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CD169 mediates the capture of exosomes in spleen and lymph node

机译:CD169介导脾和淋巴结中外来体的捕获

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摘要

Exosomes are lipid nanovesicles released following fusion of the endosoma limiting membrane with the plasma membrane; however, their fate in lymphoid organs after their release remains controversial. We determined that sialoadhesin (CD169; Siglec-1) is required for the capture of B cell-derived exosomes via their surface-expressed α2,3- linked sialic acids. Exosome-capturing macrophages were present in the marginal zone of the spleen and in the subcapsular sinus of the lymph node. In vitro assays performed on spleen and lymph node sections confirmed that exosome binding to CD169 was not solely due to preferential fluid flow to these areas. Although the circulation half-life of exosomes in blood of wild-type and CD169-/- mice was similar, exosomes displayed altered distribution in CD169-/- mice, with exosomes freely accessing the outer marginal zone rim of SIGN-R1+ macrophages and F4/80+ red pulp macrophages. In the lymph node, exosomes were not retained in the subcapsular sinus of CD169-/- mice but penetrated deeper into the paracortex. Interestingly, CD169-/- mice demonstrated an enhanced response to antigen-pulsed exosomes. This is the first report of a role for CD169 in the capture of exosomes and its potential to mediate the immune response to exosomal antigen. (Blood. 2014;123(2):208-216).
机译:外泌体是内体限制膜与质膜融合后释放的脂质纳米囊泡。然而,它们在释放后在淋巴器官中的命运仍然存在争议。我们确定唾液酸粘附素(CD169; Siglec-1)是通过表面表达的α2,3-连接的唾液酸捕获B细胞来源的外泌体所必需的。捕获外泌体的巨噬细胞存在于脾的边缘区域和淋巴结的囊下窦中。在脾脏和淋巴结切片上进行的体外测定证实,外泌体与CD169的结合不仅是由于优先的液体流向这些区域。尽管外泌体在野生型和CD169-/-小鼠血液中的循环半衰期相似,但外泌体在CD169-/-小鼠中显示出分布改变,外泌体可自由进入SIGN-R1 +巨噬细胞和F4的外缘区域边缘/ 80 +红浆巨噬细胞。在淋巴结中,外泌体未保留在CD169-/-小鼠的荚膜下窦中,而是更深地渗入了皮层旁。有趣的是,CD169-/-小鼠表现出对抗原脉冲外泌体的增强反应。这是关于CD169在捕获外泌体中的作用及其介导针对外泌体抗原的免疫反应的潜力的首次报道。 (Blood.2014; 123(2):208-216)。

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