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首页> 外文期刊>Nano letters >Optimizing 1-mu s-Resolution Single-Molecule Force Spectroscopy on a Commercial Atomic Force Microscope
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Optimizing 1-mu s-Resolution Single-Molecule Force Spectroscopy on a Commercial Atomic Force Microscope

机译:在商用原子力显微镜上优化1-μs分辨率单分子力谱

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摘要

Atomic force microscopy (AFM)-based single-molecule force spectroscopy (SMFS) is widely used to mechanically measure the folding and unfolding of proteins. However, the temporal resolution of a standard commercial cantilever is 50-1000 mu s, masking rapid transitions and short-lived intermediates. Recently, SMFS with 0.7-mu s temporal resolution was achieved using an ultrashort (L = 9 mu m) cantilever on a custom-built, high-speed AFM. By micro-machining such cantilevers with a focused ion beam, we optimized them for SMFS rather than tapping-mode imaging. To enhance usability and throughput, we detected the modified cantilevers on a commercial AFM retrofitted with a detection laser system featuring a 3-mu m circular spot size. Moreover, individual cantilevers were reused over multiple days. The improved capabilities of the modified cantilevers for SMFS were showcased by unfolding a polyprotein, a popular biophysical assay. Specifically, these cantilevers maintained a 1-mu s response time while eliminating cantilever ringing (Q congruent to 0.5). We therefore expect such cantilevers, along with the instrumentational improvements to detect them on a commercial AFM, to accelerate high-precision AFM-based SMFS studies.
机译:基于原子力显微镜(AFM)的单分子力谱(SMFS)被广泛用于机械地测量蛋白质的折叠和展开。但是,标准商品悬臂的时间分辨率为50-1000μs,掩盖了快速过渡和短命的中间体。最近,在定制的高速AFM上使用超短(L = 9μm)悬臂实现了时间分辨率为0.7μs的SMFS。通过用聚焦离子束微加工此类悬臂,我们针对SMFS(而不是敲击模式成像)对其进行了优化。为了提高可用性和吞吐量,我们在商业AFM上检测到了改进的悬臂,该AFM装有3微米圆形斑点尺寸的检测激光系统。此外,单个悬臂被重复使用了几天。修饰的悬臂对SMFS的改进功能通过展开多蛋白(一种流行的生物物理测定法)来展示。具体而言,这些悬臂保持了1-μs的响应时间,同时消除了悬臂振铃(Q等于0.5)。因此,我们希望这些悬臂以及仪器的改进能够在商用AFM上进行检测,从而加速基于AFM的高精度SMFS研究。

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