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Local Mechanical Perturbation Provides an Effective Means to Regulate the Growth and Assembly of Functional Peptide Fibrils

机译:局部机械扰动提供了一种有效的手段来调节功能性肽原纤维的生长和组装。

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摘要

Mucin 1 (MUC1) peptide fused with Q11 (MUC1-Q11) having 35 residues has previously been shown to form amyloid fibrils. Using time-dependent and highresolution atomic force microscopy (AFM) imaging, it is revealed that the formation of individual MUC1-Q11 fibrils entails nucleation and extension at both ends. This process can be altered by local mechanical perturbations using AFM probes. This work reports two specific perturbations and outcomes. First, by increasing load while maintaining tip-surface contact, the fibrils are cut during the scan due to shearing. Growth of fibrils occurs at the newly exposed termini, following similar mechanism of the MUC1-Q11 nucleation growth. As a result, branched fibrils are seen on the surface whose orientation and length can be controlled by the nuclei orientation and reaction time. In contrast to the "one-time-cut", fibrils can be continuously fragmented by modulation at sufficiently high amplitude. As a result, short and highly branched fibrils accumulate and pile on surfaces. Since the fibril formation and assembly of MUC1-Q11 can be impacted by local mechanical force, this approach offers a nonchemical and label-free means to control the presentation of MUC1 epitopes, and has promising application in MUC1 fibril-based immunotherapy.
机译:先前已显示与具有35个残基的Q11(MUC1-Q11)融合的Mucin 1(MUC1)肽可形成淀粉样蛋白原纤维。使用时间依赖性和高分辨率原子力显微镜(AFM)成像,揭示了单个MUC1-Q11原纤维的形成需要两端都有成核和延伸。可以通过使用AFM探针进行局部机械扰动来更改此过程。这项工作报告了两个具体的扰动和结果。首先,通过在保持尖端与表面接触的同时增加负载,在扫描过程中由于剪切作用而将原纤维切断。遵循MUC1-Q11成核生长的类似机理,在新暴露的末端出现原纤维的生长。结果,在表面上看到分支的原纤维,其方向和长度可以通过核的方向和反应时间来控制。与“一次性切割”相反,原纤维可以通过以足够高的幅度进行调制而连续地破碎。结果,短而高度分支的原纤维堆积并堆积在表面上。由于MUC1-Q11的原纤维形成和组装会受到局部机械力的影响,因此该方法提供了一种非化学和无标记的方法来控制MUC1表位的呈递,并且在基于MUC1的原纤维免疫治疗中具有广阔的应用前景。

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