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Ly6C+ monocyte efferocytosis and cross-presentation of cell-associated antigens

机译:Ly6C +单核细胞的放血和细胞相关抗原的交叉呈递

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摘要

Recently it was shown that circulating Ly6C+ monocytes traffic from tissue to the draining lymph nodes (LNs) with minimal alteration in their overall phenotype. Furthermore, in the steady state, Ly6C+ monocytes are as abundant as classical dendritic cells (DCs) within the draining LNs, and even more abundant during inflammation. However, little is known about the functional roles of constitutively trafficking Ly6C+ monocytes. In this study we investigated whether Ly6C+ monocytes can efferocytose (acquire dying cells) and cross-present cell-associated antigen, a functional property particularly attributed to Batf3+ DCs. We demonstrated that Ly6C+ monocytes intrinsically efferocytose and cross-present cell-associated antigen to CD8+ T cells. In addition, efferocytosis was enhanced upon direct activation of the Ly6C+ monocytes through its corresponding TLRs, TLR4 and TLR7. However, only ligation of TLR7, and not TLR4, enhanced cross-presentation by Ly6C+ monocytes. Overall, this study outlines two functional roles, among others, that Ly6C+ monocytes have during an adaptive immune response.
机译:最近发现,循环中的Ly6C + 单核细胞从组织流向引流淋巴结(LNs),其总体表型变化最小。此外,在稳定状态下,Ly6C + 单核细胞与引流LN中的经典树突状细胞(DC)一样丰富,在炎症过程中甚至更为丰富。然而,关于组成型运输Ly6C + 单核细胞的功能作用了解甚少。在这项研究中,我们研究了Ly6C + 单核细胞是否能使细胞凋亡(获得垂死细胞)和交叉呈递与细胞相关的抗原,这种功能特性特别归因于Batf3 + DC。我们证明了Ly6C + 单核细胞具有内在的胞吞作用,并能交叉呈递细胞相关抗原至CD8 + T细胞。此外,通过其对应的TLR,TLR4和TLR7直接激活Ly6C + 单核细胞,增强了胞吐作用。然而,仅TLR7的连接而不是TLR4的连接增强了Ly6C + 单核细胞的交叉呈递。总体而言,这项研究概述了Ly6C + 单核细胞在适应性免疫应答中具有的两个功能性作用。

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