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High-Speed Nanomechanical Mapping of the Early Stages of Collagen Growth by Bimodal Force Microscopy

机译:双峰力显微镜的高速纳米力学映射胶原蛋白生长的早期阶段

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摘要

High-speed atomic force microscopy (AFM) enabled the imaging of protein interactions with millisecond time resolutions (10 fps). However, the acquisition of nanomechanical maps of proteins is about 100 times slower. Here, we developed a high-speed bimodal AFM that provided high-spatial resolution maps of the elastic modulus, the loss tangent, and the topography at imaging rates of 5 fps. The microscope was applied to identify the initial stages of the self-assembly of the collagen structures. By following the changes in the physical properties, we identified four stages, nucleation and growth of collagen precursors, formation of tropocollagen molecules, assembly of tropocollagens into microfibrils, and alignment of microfibrils to generate microribbons. Some emerging collagen structures never matured, and after an existence of several seconds, they disappeared into the solution. The elastic modulus of a microfibril (similar to 4 MPa) implied very small stiffness (similar to 3 X 10(-6) N/m). Those values amplified the amplitude of the collagen thermal fluctuations on the mica plane, which facilitated microribbon build-up.
机译:高速原子力显微镜(AFM)使蛋白质相互作用的成像具有毫秒级的时间分辨率(10 fps)。然而,蛋白质纳米力学图谱的获取速度要慢100倍左右。在这里,我们开发了一种高速双峰AFM,它以5 fps的成像速率提供了弹性模量、损耗正切和地形的高空间分辨率地图。显微镜用于识别胶原结构自组装的初始阶段。通过跟踪物理性质的变化,我们确定了四个阶段:胶原前体的成核和生长、原胶原分子的形成、原胶原组装成微纤维以及微纤维的排列以生成微带。一些新出现的胶原结构从未成熟,在存在几秒钟后,它们消失在溶液中。微纤维的弹性模量(类似于4MPa)意味着非常小的刚度(类似于3x10(-6)N/m)。这些值放大了云母平面上胶原热波动的幅度,从而促进了微带的形成。

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