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迭代螺旋实空间重建方法在P型ATP酶大膜状管状晶体中的应用。

Application of the iterative helical real-space reconstruction method to large membranous tubular crystals of P-type ATPases.

作者信息

Pomfret Andrew J, Rice William J, Stokes David L

机构信息

Skirball Institute of Biomolecular Medicine, Department of Cell Biology, New York University School of Medicine, New York, NY 10016, USA.

出版信息

J Struct Biol. 2007 Jan;157(1):106-16. doi: 10.1016/j.jsb.2006.05.012. Epub 2006 Jun 14.

DOI:10.1016/j.jsb.2006.05.012
PMID:16879984
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4040983/
Abstract

Since the development of three-dimensional helical reconstruction methods in the 1960's, advances in Fourier-Bessel methods have facilitated structure determination to near-atomic resolution. A recently developed iterative helical real-space reconstruction (IHRSR) method provides an alternative that uses single-particle analysis in conjunction with the imposition of helical symmetry. In this work, we have adapted the IHRSR algorithm to work with frozen-hydrated tubular crystals of P-type ATPases. In particular, we have implemented layer-line filtering to improve the signal-to-noise ratio, Wiener-filtering to compensate for the contrast transfer function, solvent flattening to improve reference reconstructions, out-of-plane tilt compensation to deal with flexibility in three dimensions, systematic calculation of Fourier shell correlations to track the progress of the refinement, and tools to control parameters as the refinement progresses. We have tested this procedure on datasets from Na(+)/K(+)-ATPase, rabbit skeletal Ca(2+)-ATPase and scallop Ca(2+)-ATPase in order to evaluate the potential for sub-nanometer resolution as well as the robustness in the presence of disorder. We found that Fourier-Bessel methods perform better for well-ordered samples of skeletal Ca(2+)-ATPase and Na(+)/K(+)-ATPase, although improvements to IHRSR are discussed that should reduce this disparity. On the other hand, IHRSR was very effective for scallop Ca(2+)-ATPase, which was too disordered to analyze by Fourier-Bessel methods.

摘要

自20世纪60年代三维螺旋重建方法发展以来,傅里叶-贝塞尔方法的进步推动了结构测定达到近原子分辨率。最近开发的迭代螺旋实空间重建(IHRSR)方法提供了一种替代方案,该方法将单颗粒分析与螺旋对称性的施加相结合。在这项工作中,我们对IHRSR算法进行了调整,使其适用于P型ATP酶的冷冻水合管状晶体。具体而言,我们实施了层线滤波以提高信噪比,维纳滤波以补偿对比度传递函数,溶剂扁平化以改善参考重建,平面外倾斜补偿以处理三维中的灵活性,系统计算傅里叶壳层相关性以跟踪细化进度,以及在细化过程中控制参数的工具。我们在来自钠钾ATP酶、兔骨骼肌钙ATP酶和扇贝钙ATP酶的数据集上测试了该程序,以评估亚纳米分辨率的潜力以及在存在无序情况下的稳健性。我们发现,傅里叶-贝塞尔方法对于骨骼肌钙ATP酶和钠钾ATP酶的有序样本表现更好,尽管讨论了对IHRSR的改进,这些改进应减少这种差异。另一方面,IHRSR对扇贝钙ATP酶非常有效,该酶过于无序,无法通过傅里叶-贝塞尔方法进行分析。

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