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Kinetic Ductility and Force-Spike Resistance of Proteins from Single-Molecule Force Spectroscopy

机译:单分子力光谱法的动力延性与蛋白质的力 - 尖峰抗性

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摘要

Ductile materials can absorb spikes in mechanical force, whereas brittle ones fail catastrophically. Here we develop a theory to quantify the kinetic ductility of single molecules from force spectroscopy experiments, relating force-spike resistance to the differential responses of the intact protein and the unfolding transition state to an applied mechanical force. We introduce a class of unistable one-dimensional potential surfaces that encompass previous models as special cases and continuously cover the entire range from ductile to brittle. Compact analytic expressions for force-dependent rates and rupture-force distributions allow us to analyze force-clamp and force-ramp pulling experiments. We find that the force-transmitting protein domains of filamin and titin are kinetically ductile when pulled from their two termini, making them resistant to force spikes. For the mechanostable muscle protein titin, a highly ductile model reconciles data over 10 orders of magnitude in force loading rate from experiment and simulation.
机译:韧性材料可以吸收机械力的尖峰,而脆性则脆弱地失败。在这里,我们开发了一种理论,以量化来自力光谱实验的单个分子的动力学延展性,将力尖峰抗性与完整蛋白质的差分反应相关,并将展开过渡状态与施加的机械力相比。我们介绍一类不可统一的一维潜在表面,包括以前的型号作为特殊情况,并连续覆盖从韧性到脆性的整个范围。紧凑的用于力依赖性速率和破裂力分布的分析表达式允许我们分析力夹和力 - 斜坡的拉动实验。我们发现菲霉素和三肽的力传递蛋白质结构域在从两条末端拉出时是动力学,使它们能够抵抗力尖峰。对于睾丸杆菌肌蛋白三汀,高度延展性模型在实验和仿真中以力加载速率的10个级别和大幅度的数据调和。

著录项

  • 来源
    《Biophysical Journal》 |2016年第4期|共9页
  • 作者单位

    Max Planck Inst Biophys Dept Theoret Biophys Frankfurt Germany;

    Max Planck Inst Biophys Dept Theoret Biophys Frankfurt Germany;

    Natl Inst Diabet &

    Digest &

    Kidney Dis Lab Chem Phys NIH Bethesda MD USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物物理学;
  • 关键词

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