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A comprehensive simulation framework for imaging single particles and biomolecules at the European X-ray Free-Electron Laser

机译:用于在欧洲X射线自由电子激光器上对单个粒子和生物分子成像的综合模拟框架

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摘要

The advent of newer, brighter, and more coherent X-ray sources, such as X-ray Free-Electron Lasers (XFELs), represents a tremendous growth in the potential to apply coherent X-rays to determine the structure of materials from the micron-scale down to the Angstrom-scale. There is a significant need for a multi-physics simulation framework to perform source-to-detector simulations for a single particle imaging experiment, including (i) the multidimensional simulation of the X-ray source; (ii) simulation of the wave-optics propagation of the coherent XFEL beams; (iii) atomistic modelling of photon-material interactions; (iv) simulation of the time-dependent diffraction process, including incoherent scattering; (v) assembling noisy and incomplete diffraction intensities into a three-dimensional data set using the Expansion-Maximisation-Compression (EMC) algorithm and (vi) phase retrieval to obtain structural information. We demonstrate the framework by simulating a single-particle experiment for a nitrogenase iron protein using parameters of the SPB/SFX instrument of the European XFEL. This exercise demonstrably yields interpretable consequences for structure determination that are crucial yet currently unavailable for experiment design.
机译:诸如X射线自由电子激光器(XFEL)等更新,更明亮,更紧密的X射线源的问世代表着应用相干X射线从微米确定材料结构的潜力的巨大增长-缩小到埃。迫切需要一个多物理场仿真框架来为单个粒子成像实验执行从源到探测器的仿真,其中包括:(i)X射线源的多维仿真; (ii)模拟相干XFEL光束的波光学传播; (iii)光子与材料相互作用的原子建模; (iv)模拟随时间变化的衍射过程,包括非相干散射; (v)使用扩展-最大化-压缩(EMC)算法将嘈杂的和不完全的衍射强度组装到三维数据集中,以及(vi)进行相位检索以获得结构信息。我们通过使用欧洲XFEL的SPB / SFX仪器的参数模拟固氮酶铁蛋白的单颗粒实验来证明该框架。显然,该练习对结构确定产生了可解释的结果,这些结果至关重要,但目前尚无法用于实验设计。

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