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Elucidating Axonal Injuries Through Molecular Modelling of Myelin Sheaths and Nodes of Ranvier

机译:通过Myelin护套和Ranvier节点的分子建模阐明轴心损伤

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Around half of the traumatic brain injuries are thought to be axonal damage. Disruption of the cellular membranes, or alternatively cytoskeletal damage has been suggested as possible injury trigger. Here, we have used molecular models to have a better insight on the structural and mechanical properties of axon sub-cellular components. We modelled myelin sheath and node of Ranvier as lipid bilayers at a coarse grained level. We built ex-novo a model for the myelin. Lipid composition and lipid saturation were based on the available experimental data. The model contains 17 different types of lipids, distributed asymmetrically between two leaflets. Molecular dynamics simulations were performed to characterize the myelin and node-of-Ranvier bilayers at equilibrium and under deformation and compared to previous axolemma simulations. We found that the myelin bilayer has a slightly higher area compressibility modulus and higher rupture strain than node of Ranvier. Compared to the axolemma, mechanoporation occurs at 50 % higher strain in the myelin and at 23 % lower strain in the node of Ranvier. Combining the results with finite element simulations of the axon, we hypothesizes that myelin does not rupture at the thresholds proposed in the literature for axonal injury while rupture may occur at the node of Ranvier. The findings contribute to increases our knowledge of axonal sub-cellular components and help to understand better the mechanism behind axonal brain injury.
机译:大约一半的创伤性脑损伤被认为是轴突造成的。在可能的伤害触发中,已经提出了细胞膜的破坏,或者是细胞骨骼损伤。在这里,我们已经使用了分子模型对轴突亚细胞部件的结构和力学性能更好地了解。我们以粗粒水平为脂质双层的素米氏鞘和节点。我们为髓鞘建造了Ex-Novo一个模型。脂质组合物和脂质饱和度基于可用的实验数据。该模型含有17种不同类型的脂质,在两只小叶之间不对称地分布。进行分子动力学模拟,以表征骨髓素和ranvier双层在平衡和变形下进行,并与先前的Axolemma模拟相比。我们发现髓鞘双层具有略高的区域可压缩模量和比Ranvier的节点更高的破裂应变。与Axolemma相比,机械钻发生在髓鞘中的50%较高的50%,在Ranvier节点中较低的菌株23%。将结果与轴突的有限元模拟相结合,我们假设髓鞘在文献中提出的阈值下破裂,而在Ranvier的节点处可能发生破裂。调查结果有助于提高我们对轴突亚细胞成分的知识,并有助于了解轴突脑损伤背后的机制。

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