Over-expression of integrin b3 can partially overcome the defect of integrin b3 signaling in transglutaminase 2 null macrophages
Transglutaminase 2 (TG2) is a protein crosslinking enzyme with many additional biological functions. We have previously shown that in TG2 super(-) super(/) super(-) mice the in vivo clearance of apoptotic cells is defective leading to autoimmunity. TG2 contributes to the formation of phagocytic port...
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| Veröffentlicht in: | Immunology letters 2009-09, Vol.126 (1-2), p.22-28 |
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| container_title | Immunology letters |
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| creator | Toth, B Sarang, Z Vereb, G Zhang, A Tanaka, S Melino, G Fesus, L Szondy, Z |
| description | Transglutaminase 2 (TG2) is a protein crosslinking enzyme with many additional biological functions. We have previously shown that in TG2 super(-) super(/) super(-) mice the in vivo clearance of apoptotic cells is defective leading to autoimmunity. TG2 contributes to the formation of phagocytic portals by binding to both integrin b sub(3), a known phagocytic receptor, and its bridging molecule, MFG-E8. In TG2 null macrophages integrin b sub(3) cannot accumulate around the apoptotic cells and its signaling is impaired. In the present study we describe a subline of TG2 null mice, in which a compensatory increase in integrin b sub(3) expression, which resulted alone in a high receptor concentration around the apoptotic cells without the requirement for accumulation, partially corrected the defect in integrin b sub(3) signaling. Our data provide a proof for the concept that the function of TG2 is to stabilize accumulated integrin b sub(3) concentration in the phagocytic cup. |
| doi_str_mv | 10.1016/j.imlet.2009.07.009 |
| format | Article |
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| title | Over-expression of integrin b3 can partially overcome the defect of integrin b3 signaling in transglutaminase 2 null macrophages |
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