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整合素相关蛋白是镰状红细胞上用于固定化血小板反应蛋白的黏附受体。

Integrin-associated protein is an adhesion receptor on sickle red blood cells for immobilized thrombospondin.

作者信息

Brittain J E, Mlinar K J, Anderson C S, Orringer E P, Parise L V

机构信息

Department of Pharmacology, School of Medicine, The University of North Carolina at Chapel Hill 27599, USA.

出版信息

Blood. 2001 Apr 1;97(7):2159-64. doi: 10.1182/blood.v97.7.2159.

DOI:10.1182/blood.v97.7.2159
PMID:11264185
Abstract

The adhesive protein thrombospondin (TSP) potentially mediates sickle (SS) red blood cell (RBC) adhesion to the blood vessel wall, thereby contributing to vaso-occlusive crises in sickle cell disease. We previously reported that SS RBCs bind to immobilized TSP under flow conditions, whereas normal (AA) red cells do not. However, the SS RBC receptors that mediate this interaction are largely unknown. Here it is reported that integrin-associated protein (IAP), or CD47, mediates the adhesion of these cells to immobilized TSP under both flow and static conditions. A peptide derived from the C-terminal IAP binding site of TSP also supports sickle cell adhesion; adhesion to this peptide or to TSP is inhibited specifically by the anti-IAP monoclonal antibody, 1F7. Furthermore, these data suggest that IAP on SS RBCs is structurally different from that expressed on AA RBCs but that IAP expression levels do not vary between AA and SS RBCs. This structural difference may contribute to the enhanced adhesion of SS RBCs to immobilized TSP. These results identify IAP as a TSP receptor on SS RBCs and suggest that this receptor and its binding site within TSP represent potential therapeutic targets to decrease vaso-occlusion. (Blood. 2001;97:2159-2164)

摘要

黏附蛋白血小板反应蛋白(TSP)可能介导镰状(SS)红细胞(RBC)与血管壁的黏附,从而导致镰状细胞病的血管阻塞性危机。我们先前报道,在流动条件下,SS红细胞可与固定化的TSP结合,而正常(AA)红细胞则不能。然而,介导这种相互作用的SS红细胞受体在很大程度上尚不清楚。本文报道,整合素相关蛋白(IAP)即CD47,在流动和静态条件下均可介导这些细胞与固定化TSP的黏附。源自TSP的C末端IAP结合位点的肽也支持镰状细胞黏附;抗IAP单克隆抗体1F7可特异性抑制与该肽或TSP的黏附。此外,这些数据表明,SS红细胞上的IAP在结构上与AA红细胞上表达的IAP不同,但IAP的表达水平在AA和SS红细胞之间并无差异。这种结构差异可能导致SS红细胞与固定化TSP的黏附增强。这些结果确定IAP为SS红细胞上的TSP受体,并表明该受体及其在TSP内的结合位点代表了减少血管阻塞的潜在治疗靶点。(《血液》。2001年;97:2159 - 2164)

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