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首页> 外文期刊>Frontiers in Pharmacology >Hydrogen-Deuterium Exchange Mass-Spectrometry of Secondary Active Transporters: From Structural Dynamics to Molecular Mechanisms
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Hydrogen-Deuterium Exchange Mass-Spectrometry of Secondary Active Transporters: From Structural Dynamics to Molecular Mechanisms

机译:二次活性转运液的氢 - 氘交换质谱:从结构动力学到分子机制

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Membrane transporters allow the selective transport of otherwise poorly permeable solutes across the cell membrane and thus, play a key role in maintaining cellular homeostasis in all kingdoms of life. Importantly, these proteins also serve as important drug targets. Over the last decades, major progress in structural biology methods has elucidated important structure-function relationships in membrane transporters. However, structures obtained using methods such as X-ray crystallography and high-resolution cryogenic electron microscopy merely provide static snapshots of an intrinsically dynamic, multi-step transport process. Therefore, there is a growing need for developing new experimental approaches capable of exploiting the data obtained from the high-resolution snapshots in order to investigate the dynamic features of membrane proteins. Here, we present the basic principles of hydrogen-deuterium exchange mass-spectrometry (HDX-MS) and recent advancements in its use to study membrane transporters. In HDX-MS experiments, minute amounts of a protein sample can be used to investigate its structural dynamics under native conditions, without the need for chemical labelling and with practically no limit on the protein size. Thus, HDX-MS is instrumental for resolving the structure-dynamic landscapes of membrane proteins in their apo (ligand-free) and ligand-bound forms, shedding light on the molecular mechanism underlying the transport process and drug binding.
机译:膜转运蛋白允许在细胞膜上选择差别透明溶质的选择性旋转,从而在维持所有生命界的细胞稳态中起着关键作用。重要的是,这些蛋白质也作为重要的药物靶标。在过去的几十年中,结构生物学方法的主要进步阐述了膜转运蛋白中的重要结构功能关系。然而,使用诸如X射线晶体学和高分辨率低温电磁学显微镜等方法获得的结构仅仅提供了本质上动态,多步运输过程的静态快照。因此,越来越需要开发能够利用高分辨率快照获​​得的数据的新实验方法,以便研究膜蛋白的动态特征。在这里,我们介绍了氢 - 氘交换质谱(HDX-MS)的基本原理和用于研究膜转运蛋白的最近进步。在HDX-MS实验中,可以使用微量蛋白质样品在天然条件下研究其结构动态,而无需化学标记,并且实际上没有限制蛋白质。因此,HDX-MS是用于在其APO(无配体)和配体粘合的形式中的膜蛋白的结构 - 动态景观,脱落在运输过程和药物结合的分子机制上的结构 - 动态景观。

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