The distinct leukocyte integrins of mouse spleen dendritic cells as identified with new hamster monoclonal antibodies.

生物 CD11c公司 分子生物学 整合素 整合素αM 单克隆抗体 脾脏 表位 CD18型 树突状细胞 细胞生物学 CD49b 滤泡树突状细胞 抗原提呈细胞 抗体 T细胞 免疫系统 免疫学 流式细胞术 细胞 表型 生物化学 基因
作者
Joshua P. Metlay,Margit D. Witmer-Pack,Ralf Agger,Mary T. Crowley,D Lawless,Ralph M. Steinman
出处
期刊:Journal of Experimental Medicine [Rockefeller University Press]
卷期号:171 (5): 1753-1771 被引量:563
标识
DOI:10.1084/jem.171.5.1753
摘要

Hybridoma fusions with hamster hosts were undertaken to generate mAbs to mouse spleen dendritic cells. Two mAb were obtained and used to uncover the distinct integrins of these APC. One, 2E6, bound a determinant common to all members of the CD11/CD18 family, most likely the shared 90 kD CD18 beta chain. 2E6 immunoprecipitated the characteristic beta 2 integrin heterodimers from lymphocytes (p180, 90; CD11a) and macrophages (p170,90; CD11b), but from dendritic cells, a p150,90 (presumably CD11c) integrin was the predominant species. 2E6 inhibited the binding function of the CD11a and CD11b integrins on B cells and macrophages in appropriate assays, but 2E6 exerted little or no inhibition on the clustering of dendritic cells to T cells early in primary MLR, suggesting a CD11/CD18-independent mechanism for this binding. The second mAb, N418, precipitated a 150, 90 kD heterodimer that shared the 2E6 CD18 epitope. This N418 epitope may be the murine homologue of the previously characterized human CD11c molecule, but the epitope was only detected on dendritic cells. N418 did not react with peritoneal macrophages, anti-Ig-induced spleen B blasts, or bulk lymph node cells. When used to stain sections of spleen, N418 stained dendritic cells in the T-dependent areas, much like anti-class II mAbs that were also generated in these fusions. In addition, N418 revealed nests of dendritic cells that punctuated the rim of marginal zone macrophages between red and white pulp. This localization positioned most dendritic cells at regions where arterial vessels and T cells enter the white pulp. We conclude that the p150, 90 heterodimer is the major beta 2 integrin of spleen dendritic cells, and we speculate that it may function to localize these APC at sites that permit access to the recirculating pool of resting T cells.

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