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利用重组入荧光脂质体的CD23证明免疫球蛋白E低亲和力受体(CD23)的第二种配体。

Demonstration of a second ligand for the low affinity receptor for immunoglobulin E (CD23) using recombinant CD23 reconstituted into fluorescent liposomes.

作者信息

Pochon S, Graber P, Yeager M, Jansen K, Bernard A R, Aubry J P, Bonnefoy J Y

机构信息

Glaxo Institute for Molecular Biology, Plan-Les-Ouates, Geneva, Switzerland.

出版信息

J Exp Med. 1992 Aug 1;176(2):389-97. doi: 10.1084/jem.176.2.389.

Abstract

Recombinant full-length human CD23 has been incorporated into fluorescent liposomes to demonstrate the existence of a ligand for CD23 that is different from the previously known ligand, immunoglobulin E (IgE). The novel ligand for CD23 is expressed on subsets of normal T cells and B cells as well as on some myeloma cell lines. The interaction of full-length CD23 with its ligand is specifically inhibited by anti-CD23 monoclonal antibodies and by IgE, and it is Ca2+ dependent. Moreover, tunicamycin treatment of a CD23-binding cell line, RPMI 8226, significantly reduced the binding of CD23 incorporated into fluorescent liposomes, and a sugar, fucose-1-phosphate, was found to inhibit CD23-liposome binding to RPMI 8226 cells, suggesting the contribution of sugar structures on the CD23 ligand. In addition, CD23-transfected COS cells were shown to form specific conjugates with the cell line RPMI 8226. These data demonstrate that CD23 interacts with a ligand, which is different from IgE, and that CD23 can be considered as a new surface adhesion molecule involved in cell-cell interactions.

摘要

重组全长人CD23已被整合到荧光脂质体中,以证明存在一种不同于先前已知配体免疫球蛋白E(IgE)的CD23配体。CD23的新型配体在正常T细胞和B细胞亚群以及一些骨髓瘤细胞系上表达。全长CD23与其配体的相互作用被抗CD23单克隆抗体和IgE特异性抑制,并且它依赖于Ca2+。此外,用衣霉素处理CD23结合细胞系RPMI 8226,显著降低了整合到荧光脂质体中的CD23的结合,并且发现一种糖,岩藻糖-1-磷酸,可抑制CD23脂质体与RPMI 8226细胞的结合,这表明糖结构对CD23配体有贡献。此外,已证明转染CD23的COS细胞与细胞系RPMI 8226形成特异性结合物。这些数据表明CD23与一种不同于IgE的配体相互作用,并且CD23可被视为参与细胞间相互作用的一种新的表面粘附分子。

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