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首页> 外文期刊>Scientific reports. >Membrane topologies of the PGLa antimicrobial peptide and a transmembrane anchor sequence by Dynamic Nuclear Polarization/solid-state NMR spectroscopy
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Membrane topologies of the PGLa antimicrobial peptide and a transmembrane anchor sequence by Dynamic Nuclear Polarization/solid-state NMR spectroscopy

机译:PGLA抗微生物肽的膜拓扑和动态核偏振/固态NMR光谱通过动态核偏振肽和跨膜锚序列

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Dynamic Nuclear Polarization (DNP) has been introduced to overcome the sensitivity limitations of nuclear magnetic resonance (NMR) spectroscopy also of supported lipid bilayers. When investigated by solid-state NMR techniques the approach typically involves doping the samples with biradicals and their investigation at cryo-temperatures. Here we investigated the effects of temperature and membrane hydration on the topology of amphipathic and hydrophobic membrane polypeptides. Although the antimicrobial PGLa peptide in dimyristoyl phospholipids is particularly sensitive to topological alterations, the DNP conditions represent well its membrane alignment also found in bacterial lipids at ambient temperature. With a novel membrane-anchored biradical and purpose-built hardware a 17-fold enhancement in NMR signal intensity is obtained by DNP which is one of the best obtained for a truly static matrix-free system. Furthermore, a membrane anchor sequence encompassing 19 hydrophobic amino acid residues was investigated. Although at cryotemperatures the transmembrane domain adjusts it membrane tilt angle by about 10 degrees, the temperature dependence of two-dimensional separated field spectra show that freezing the motions can have beneficial effects for the structural analysis of this sequence.
机译:已经引入了动态核偏振(DNP)以克服核磁共振(NMR)光谱也是支持的脂质双层的敏感性限制。当通过固态NMR技术研究时,该方法通常涉及将样品与双抗体和它们的Cryo-Metifys进行调查掺杂。在这里,我们研究了温度和膜水合对两性和疏水膜多肽拓扑的影响。虽然DiMyristoyl磷脂中的抗微生物PGLA肽对拓扑改变特别敏感,但DNP条件也表示在环境温度下的细菌脂质中也发现其膜对准。通过一种新型膜锚定的型肌型和目的构造的硬件,DNP获得了NMR信号强度的17倍的增强,这是真正静态矩阵系统的最佳获得之一。此外,研究了包含19个疏水性氨基酸残基的膜锚序列。虽然在低温培养术处,跨膜结构域将其调节其膜倾斜角度约为10度,但二维分离的场光谱的温度依赖性显示冷冻运动可以对该序列的结构分析具有有益的效果。

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