Jolley Craig C, Wells Stephen A, Fromme Petra, Thorpe M F
Center for Biological Physics, Bateman Physical Sciences, Arizona State University, Tempe, Arizona, USA.
Biophys J. 2008 Mar 1;94(5):1613-21. doi: 10.1529/biophysj.107.115949. Epub 2007 Nov 9.
Recent experimental advances in producing density maps from cryo-electron microscopy (cryo-EM) have challenged theorists to develop improved techniques to provide structural models that are consistent with the data and that preserve all the local stereochemistry associated with the biomolecule. We develop a new technique that maintains the local geometry and chemistry at each stage of the fitting procedure. A geometric simulation is used to drive the structure from some appropriate starting point (a nearby experimental structure or a modeled structure) toward the experimental density, via a set of small incremental motions. Structural motifs such as alpha-helices can be held rigid during the fitting procedure as the starting structure is brought into alignment with the experimental density. After validating this procedure on simulated data for adenylate kinase and lactoferrin, we show how cryo-EM data for two different GroEL structures can be fit using a starting x-ray crystal structure. We show that by incorporating the correct local stereochemistry in the modeling, structures can be obtained with effective resolution that is significantly higher than might be expected from the nominal cryo-EM resolution.
近期,利用冷冻电子显微镜(cryo-EM)生成密度图的实验进展,促使理论学家开发改进技术,以提供与数据一致且保留与生物分子相关的所有局部立体化学信息的结构模型。我们开发了一种新技术,在拟合过程的每个阶段都能保持局部几何形状和化学性质。通过一组小的增量运动,利用几何模拟将结构从某个合适的起始点(附近的实验结构或建模结构)驱动至实验密度。在将起始结构与实验密度对齐的拟合过程中,诸如α-螺旋等结构基序可以保持刚性。在对腺苷酸激酶和乳铁蛋白的模拟数据验证此过程后,我们展示了如何使用起始X射线晶体结构来拟合两种不同GroEL结构的冷冻电子显微镜数据。我们表明,通过在建模中纳入正确的局部立体化学信息,可以获得有效分辨率显著高于名义冷冻电子显微镜分辨率预期的结构。