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Mechanics of proteins with a focus on atomic force microscopy

机译:蛋白质力学着重于原子力显微镜

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摘要

The capacity of proteins to function relies on a balance between molecular stability to maintain their folded state and structural flexibility allowing conformational changes related to biological function. Among many others, four different examples can be chosen. The giant protein titin is stretched and can unfold during muscle contraction providing passive elasticity to muscle tissue; myoglobin adsorbs and releases oxygen molecules thank to conformational changes in its structure; the outer membrane protein G (OmpG) is a bacterial porin with a long and flexible loop that modulates gating; and the proton pump bacteriorhodopsin adapts its cytosolic half to allow proton pumping. All these conformational changes triggered either by chemical or by physical cues, require mechanical flexibility or elasticity of certain protein domains. While the methods to determine protein structure, X-ray crystallography above all, have been dramatically improved over the last decades, the number of tools that directly measure the mechanical flexibility of proteins and protein domains is still limited. In this tutorial, after a brief introduction to protein structure, we present some of the available techniques to estimate protein flexibility, then focusing on atomic force microscopy (AFM). We describe the principles of the technique and its various imaging and force spectroscopy modes of operation that allow probing the elasticity of proteins, protein domains and their surrounding environment.
机译:蛋白质功能的能力取决于维持其折叠状态的分子稳定性与允许与生物学功能有关的构象变化的结构柔性之间的平衡。在许多其他示例中,可以选择四个不同的示例。巨大的蛋白纤溶蛋白被拉伸,在肌肉收缩过程中可以展开,从而为肌肉组织提供被动弹性。肌红蛋白的结构发生构象变化,从而吸附和释放氧分子;外膜蛋白G(OmpG)是一种细菌蛋白,具有长而灵活的环,可调节门控;质子泵细菌视紫红质会调整其胞质的一半以允许质子泵送。由化学或物理线索触发的所有这些构象变化都需要某些蛋白质结构域的机械柔韧性或弹性。尽管在过去的几十年中,用于确定蛋白质结构的方法(尤其是X射线晶体学)已得到显着改善,但是直接测量蛋白质和蛋白质域的机械柔韧性的工具数量仍然有限。在本教程中,在简要介绍了蛋白质结构之后,我们介绍了一些可用的技术来估计蛋白质的柔韧性,然后重点介绍原子力显微镜(AFM)。我们描述了该技术的原理及其各种成像和力谱操作模式,这些模式允许探测蛋白质,蛋白质结构域及其周围环境的弹性。

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