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The filament forming reactions of vimentin tetramers studied in a serial-inlet microflow device by small angle x-ray scattering

机译:波形蛋白四聚体的长丝形成反应在串联入口微流装置中通过小角度X射线散射研究

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摘要

The structural organization of metazoan cells and their shape are established through the coordinated interaction of a composite network consisting of three individual filament systems, collectively termed the cytoskeleton. Specifically, microtubules and actin filaments, which assemble from monomeric globular proteins, provide polar structures that serve motor proteins as tracks. In contrast, intermediate filaments (IFs) assemble from highly charged, extended coiled coils in a hierarchical assembly mechanism of lateral and longitudinal interaction steps into non-polar structures. IF proteins are expressed in a distinctly tissue-specific way and thereby serve to generate the precise plasticity of the respective cells and tissues. Accordingly, in the cell, numerous parameters such as pH and salt concentration are adjusted such that the generation of functional networks is ensured. Here, we transfer the problem for the mesenchymal IF protein vimentin to an in vitro setting and combine small angle x-ray scattering with microfluidics and finite element method simulations. Our approach is adapted to resolve the early assembly steps, which take place in the sub-second to second range. In particular, we reveal the influence of ion species and concentrations on the assembly. By tuning the flow rates and thus concentration profiles, we find a minimal critical salt concentration for the initiation of the assembly. Furthermore, our analysis of the surface sensitive Porod regime in the x-ray data reveals that the formation of first assembly intermediates, so-called unit length filaments, is not a one-step reaction but consists of distinct consecutive lateral association steps followed by radial compaction as well as smoothening of the surface of the full-width filament.
机译:后生动物细胞的结构组织及其形状是通过由三个单独的细丝系统(统称为细胞骨架)组成的复合网络的协调相互作用而建立的。具体而言,由单体球状蛋白组装而成的微管和肌动蛋白丝提供了极性结构,将运动蛋白用作轨道。相比之下,中间丝(IF)由高度带电的扩展线圈以横向和纵向相互作用步骤的分层组装机制组装成非极性结构。 IF蛋白以明显的组织特异性方式表达,从而用于产生各个细胞和组织的精确可塑性。因此,在电池中,调节许多参数,例如pH和盐浓度,以确保功能网络的产生。在这里,我们将间质IF蛋白波形蛋白的问题转移到体外,并将小角度X射线散射与微流控和有限元方法模拟相结合。我们的方法适用于解决早期组装步骤,该步骤发生在亚秒级到秒级范围内。特别是,我们揭示了离子种类和浓度对组装的影响。通过调整流速和浓度曲线,我们找到了启动组装所需的最低临界盐浓度。此外,我们在X射线数据中对表面敏感的Porod态的分析表明,第一组装中间体(所谓的单位长度长丝)的形成不是一步反应,而是由不同的连续横向缔合步骤以及随后的径向压实以及使全幅长丝表面光滑。

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