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On the Combined Analysis of 2H and 15N/1H Solid-State NMR Data for Determination of Transmembrane Peptide Orientation and Dynamics

机译:2H和15N / 1H固态NMR数据的组合分析用于确定跨膜肽的方向和动力学

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摘要

The dynamics of membrane-spanning peptides have a strong affect on the solid-state NMR observables. We present a combined analysis of 2H-alanine quadrupolar splittings together with 15N/1H dipolar couplings and 15N chemical shifts, using two models to treat the dynamics, for the systematic evaluation of transmembrane peptides based on the GWALP23 sequence (acetyl-GGALW(LA)6LWLAGA-amide). The results indicate that derivatives of GWALP23 incorporating diverse guest residues adopt a range of apparent tilt angles that span 5°–35° in lipid bilayer membranes. By comparing individual and combined analyses of specifically 2H- or 15N-labeled peptides incorporated in magnetically or mechanically aligned lipid bilayers, we examine the influence of data-set size/identity, and of explicitly modeled dynamics, on the deduced average orientations of the peptides. We conclude that peptides with small apparent tilt values (<∼10°) can be fitted by extensive families of solutions, which can be narrowed by incorporating additional 15N as well as 2H restraints. Conversely, peptides exhibiting larger tilt angles display more narrow distributions of tilt and rotation that can be fitted using smaller sets of experimental constraints or even with 2H or 15N data alone. Importantly, for peptides that tilt significantly more than 10° from the bilayer-normal, the contribution from rigid body dynamics can be approximated by a principal order parameter.
机译:跨膜肽的动力学对固态NMR观测值有很大影响。我们对 2 H-丙氨酸四极分裂以及 15 N / 1 H双极偶合和 15 N化学位移,使用两种模型处理动力学,以基于GWALP23序列(乙酰基-GGALW(LA)6LWLAGA-酰胺)对跨膜肽进行系统评估。结果表明,包含多种客体残基的GWALP23衍生物在脂质双层膜中采用了范围为5°–35°的表观倾斜角。通过比较分别结合到磁性或机械排列的脂质双层中的 2 H-或 15 N标记的肽的单独和组合分析,我们研究了数据集大小/推导的肽的平均方向上的相同性和显式建模的动力学。我们得出结论,表观倾斜值(<〜10°)小的肽可以被广泛的溶液系列所拟合,可以通过加入额外的 15 N和 2 H约束。相反,具有较大倾斜角的肽显示的倾斜度和旋转度分布更窄,可以使用较小的实验约束集甚至仅使用 2 H或 15 N数据进行拟合。重要的是,对于从双层法线倾斜超过10°的肽,刚体动力学的贡献可以通过主阶参数来近似。

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