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The molecular structure of the Toll-like receptor 3 ligand-binding domain.

机译:Toll样受体3配体结合域的分子结构。

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摘要

Innate immunity is the first line of defense against invading pathogens. Toll-like receptors (TLRs) act as sentinels of the innate immune system, sensing a variety of ligands from lipopolysaccharide to flagellin to dsRNA through their ligand-binding domain that is composed of leucine-rich repeats (LRRs). Ligand binding initiates a signaling cascade that leads to the up-regulation of inflammation mediators. In this study, we have expressed and crystallized the ectodomain (ECD) of human TLR3, which recognizes dsRNA, a molecular signature of viruses, and have determined the molecular structure to 2.4-A resolution. The overall horseshoe-shaped structure of the TLR3-ECD is formed by 23 repeating LRRs that are capped at each end by specialized non-LRR domains. The extensive beta-sheet on the molecule's concave surface forms a platform for several modifications, including insertions in the LRRs and 11 N-linked glycans. The TLR3-ECD structure indicates how LRR loops can establish distinct pathogen recognition receptors.
机译:先天免疫是抵御​​病原体入侵的第一道防线。 Toll样受体(TLR)充当先天免疫系统的前哨,通过其配体结合域(由富含亮氨酸的重复序列(LRR)组成),感知从脂多糖到鞭毛蛋白到dsRNA的各种配体。配体结合启动信号级联反应,导致炎症介质的上调。在这项研究中,我们已经表达并结晶了人类TLR3的胞外域(ECD),该胞外域识别dsRNA(一种病毒的分子标记),并确定了分子结构达到2.4-A分辨率。 TLR3-ECD的整体马蹄形结构由23个重复的LRR组成,每个LRR的末端均被专门的非LRR域所覆盖。分子凹表面上广泛的β-折叠形成了多种修饰的平台,包括插入LRR和11个N-连接的聚糖。 TLR3-ECD结构表明LRR环如何建立独特的病原体识别受体。

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