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首页> 外文期刊>ACS Chemical Biology >Photoaffinity Ligand for the Inhalational Anesthetic Sevoflurane Allows Mechanistic Insight into Potassium Channel Modulation
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Photoaffinity Ligand for the Inhalational Anesthetic Sevoflurane Allows Mechanistic Insight into Potassium Channel Modulation

机译:吸入麻醉剂的光亚蜜配体七氟脲允许机械洞察钾通道调制

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摘要

Sevoflurane is a commonly used inhaled general anesthetic. Despite this, its mechanism of action remains largely elusive. Compared to other anesthetics, sevoflurane exhibits distinct functional activity. In particular, sevoflurane is a positive modulator of voltage-gated Shaker-related potassium channels (K(v)1.x), which are key regulators of action potentials. Here, we report the synthesis and validation of azisevoflurane, a photoaffinity ligand for the direct identification of sevoflurane binding sites in the K(v)1.2 channel. Azisevoflurane retains major sevoflurane protein binding interactions and pharmacological properties within in vivo models. Photoactivation of azisevoflurane induces adduction to amino acid residues that accurately reported sevoflurane protein binding sites in model proteins. Pharmacologically relevant concentrations of azisevoflurane analogously potentiated wild-type K(v)1.2 and the established mutant K(v)1.2 G329T. In wild-type K(v)1.2 channels, azisevoflurane photolabeled Leu317 within the internal S4-S5 linker, a vital helix that couples the voltage sensor to the pore region. A residue lining the same binding cavity was photolabeled by azisevoflurane and protected by sevoflurane in the K(v)1.2 G329T. Mutagenesis of Leu317 in WT K(v)1.2 abolished sevoflurane voltage-dependent positive modulation. Azisevoflurane additionally photolabeled a second distinct site at Thr384 near the external selectivity filter in the K(v)1.2 G329T mutant. The identified sevoflurane binding sites are located in critical regions involved in gating of K-v channels and related ion channels. Azisevoflurane has thus emerged as a new tool to discover inhaled anesthetic targets and binding sites and investigate contributions of these targets to general anesthesia.
机译:七氟醚是一种常用的吸入一般麻醉剂。尽管如此,其行动机制仍然很大程度上难以捉摸。与其他麻醉剂相比,七氟醚表现出不同的功能性活性。特别是,七氟醚是电压门控振荡器相关钾通道(K(v)1.x)的正调制器,这是动作电位的关键调节器。在这里,我们报告了AzisevofluRane的合成和验证,光亚戊烷的直接鉴定K(v)1.2沟道中的七氟醚结合位点的直接鉴定。阿扎伊弗洛兰在体内模型中保留了主要的七氟醚蛋白结合相互作用和药理学性质。 AzisevofluRane的光痉挛诱导氨基酸残基的内容,所述氨基酸残基在模型蛋白中准确地报告七氟醚蛋白结合位点。 AzisevofluRane的药理学相关浓度类似地具有增强的野生型K(v)1.2和已建立的突变k(v)1.2 g329t。在野生型K(v)1.2通道中,AzisevofluRane在内部S4-S5接头内的光olabeled Leu317,一个重要的螺旋,使电压传感器耦合到孔区域。衬里的残留物相同的结合腔用阿扎斯韦氟脲光致成标签,并在K(v)1.2g329t中的七氟醚保护。 WT K(v)1.2中Leu317的诱变废除了七氟醚电压依赖性阳性调节。 AzisevofluRane在K(v)1.2g329t突变体中,在外部选择性滤波器附近另外将第二明显部位光刻。所鉴定的七氟醚结合位点位于涉及K-V通道和相关离子通道的临界区域中。因此,AzisevofluRane成为一种新的工具,以发现吸入的麻醉靶和结合位点并调查这些靶标对全身麻醉的贡献。

著录项

  • 来源
    《ACS Chemical Biology》 |2017年第5期|共10页
  • 作者单位

    Univ Penn Perelman Sch Med Dept Anesthesiol &

    Crit Care 3620 Hamilton Walk Philadelphia PA 19104 USA;

    Univ Penn Sch Arts &

    Sci Dept Chem 231 S 34th St Philadelphia PA 19104 USA;

    Thomas Jefferson Univ Sidney Kimmel Med Coll Dept Neurosci 900 Walnut St JHN 417 Philadelphia PA 19107 USA;

    Thomas Jefferson Univ Sidney Kimmel Med Coll Dept Neurosci 900 Walnut St JHN 417 Philadelphia PA 19107 USA;

    Univ Penn Perelman Sch Med Dept Syst Pharmacol &

    Translat Therapeut 3620 Hamilton Walk Philadelphia PA 19104 USA;

    Drexel Univ Dept Biochem &

    Mol Biol Coll Med Philadelphia PA 19129 USA;

    Univ Penn Perelman Sch Med Epigenet Program Dept Biochem &

    Biophys 3400 Civ Ctr Bldg 421 Philadelphia PA 19104 USA;

    Univ Penn Perelman Sch Med Epigenet Program Dept Biochem &

    Biophys 3400 Civ Ctr Bldg 421 Philadelphia PA 19104 USA;

    Thomas Jefferson Univ Sidney Kimmel Med Coll Dept Neurosci 900 Walnut St JHN 417 Philadelphia PA 19107 USA;

    Drexel Univ Dept Biochem &

    Mol Biol Coll Med Philadelphia PA 19129 USA;

    Univ Penn Sch Arts &

    Sci Dept Chem 231 S 34th St Philadelphia PA 19104 USA;

    Univ Penn Perelman Sch Med Dept Anesthesiol &

    Crit Care 3620 Hamilton Walk Philadelphia PA 19104 USA;

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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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