Complement receptor
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A complement receptor is a membrane-bound receptor belonging to the complement system, which is part of the innate immune system. Complement receptors bind effector protein fragments that are produced in response to antigen-antibody complexes or damage-associated molecules.<ref name="ar14">,
Complement and its receptors: new insights into human disease, Annual Review of Immunology, Vol. 32, pp. 433–59, DOI: 10.1146/annurev-immunol-032713-120154, PMID: 24499275,</ref> Complement receptor activation contributes to the regulation of inflammation, leukocyte extravasation, and phagocytosis; it also contributes to the adaptive immune response.<ref name="cr17">, Complement Receptors, eLS, pp. 1–17, DOI: 10.1002/9780470015902.a0000512.pub3,</ref><ref name="pmid19388161">, Complement and humoral immunity, Vaccine, Vol. 26 Suppl 8(Issue: Suppl 8), pp. I28-33, DOI: 10.1016/j.vaccine.2008.11.022, PMID: 19388161, PMC: 4018718,</ref> Different complement receptors can participate in either the classical complement pathway, the alternative complement pathway, or both.<ref name="Janeway 2001">, Immunobiology: The Immune System in Health and Disease. online version, 5th edition, New York:Garland Science, 2001, Accessed: 2020-06-17.</ref>
Expression and function
White blood cells, particularly monocytes and macrophages, express complement receptors on their surface. All four complement receptors can bind to fragments of complement component 3 or complement component 4 coated on pathogen surface, but the receptors trigger different downstream activities.<ref name="ar14"/> Complement receptor (CR) 1, 3, and 4 function as opsonins which stimulate phagocytosis, whereas CR2 is expressed only on B cells as a co-receptor.
Red blood cells (RBCs) also express CR1, which enables RBCs to carry complement-bound antigen-antibody complexes to the liver and spleen for degradation.<ref>Peter,
The Immune System, 2nd edition, Garland Science, ISBN 9780815340935,</ref>
| CR # | Name | Molecular weight (Da, approx.)<ref name="ar14"/> | Ligand<ref name="Janeway 2001" /> | CD | Major cell types<ref name="Janeway 2001"/>a | Major activities<ref name="ar14"/> |
|---|---|---|---|---|---|---|
| CR1 | Complement receptor 1 | 190,000–250,000 | C3b, C4b, iC3b | CD35 | B, E, FDC, Mac, M0, PMN | Immune complex transport (E); phagocytosis (PMN, Mac); immune adhesion (E); cofactor and decay-acceleration; secondary Epstein-Barr virus receptor |
| CR2 | Complement receptor 2 | 145,000 | C3d, iC3b, C3dg, Epstein-Barr virus | CD21 | B, FDC | B cell coactivator, primary Epstein-Barr virus receptor, CD23 receptor |
| CR3 | Macrophage-1 antigen or "integrin αMβ2" | 170,000 α chain + common 95,000 β chain | iC3b | CD11b+CD18 | FDC, Mac, M0, PMN | Leukocyte adherence, phagocytosis of iC3b-bound particles |
| CR4 | Integrin alphaXbeta2 or "p150,95" | 150,000 α chain + common 95,000 β chain | iC3b | CD11c+CD18 | D, Mac, M0, PMN | Leukocyte adhesion |
| C3AR1 | C3a receptor | 75,000 | C3a | - | Endo, MC, Pha | Cell activation |
| C5AR1 | C5a receptor | 50,000 | C5a | CD88 | Endo, MC, Pha | Cell activation, immune polarization, chemotaxis |
- a.^
B: B cell. E: erythrocyte. Endo: endothelial cell. D: dendritic cell. FDC: follicular dendritic cell. Mac: macrophage. MC: mast cell. M0: monocyte. Pha: phagocyte. PMN: polymorphonuclear leukocyte.
Clinical significance
Deficits in complement receptor expression can cause disease.<ref name="eMedicine Dermatology">
Complement Receptor Deficiency: eMedicine Dermatology(link). Medscape.
Accessed 2010-12-07.
</ref> Mutations in complement receptors which alter receptor function can also increase risk of certain diseases.<ref name="ar14"/>
See also
References
<references group="" responsive="1"></references>
External links
- Complement+receptors at the US National Library of Medicine Medical Subject Headings (MeSH)
| Complement system | ||||||||||
|---|---|---|---|---|---|---|---|---|---|---|
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| Innate immune system: Pattern recognition receptors | ||||||||
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