The ‘metabolon’, CD47, and the ‘phagocytic synapse’: molecular co-localization and species divergence

钙网蛋白 CD47型 生物 糖蛋白 细胞生物学 红细胞 化学 血浆蛋白结合 唾液酸糖蛋白 膜蛋白 免疫突触 吞噬作用 生物化学 内质网
作者
Shyamsundar Subramanian,Richard K. Tsai,Dennis E. Discher
出处
期刊:Transfusion Clinique Et Biologique [Elsevier]
卷期号:13 (1-2): 31-38 被引量:16
标识
DOI:10.1016/j.tracli.2006.02.009
摘要

CD47 is a widely expressed integral membrane protein, found also on red blood cells where it reportedly has a key role in inhibiting phagocytic clearance of RBC by signaling within a multi-molecular ‘phagocytic synapse’. Calreticulin is postulated to be on the RBC surface and stimulate phagocytosis, whereupon CD47 on the RBC binds SIRPα on the phagocyte and signals a block against phagocytosis. While studies of mouse suggest such an inhibitory role for CD47, CD47 seems to have distinct interactions in human RBC—particularly within a ‘metabolon’ complex of CD47, Rh proteins, and several other proteins. We have assessed the relative density, co-clustering, and mobility of some of the implicated proteins on human RBC versus murine RBC (hu-RBC and mu-RBC, respectively), and we find a few major differences. While RBC from both species express similar densities of CD47 and SIRPα interactions are measurably modest, the interactions prove species-specific. While RBC from both species also have detectable calreticulin, fresh hu-RBC are found to have 10–100-fold more calreticulin binding sites on their surface. Imaging of clusters of SIRPα-CD47 on both species of RBC show that RhD does co-localize with CD47 on hu-RBC, but neither calreticulin nor Glycophorin-A appear enriched in the metabolon complexes. Furthermore, mouse-cells alone tend to aggregate due to cross-bridging by SIRPα complexes, showing accumulation of CD47 in the adhesion zone, which is consistent with a high mobility of CD47 unique to mu-RBC.
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