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Dual strategies for peptidoglycan discrimination by peptidoglycan recognition proteins (PGRPs)

机译:通过肽聚糖识别蛋白(PGRP)识别肽聚糖的双重策略

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The innate immune system constitutes the first line of defense against microorganisms in both vertebrates and invertebrates. Although much progress has been made toward identifying key receptors and understanding their role in host defense, far less is known about how these receptors recognize microbial ligands. Such studies have been severely hampered by the need to purify ligands from microbial sources and a reliance on biological assays, rather than direct binding, to monitor recognition. We used synthetic peptidoglycan (PGN) derivatives, combined with microcalo-rimetry, to define the binding specificities of human and insect peptidogycan recognition proteins (PGRPs). We demonstrate that these innate immune receptors use dual strategies to distinguish between PGNs from different bacteria: one based on the composition of the PGN peptide stem and another that senses the peptide bridge crosslinking the stems. To pinpoint the site of PGRPs that mediates discrimination, we engineered structure-based variants having altered PGN-binding properties. The plasticity of the PGRP-binding site revealed by these mutants suggests an intrinsic capacity of the innate immune system to rapidly evolve specificities to meet new microbial challenges.
机译:先天免疫系统是脊椎动物和无脊椎动物中抵御微生物的第一道防线。尽管在识别关键受体和理解其在宿主防御中的作用已取得很大进展,但对这些受体如何识别微生物配体的了解还很少。由于需要从微生物来源纯化配体,并且依赖于生物学分析而不是直接结合来监测识别,因此严重阻碍了此类研究。我们使用合成的肽聚糖(PGN)衍生物,结合微热量测定法,来定义人和昆虫肽聚糖识别蛋白(PGRPs)的结合特异性。我们证明这些先天性免疫受体使用双重策略来区分来自不同细菌的PGN:一种基于PGN肽茎的组成,另一种则是感知交联茎的肽桥。为了查明介导歧视的PGRP的位点,我们设计了具有改变的PGN结合特性的基于结构的变体。这些突变体揭示的PGRP结合位点的可塑性表明,先天免疫系统具有内在的能力,可以迅速进化出特异性以应对新的微生物挑战。

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