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A lipid site shapes the agonist response of a pentameric ligand-gated ion channel

机译:脂质部位塑造了五聚体配体门通道的激动剂响应

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摘要

Phospholipids are key components of cellular membranes and are emerging as important functional regulators of different membrane proteins, including pentameric ligand-gated ion channels (pLGICs). Here, we take advantage of the prokaryote channel ELIC (Erwinia ligand-gated ion channel) as a model to understand the determinants of phospholipid interactions in this family of receptors. A high-resolution structure of ELIC in a lipid-bound state reveals a phospholipid site at the lower half of pore-forming transmembrane helices M1 and M4 and at a nearby site for neurosteroids, cholesterol or general anesthetics. This site is shaped by an M4-helix kink and a Trp-Arg-Pro triad that is highly conserved in eukaryote GABA(A/C) and glycine receptors. A combined approach reveals that M4 is intrinsically flexible and that M4 deletions or disruptions of the lipid-binding site accelerate desensitization in ELIC, suggesting that lipid interactions shape the agonist response. Our data offer a structural context for understanding lipid modulation in pLGICs.
机译:磷脂是细胞膜的关键组分,并作为不同膜蛋白的重要功能调节剂,包括五聚体配体镶嵌离子通道(PLGIC)。在这里,我们利用原核频道ELIC(ERWinia配体门通道)作为模型,以了解该受体家族中磷脂相互作用的决定因素。脂质结合状态的ELIC的高分辨率结构揭示了孔形成跨膜螺旋M1和M4的下半部分的磷脂位点,并在附近的神经活体,胆固醇或全部麻醉网站。该网站由M4-Helix Kink和TRP-Arg-Pro Triads塑造,该TRP-ARG-PROD在真核生物GABA(A / C)和甘氨酸受体中高度保守。一种组合的方法表明,M4本质上是柔性的,并且M4缺失或脂质结合位点的破坏加速了ELIC中的脱敏,表明脂质相互作用形状为激动剂反应。我们的数据为理解PLGICS中的脂质调制提供了结构背景。

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  • 来源
    《Nature chemical biology》 |2019年第12期|共12页
  • 作者单位

    Univ Ottawa Dept Biochem Microbiol &

    Immunol Ottawa ON Canada;

    Univ Libre Bruxelles Ctr Struct Biol &

    Bioinformat Lab Struct &

    Funct Biol Membranes Brussels Belgium;

    Katholieke Univ Leuven Dept Cellular &

    Mol Med Lab Struct Neurobiol Leuven Belgium;

    Katholieke Univ Leuven Dept Cellular &

    Mol Med Lab Struct Neurobiol Leuven Belgium;

    Univ Queensland Queensland Brain Inst Brisbane Qld Australia;

    Univ Queensland Queensland Brain Inst Brisbane Qld Australia;

    HiQscreen Geneva Switzerland;

    Vrije Univ Brussel Struct Biol Brussels Brussels Belgium;

    Katholieke Univ Leuven Dept Cellular &

    Mol Med Lab Struct Neurobiol Leuven Belgium;

    Rutgers Univ Camden Ctr Computat &

    Integrat Biol Camden NJ USA;

    TTUHSC Ctr Membrane Prot Res Dept Cell Physiol &

    Mol Biophys Lubbock TX USA;

    TTUHSC Ctr Membrane Prot Res Dept Cell Physiol &

    Mol Biophys Lubbock TX USA;

    Rutgers Univ Camden Ctr Computat &

    Integrat Biol Camden NJ USA;

    Univ Grenoble Alpes CNRS IBS Grenoble France;

    Vrije Univ Brussel Struct Biol Brussels Brussels Belgium;

    Univ Ottawa Dept Biochem Microbiol &

    Immunol Ottawa ON Canada;

    Katholieke Univ Leuven Dept Cellular &

    Mol Med Lab Struct Neurobiol Leuven Belgium;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物化学;
  • 关键词

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