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M细胞衍生的囊泡提示了一种独特的跨上皮抗原递送途径。

M cell-derived vesicles suggest a unique pathway for trans-epithelial antigen delivery.

作者信息

Sakhon Olivia S, Ross Brittany, Gusti Veronica, Pham An Joseph, Vu Kathy, Lo David D

机构信息

Division of Biomedical Sciences; School of Medicine ; University of California , Riverside; Riverside, CA USA.

出版信息

Tissue Barriers. 2015 Apr 3;3(1-2):e1004975. doi: 10.1080/21688370.2015.1004975. eCollection 2015.

Abstract

M cells are a subset of mucosal epithelial cells with specialized capability to transport antigens across the mucosal barrier, but there is limited information on antigen transfer in the subepithelial zone due to the challenges in tracking microparticles and antigens that are transcytosed by this unique cell. Using transgenic reporter mice expressing dsRed in the cytoplasm of M cells and EGFP in myeloid cells, we observed that the M cell basolateral pocket hosts a close interaction between B lymphocytes and dendritic cells. Interestingly, we identified a population of previously undescribed M cell-derived vesicles (MCM) that are constitutively shed into the subepithelial space and readily taken up by CX3CR1(+)CD11b(+) CD11c(+) dendritic cells. These MCM are characterized by their cytoplasmic dsRed confirming their origin from the M cell cytoplasm. MCM showed preferential colocalization in dendritic cells with transcytosed bacteria but not transcytosed polystyrene beads, indicating a selective sorting of cargo fate in the subepithelial zone. The size and number of MCM were found to be upregulated by bacterial transcytosis and soluble toll-like receptor 2 (TLR2) agonist, further pointing to dynamic regulation of this mechanism. These results suggest that MCM provide a unique function by delivering to dendritic cells, various materials such as M cell-derived proteins, effector proteins, toxins, and particles found in the M cell cytoplasm during infection or surveillance.

摘要

M细胞是黏膜上皮细胞的一个亚群,具有将抗原转运穿过黏膜屏障的特殊能力,但由于追踪被这种独特细胞转胞吞的微粒和抗原存在挑战,关于上皮下区域抗原转运的信息有限。利用在M细胞胞质中表达dsRed且在髓样细胞中表达EGFP的转基因报告小鼠,我们观察到M细胞基底外侧袋内B淋巴细胞和树突状细胞之间存在紧密相互作用。有趣的是,我们鉴定出一群先前未描述过的M细胞衍生囊泡(MCM),它们持续脱落到上皮下间隙,并容易被CX3CR1(+)CD11b(+)CD11c(+)树突状细胞摄取。这些MCM的特征是其胞质中有dsRed,证实它们起源于M细胞胞质。MCM在树突状细胞中与转胞吞的细菌而非转胞吞的聚苯乙烯珠优先共定位,表明上皮下区域货物命运存在选择性分选。发现MCM的大小和数量因细菌转胞吞作用和可溶性Toll样受体2(TLR2)激动剂而上调,进一步表明该机制的动态调节。这些结果表明,MCM通过在感染或监测期间将M细胞胞质中发现的各种物质,如M细胞衍生蛋白、效应蛋白、毒素和颗粒递送至树突状细胞,发挥独特功能。

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