Integrative spatiotemporal modeling of biomolecular processes: application to the assembly of the Nuclear Pore Complex

bioRxiv Pub Date : 2024-08-08 DOI:10.1101/2024.08.06.606842
Andrew P. Latham, Jeremy O. B. Tempkin, S. Otsuka, Wanlu Zhang, J. Ellenberg, Andrej Šali
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Abstract

Dynamic processes involving biomolecules are essential for the function of the cell. Here, we introduce an integrative method for computing models of these processes based on multiple heterogeneous sources of information, including time-resolved experimental data and physical models of dynamic processes. We first compute integrative structure models at fixed time points and then optimally select and connect these snapshots into a series of trajectories that optimize the likelihood of both the snapshots and transitions between them. The method is demonstrated by application to the assembly process of the human Nuclear Pore Complex in the context of the reforming nuclear envelope during mitotic cell division, based on live-cell correlated electron tomography, bulk fluorescence correlation spectroscopy-calibrated quantitative live imaging, and a structural model of the fully-assembled Nuclear Pore Complex. Modeling of the assembly process improves the model precision over static integrative structure modeling alone. The method is applicable to a wide range of time-dependent systems in cell biology, and is available to the broader scientific community through an implementation in the open source Integrative Modeling Platform software.
生物分子过程的综合时空建模:应用于核孔复合体的组装
涉及生物分子的动态过程对细胞功能至关重要。在此,我们介绍一种基于多种异构信息源(包括时间分辨实验数据和动态过程物理模型)计算这些过程模型的整合方法。我们首先计算固定时间点的整合结构模型,然后优化选择并将这些快照连接成一系列轨迹,从而优化快照和它们之间转换的可能性。该方法基于活细胞相关电子断层扫描、体荧光相关光谱校准定量活体成像以及完全组装的核孔复合体结构模型,应用于有丝分裂过程中核膜重组背景下人类核孔复合体的组装过程。与单独的静态综合结构建模相比,组装过程建模提高了模型精度。该方法适用于细胞生物学中广泛的随时间变化的系统,并通过开源的整合建模平台软件的实施提供给更广泛的科学界。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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