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Helical structure of actin stress fibers and its possible contribution to inducing their direction-selective disassembly upon cell shortening

机译:肌动蛋白应激纤维的螺旋结构及其对细胞缩短时诱导其方向选择性拆卸的可能贡献

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Mechanisms of the assembly of actin stress fibers (SFs) have been extensively studied, while those of the disassembly-particularly cell shortening-induced ones-remain unclear. Here, we show that SFs have helical structures composed of multi-subbundles, and they tend to be delaminated upon cell shortening. Specifically, we observed with atomic force microscopy delamination of helical SFs into their subbundles. We physically caught individual SFs using a pair of glass needles to observe rotational deformations during stretching as well as ATP-driven active contraction, suggesting that they deform in a manner reflecting their intrinsic helical structure. A minimal analytical model was then developed based on the Frenet-Serret formulas with force-strain measurement data to suggest that helical SFs can be delaminated into the constituent subbundles upon axial shortening. Given that SFs are large molecular clusters that bear cellular tension but must promptly disassemble upon loss of the tension, the resulting increase in their surface area due to the shortening-induced delamination may facilitate interaction with surrounding molecules to aid subsequent disintegration. Thus, our results suggest a new mechanism of the disassembly that occurs only in the specific SFs exposed to forced shortening.
机译:已经广泛地研究了肌动蛋白应激纤维组件(SFS)的机制,而拆卸 - 特别是细胞缩短诱导的那些仍然不清楚。在这里,我们表明SFS具有由多亚括号组成的螺旋结构,并且它们倾向于在细胞缩短时被分解。具体而言,我们观察到螺旋SFS的原子力显微镜分层分解成其亚骨。我们使用一对玻璃针物理地捕获单个SFS,以观察拉伸期间的旋转变形以及ATP驱动的活性收缩,表明它们以反射其固有螺旋结构的方式变形。然后基于具有力 - 应变测量数据的FRENET-SERRET公式开发了最小的分析模型,表明螺旋SF可以在轴向缩短时被分解成组成亚级。鉴于SFS是具有携带细胞张力的大分子簇,但必须在损失张力时立即拆卸,因此由于缩短诱导的分层而导致的表面积增加可以促进与周围分子的相互作用以帮助随后的崩解。因此,我们的结果表明,仅在暴露于强制缩短的特定SFS中发生的拆卸的新机制。

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