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CD63 is tightly associated with intracellular, secretory events chaperoning piecemeal degranulation and compound exocytosis in human eosinophils

胞吐 CD63 脱颗粒 细胞生物学 生物 分泌物 嗜酸性粒细胞过氧化物酶 嗜酸性阳离子蛋白 四斯潘宁 细胞内 嗜酸性粒细胞 微泡 嗜酸性粒细胞颗粒蛋白 致密颗粒 免疫学 生物化学 细胞 抗体 弓形虫 哮喘 受体 小RNA 基因
作者
Lívia A. S. Carmo,Kennedy Bonjour,Shigeharu Ueki,Josiane S. Neves,Linying Liu,Lisa A. Spencer,Ann M. Dvořàk,Peter F. Weller,Rossana C. N. Melo
出处
期刊:Journal of Leukocyte Biology [Oxford University Press]
卷期号:100 (2): 391-401 被引量:58
标识
DOI:10.1189/jlb.3a1015-480r
摘要

Abstract Eosinophil activation leads to secretion of presynthesized, granule-stored mediators that determine the course of allergic, inflammatory, and immunoregulatory responses. CD63, a member of the transmembrane-4 glycoprotein superfamily (tetraspanins) and present on the limiting membranes of eosinophil-specific (secretory) granules, is considered a potential surface marker for eosinophil degranulation. However, the intracellular secretory trafficking of CD63 in eosinophils and other leukocytes is not understood. Here, we provide a comprehensive investigation of CD63 trafficking at high resolution within human eosinophils stimulated with inflammatory stimuli, CCL11 and tumor necrosis factor α, which induce distinctly differing secretory processes in eosinophils: piecemeal degranulation and compound exocytosis, respectively. By using different transmission electron microscopy approaches, including an immunonanogold technique, for enhanced detection of CD63 at subcellular compartments, we identified a major intracellular pool of CD63 that is directly linked to eosinophil degranulation events. Transmission electron microscopy quantitative analyses demonstrated that, in response to stimulation, CD63 is concentrated within granules undergoing secretion by piecemeal degranulation or compound exocytosis and that CD63 tracks with the movements of vesicles and granules in the cytoplasm. Although CD63 was observed at the cell surface after stimulation, immunonanogold electron microscopy revealed that a strong CD63 pool remains in the cytoplasm. It is remarkable that CCL11 and tumor necrosis factor α triggered increased formation of CD63+ large vesiculotubular carriers (eosinophil sombrero vesicles), which fused with granules in the process of secretion, likely acting in the intracellular translocation of CD63. Altogether, we identified active, intracellular CD63 trafficking connected to eosinophil granule-derived secretory pathways. This is important for understanding the complex secretory activities of eosinophils underlying immune responses.
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