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Spectrin Folding versus Unfolding Reactions and RBC Membrane Stiffness

机译:血影蛋白折叠与展开反应和RBC膜的刚度

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摘要

Spectrin (Sp), a key component of the erythrocyte membrane, is routinely stretched to near its fully folded contour length during cell deformations. Such dynamic loading may induce domain unfolding as suggested by recent experiments. Herein we develop a model to describe the folding/unfolding of spectrin during equilibrium or nonequilibrium extensions. In both cases, our model indicates that there exists a critical extension beyond which unfolding occurs. We further deploy this model, together with a three-dimensional model of the junctional complex in the erythrocyte membrane, to explore the effect of Sp unfolding on the membrane's mechanical properties, and on the thermal fluctuation of membrane-attached beads. At large deformations our results show a distinctive strain-induced unstiffening behavior, manifested in the slow decrease of the shear modulus, and accompanied by an increase in bead fluctuation. Bead fluctuation is also found to be influenced by mode switching, a phenomenon predicted by our three-dimensional model. The amount of stiffness reduction, however, is modest compared with that reported in experiments. A possible explanation for the discrepancy is the occurrence of spectrin head-to-head disassociation which is also included within our modeling framework and used to analyze bead motion as observed via experiment.
机译:血影蛋白(Sp)是红细胞膜的关键组成部分,在细胞变形过程中通常会拉伸到接近其完全折叠的轮廓长度。如最近的实验所建议的,这种动态加载可能诱导域展开。在本文中,我们开发了一个模型来描述平衡或非平衡延伸过程中血影蛋白的折叠/展开。在这两种情况下,我们的模型都表明存在一个关键扩展,超出该扩展就会发生。我们进一步部署此模型,以及红细胞膜中的连接复合物的三维模型,以探索Sp展开对膜的机械性能以及膜附着珠的热波动的影响。在大变形下,我们的结果显示出独特的应变诱导的非刚度行为,表现为剪切模量的缓慢降低,并伴随着胎圈波动的增加。还发现磁珠波动受模式转换的影响,模式转换是我们的三维模型预测的现象。但是,与实验报告的相比,刚度降低的程度是适度的。差异的可能解释是发生了血影蛋白头对头分离,这也包含在我们的建模框架中,并用于分析通过实验观察到的珠子运动。

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