extensive sequence homology with subunits of membrane protein complexes that bind fibronectin and vitronectin, implicating that they all belong to an extended set of surface adhesion molecules not restricted to the immune system. p150,95 is also expressed on macrophages and it has iC3b binding activity. It also shares some functional properties with CR3 as an ahesion surface molecule.
C3 receptors on macrophages
S. K. ALEX LAW; C3 receptors on macrophages. J Cell Sci 1 January 1988; 1988 (Supplement_9): 67–97. doi: https://doi.org/10.1242/jcs.1988.Supplement_9.4
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