“…Signal regulatory protein α mutant mice, which express a mutant form of SIRPα that lacks most of the cytoplasmic region and thus fail to bind Shp1 and Shp2, manifested mild anemia associated with a short lifetime of RBCs as a result of increased phagocytotic activity of splenic macrophages against RBCs, suggesting the importance of SIRPα for both the lifespan of RBCs and their number in the circulation. In addition, DC‐specific SIRPα knockout mice showed a reduced number of DCs, as well as of fibroblastic reticular cells, a subset of stromal cells, in the spleen . Moreover, SIRPα mutant mice, as well as CD47‐deficient mice, were resistant to the development of autoimmune animal models, such as experimental autoimmune encephalomyelitis, suggesting that the interaction of SIRPα with CD47 is involved in the development of autoimmune diseases.…”