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Complexity of the Tensegrity Structure for Dynamic Energy and Force Distribution of Cytoskeleton during Cell Spreading

机译:细胞扩散过程中细胞骨架动态能量和力分布的张力结构的复杂性

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摘要

Cytoskeleton plays important roles in intracellular force equilibrium and extracellular force transmission from/to attaching substrate through focal adhesions (FAs). Numerical simulations of intracellular force distribution to describe dynamic cell behaviors are still limited. The tensegrity structure comprises tension-supporting cables and compression-supporting struts that represent the actin filament and microtubule respectively, and has many features consistent with living cells. To simulate the dynamics of intracellular force distribution and total stored energy during cell spreading, the present study employed different complexities of the tensegrity structures by using octahedron tensegrity (OT) and cuboctahedron tensegrity (COT). The spreading was simulated by assigning specific connection nodes for radial displacement and attachment to substrate to form FAs. The traction force on each FA was estimated by summarizing the force carried in sounding cytoskeletal elements. The OT structure consisted of 24 cables and 6 struts and had limitations soon after the beginning of spreading by declining energy stored in struts indicating the abolishment of compression in microtubules. The COT structure, double the amount of cables and struts than the OT structure, provided sufficient spreading area and expressed similar features with documented cell behaviors. The traction force pointed inward on peripheral FAs in the spread out COT structure. The complex structure in COT provided further investigation of various FA number during different spreading stages. Before the middle phase of spreading (half of maximum spreading area), cell attachment with 8 FAs obtained minimized cytoskeletal energy. The maximum number of 12 FAs in the COT structure was required to achieve further spreading. The stored energy in actin filaments increased as cells spread out, while the energy stored in microtubules increased at initial spreading, peaked in middle phase, and then declined as cells reached maximum spreading. The dynamic flows of energy in struts imply that microtubules contribute to structure stabilization.
机译:细胞骨架在细胞内力平衡和细胞外力通过粘着粘附(FA)从/向附着基质的传递中起重要作用。细胞内力分布来描述动态细胞行为的数值模拟仍然是有限的。张力结构包括分别代表肌动蛋白丝和微管的张力支撑电缆和压缩支撑支柱,并具有许多与活细胞一致的特征。为了模拟细胞扩散过程中细胞内力分布和总存储能量的动力学,本研究通过使用八面体张力(OT)和立方八面体张力(COT)采用了不同的张力结构复杂性。通过为径向位移分配特定的连接节点并附着到基板以形成FA来模拟扩展。通过汇总听起来健全的细胞骨架成分所承受的力来估算每个FA上的牵引力。 OT结构由24根电缆和6个支杆组成,并且在扩展开始后不久就受到限制,其原因是存储在支杆中的能量下降,表明微管中的压缩消失。与OT结构相比,COT结构使电缆和支柱的数量增加了一倍,提供了足够的扩展区域,并表现出类似的特征,并记录了细胞行为。牵引力向内指向散布的COT结构中的外围FA。 COT中复杂的结构为进一步研究不同铺展阶段的FA数提供了条件。在扩展的中间阶段(最大扩展区域的一半)之前,具有8个FA的细胞附着获得了最小的细胞骨架能量。为了实现进一步扩展,COT结构中最多需要12个FA。肌动蛋白丝中储存的能量随着细胞的扩散而增加,而微管中储存的能量在初始扩散时增加,在中间阶段达到峰值,然后随着细胞达到最大扩散而下降。支撑杆中的动态能量流动表明微管有助于结构稳定。

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