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Quantitative Glycomics from Fluidic Glycan Microarrays

机译:流体糖微阵列中的定量糖

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摘要

A hallmark of cell-surface processes involving glycans is their multivalent interaction with glycan binding proteins (GBPs). Such a multivalent interaction depends critically on the mobility and density of signaling molecules on the membrane surface. While glycan microarrays have been used in exploring multivalent interactions, the lack of mobility and the difficulty in controlling surface density both limit their quantitative applications. Here we apply a fluidic glycan microarray, with glycan density varying for orders of magnitude, to profile cell surface interaction using a model system, the adhesion of Escherichia coli to mannose. We show the quantitative determination of monovalent and multivalent adhesion channels; the latter can be inhibited by nanopartices presenting a high density of mannosyl groups. These results reveal a new E. coli adhesion mechanism: the switching in the FimH adhesion protein avidity from monovalent to multivalent as the density of mobile mannosyl groups increases; such avidity switching enhances binding affinity and triggers multiple fimbriae anchoring. Affinity enhancement toward FimH has only been observed before for oligo-mannose due to the turn on of secondary interactions outside the mannose binding pocket. We suggest that the new mechanism revealed by the fluidic microarray is of general significance to cell surface interactions: the dynamic clustering of simple sugar groups (homogeneous or heterogeneous) on the fluidic membrane surface may simulate the functions of complex glycan molecules.
机译:涉及聚糖的细胞表面过程的标志是它们与聚糖结合蛋白(GBP)的多价相互作用。这种多价相互作用主要取决于膜表面上信号分子的迁移率和密度。尽管聚糖微阵列已用于探索多价相互作用,但缺乏迁移率和难以控制表面密度都限制了它们的定量应用。在这里,我们应用糖基密度变化几个数量级的流体聚糖微阵列,使用模型系统(即大肠杆菌对甘露糖的粘附力)分析细胞表面相互作用。我们展示了单价和多价粘附通道的定量测定;后者可以被表现出高密度甘露糖基基团的纳米颗粒抑制。这些结果揭示了一种新的大肠杆菌粘附机制:随着移动甘露糖基基团密度的增加,FimH粘附蛋白亲和力从单价转变为多价。这种亲和力切换增强了结合亲和力并触发了多个菌毛锚定。由于甘露糖结合口袋外部的次级相互作用的开启,之前仅对寡甘露糖观察到了对FimH的亲和力增强。我们建议,由流体微阵列揭示的新机制对细胞表面相互作用具有普遍意义:在流体膜表面上简单糖基(均相或异相)的动态聚类可以模拟复杂聚糖分子的功能。

著录项

  • 来源
    《Journal of the American Chemical Society》 |2009年第38期|13646-13650|共5页
  • 作者单位

    Department of Chemistry, University of Minnesota, Minneapolis, Minnesota 55455;

    MicroSurfaces, Inc., 4001 Stinson Boulevard, Suite 430, Minneapolis, Minnesota 55421;

    MicroSurfaces, Inc., 4001 Stinson Boulevard, Suite 430, Minneapolis, Minnesota 55421;

    Department of Biochemistry & Molecular Biology, University of Maryland, Baltimore, Maryland 21201;

    Department of Population Health & Pathobiology, North Carolina State University, Raleigh, North Carolina 27606;

    MicroSurfaces, Inc., 4001 Stinson Boulevard, Suite 430, Minneapolis, Minnesota 55421;

  • 收录信息 美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
  • 原文格式 PDF
  • 正文语种 eng
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  • 入库时间 2022-08-18 03:17:18

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