Dectin-1 Is A Major β-Glucan Receptor On Macrophages

酵母多糖 甘露糖受体 受体 单克隆抗体 生物 甘露聚糖 葡聚糖 葡萄聚糖 甘露糖 生物化学 巨噬细胞 补体受体 细胞生物学 补体系统 免疫学 抗体 多糖 体外
作者
Gordon D. Brown,Philip R. Taylor,Delyth M. Reid,Janet A. Willment,David L. Williams,Luisa Martínez‐Pomares,Simon Y. C. Wong,Siamon Gordon
出处
期刊:Journal of Experimental Medicine [Rockefeller University Press]
卷期号:196 (3): 407-412 被引量:974
标识
DOI:10.1084/jem.20020470
摘要

Zymosan is a β-glucan– and mannan-rich particle that is widely used as a cellular activator for examining the numerous responses effected by phagocytes. The macrophage mannose receptor (MR) and complement receptor 3 (CR3) have historically been considered the major macrophage lectins involved in the nonopsonic recognition of these yeast-derived particles. Using specific carbohydrate inhibitors, we show that a β-glucan receptor, but not the MR, is a predominant receptor involved in this process. Furthermore, nonopsonic zymosan binding was unaffected by genetic CD11b deficiency or a blocking monoclonal antibody (mAb) against CR3, demonstrating that CR3 was not the β-glucan receptor mediating this activity. To address the role of the recently described β-glucan receptor, Dectin-1, we generated a novel anti–Dectin-1 mAb, 2A11. Using this mAb, we show here that Dectin-1 was almost exclusively responsible for the β-glucan–dependent, nonopsonic recognition of zymosan by primary macro-phages. These findings define Dectin-1 as the leukocyte β-glucan receptor, first described over 50 years ago, and resolves the long-standing controversy regarding the identity of this important molecule. Furthermore, these results identify Dectin-1 as a new target for examining the immunomodulatory properties of β-glucans for therapeutic drug design.

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