首页> 美国卫生研究院文献>Biochemical Journal >Sound attenuation of polymerizing actin reflects supramolecular structures: viscoelastic properties of actin gels modified by cytochalasin D profilin and alpha-actinin.
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Sound attenuation of polymerizing actin reflects supramolecular structures: viscoelastic properties of actin gels modified by cytochalasin D profilin and alpha-actinin.

机译:聚合肌动蛋白的声音衰减反映了超分子结构:被细胞松弛素D前体蛋白和α-肌动蛋白修饰的肌动蛋白凝胶的粘弹性质。

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摘要

Polymerization and depolymerization of cytoskeletal elements maintaining cytoplasmic stiffness are key factors in the control of cell crawling. Rheometry is a significant tool in determining the mechanical properties of the single elements in vitro. Viscoelasticity of gels formed by these polymers strongly depends on both the length and the associations of the filaments (e.g. entanglements, annealings and side-by-side associations). Ultrasound attenuation is related to viscosity, sound velocity and supramolecular structures in the sample. In combination with a small glass fibre (2 mm x 50 microm), serving as a viscosity sensor, an acoustic microscope was used to measure the elasticity and acoustic attenuation of actin solutions. Changes in acoustic attenuation of polymerizing actin by far exceed the values expected from calculations based on changes in viscosity and sound velocity. During the lag-phase of actin polymerization, attenuation slightly decreases, depending on actin concentration. After the half-maximum viscosity is accomplished and elasticity turns into steady state, attenuation distinctly rises. Changes in ultrasound attenuation depend on actin concentration, and they are modulated by the addition of alpha-actinin, cytochalasin D and profilin. Thus absorption and scattering of sound on the polymerization of actin is related to the packing density of the actin net, entanglements and the length of the actin filaments. Shortening of actin filaments by cytochalasin D was also confirmed by electron micrographs and falling-ball viscosimetry. In addition to viscosity and elasticity, the attenuation of sound proved to be a valuable parameter in characterizing actin polymerization and the supramolecular associations of F-actin.
机译:维持细胞质刚度的细胞骨架元素的聚合和解聚是控制细胞爬行的关键因素。流变仪是确定体外单个元素机械性能的重要工具。由这些聚合物形成的凝胶的粘弹性在很大程度上取决于长丝的长度和缔合(例如缠结,退火和并列缔合)。超声衰减与样品中的粘度,声速和超分子结构有关。与用作粘度传感器的细小的玻璃纤维(2毫米x 50微米)结合,使用声学显微镜测量肌动蛋白溶液的弹性和声衰减。聚合肌动蛋白的声衰减变化远远超过了基于粘度和声速变化的计算所期望的值。在肌动蛋白聚合的滞后阶段,衰减根据肌动蛋白浓度而略微降低。在达到最大粘度的一半并且弹性变成稳态之后,衰减明显增加。超声衰减的变化取决于肌动蛋白的浓度,并且通过添加α-肌动蛋白,细胞松弛素D和脯氨酸蛋白来调节。因此,肌动蛋白聚合过程中声音的吸收和散射与肌动蛋白网的堆积密度,缠结和肌动蛋白丝的长度有关。电子显微镜和落球粘度测定法也证实了细胞松弛素D导致肌动蛋白丝的缩短。除粘度和弹性外,声音的衰减被证明是表征肌动蛋白聚合和F-肌动蛋白超分子缔合的重要参数。

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