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首页> 外文期刊>Structure >D-Serine Potently Drives Ligand-Binding Domain Closure in the Ionotropic Glutamate Receptor GluD2
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D-Serine Potently Drives Ligand-Binding Domain Closure in the Ionotropic Glutamate Receptor GluD2

机译:D-丝氨酸在离子辐射谷氨酸受体GLUD2中易于驱动配体结合域闭合

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摘要

Despite their classification as ionotropic glutamate receptors, GluD receptors are not functional ligand-gated ion channels and do not bind glutamate. GluD2 receptors bind D-serine and coordinate transsynaptic complexes that regulate synaptic plasticity. Instead of opening the ion channel pore, mechanical tension produced from closure of GluD2 ligand-binding domains (LBDs) drives conformational rearrangements for non-ionotropic signaling. We report computed conformational free energy landscapes for the GluD2 LBD in apo and D-serine-bound states. Unexpectedly, the conformational free energy associated with GluD2 LBD closure upon D-serine binding is greater than that for AMPA, NMDA, and kainate receptor LBDs upon agonist binding. This excludes insufficient force generation as an explanation for lack of ion channel activity in GluD2 receptors and suggests that non-ionotropic conformational rearrangements do more work than pore opening. We also report free energy landscapes for GluD2 LBD harboring a neurodegenerative mutation and demonstrate selective stabilization of closed conformations in the apo state.
机译:None

著录项

  • 来源
    《Structure》 |2020年第10期|共13页
  • 作者单位

    Johns Hopkins Univ Dept Biophys &

    Biophys Chem Sch Med Baltimore MD 21205 USA;

    Johns Hopkins Univ Dept Biophys &

    Biophys Chem Sch Med Baltimore MD 21205 USA;

    Johns Hopkins Univ Dept Biophys &

    Biophys Chem Sch Med Baltimore MD 21205 USA;

    Johns Hopkins Univ Dept Biophys &

    Biophys Chem Sch Med Baltimore MD 21205 USA;

    Johns Hopkins Univ Dept Biophys &

    Biophys Chem Sch Med Baltimore MD 21205 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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