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C 型凝集素受体 MR 和 DC-SIGN 参与对半血蓝蛋白的识别,从而影响其对人类树突状细胞的免疫刺激作用。

C-type lectin receptors MR and DC-SIGN are involved in recognition of hemocyanins, shaping their immunostimulatory effects on human dendritic cells.

机构信息

Fundación Ciencia y Tecnología para el Desarrollo (FUCITED), Santiago, Chile.

Biosonda Corporation, Santiago, Chile.

出版信息

Eur J Immunol. 2021 Jul;51(7):1715-1731. doi: 10.1002/eji.202149225. Epub 2021 May 6.

DOI:10.1002/eji.202149225
PMID:33891704
Abstract

Hemocyanins are used as immunomodulators in clinical applications because they induce a strong Th1-biased cell-mediated immunity, which has beneficial effects. They are multiligand glycosylated molecules with abundant and complex mannose-rich structures. It remains unclear whether these structures influence hemocyanin-induced immunostimulatory processes in human APCs. We have previously shown that hemocyanin glycans from Concholepas concholepas (CCH), Fissurella latimarginata (FLH), and Megathura crenulata (KLH), participate in their immune recognition and immunogenicity in mice, interacting with murine C-type lectin receptors (CLRs). Here, we studied the interactions of these hemocyanins with two major mannose-binding CLRs on monocyte-derived human DCs: MR (mannose receptor) and DC-SIGN (DC-specific ICAM-3-grabbing nonintegrin). Diverse analyses showed that hemocyanins are internalized by a mannose-sensitive mechanism. This process was calcium dependent. Moreover, hemocyanins colocalized with MR and DC-SIGN, and were partly internalized through clathrin-mediated endocytosis. The hemocyanin-mediated proinflammatory cytokine response was impaired when using deglycosylated FLH and KLH compared to CCH. We further showed that hemocyanins bind to human MR and DC-SIGN in a carbohydrate-dependent manner with affinity constants in the physiological concentration range. Overall, we showed that these three clinically valuable hemocyanins interact with human mannose-sensitive CLRs, initiating an immune response and promoting a Th1 cell-driving potential.

摘要

血蓝蛋白在临床应用中被用作免疫调节剂,因为它们诱导强烈的 Th1 偏向的细胞介导免疫,具有有益的作用。它们是多配体糖基化分子,具有丰富而复杂的甘露糖丰富结构。目前尚不清楚这些结构是否影响血蓝蛋白在人类 APC 中诱导免疫刺激过程。我们之前已经表明,来自 Concholepas concholepas(CCH)、Fissurella latimarginata(FLH)和 Megathura crenulata(KLH)的血蓝蛋白糖参与了它们在小鼠中的免疫识别和免疫原性,与小鼠 C 型凝集素受体(CLRs)相互作用。在这里,我们研究了这些血蓝蛋白与单核细胞衍生的人 DC 上的两种主要甘露糖结合 CLR 之间的相互作用:MR(甘露糖受体)和 DC-SIGN(DC 特异性 ICAM-3 抓取非整联蛋白)。多种分析表明,血蓝蛋白通过甘露糖敏感机制被内化。该过程依赖于钙。此外,血蓝蛋白与 MR 和 DC-SIGN 共定位,并通过网格蛋白介导的内吞作用部分内化。与 CCH 相比,用去糖基化的 FLH 和 KLH 处理会损害血蓝蛋白介导的促炎细胞因子反应。我们进一步表明,血蓝蛋白以碳水化合物依赖性方式与人 MR 和 DC-SIGN 结合,亲和力常数在生理浓度范围内。总体而言,我们表明这三种具有临床价值的血蓝蛋白与人类甘露糖敏感的 CLRs 相互作用,引发免疫反应并促进 Th1 细胞驱动潜力。

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