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轴向和径向杨氏模量测量揭示了鼠朊病毒纳米原纤维的高固有机械柔韧性。

High intrinsic mechanical flexibility of mouse prion nanofibrils revealed by measurements of axial and radial Young's moduli.

机构信息

Centre for High-Throughput Biology, University of British Colombia , Vancouver, BC, Canada V6T 1Z4.

出版信息

ACS Nano. 2014 Apr 22;8(4):3851-61. doi: 10.1021/nn5007013. Epub 2014 Mar 6.

Abstract

Self-templated protein aggregation and intracerebral deposition of aggregates, sometimes in the form of amyloid fibrils, is a hallmark of mammalian prion diseases. What distinguishes amyloid fibrils formed by prions from those formed by other proteins is not clear. On the basis of previous studies on yeast prions that correlated high intrinsic fragmentation rates of fibrils with prion propagation efficiency, it has been hypothesized that the nanomechanical properties of prion amyloid such as strength and elastic modulus may be the distinguishing feature. Here, we reveal that fibrils formed by mammalian prions are relatively soft and clearly in a different class of rigidities when compared to nanofibrils formed by nonprions. We found that amyloid fibrils made of both wild-type and mutant mouse recombinant PrP(23-231) have remarkably low axial elastic moduli of 0.1-1.4 GPa. We demonstrate that even the proteinase K resistant core of these fibrils has similarly low intrinsic rigidities. Using a new mode of atomic force microscopy called AM-FM mode, we estimated the radial modulus of PrP fibrils at ∼0.6 GPa, consistent with the axial moduli derived by using an ensemble method. Our results have far-reaching implications for the understanding of protein-based infectivity and the design of amyloid biomaterials.

摘要

自模板化蛋白聚集和聚集物的脑内沉积,有时呈淀粉样纤维的形式,是哺乳动物朊病毒病的标志。导致由朊病毒形成的淀粉样纤维不同于由其他蛋白质形成的纤维的原因尚不清楚。基于先前关于酵母朊病毒的研究,该研究将纤维的固有高断裂率与朊病毒传播效率相关联,人们假设朊病毒淀粉样的纳米力学特性,如强度和弹性模量,可能是朊病毒的特征。在这里,我们揭示了与非朊病毒形成的纳米纤维相比,哺乳动物朊病毒形成的纤维相对较软,并且在刚度上明显属于不同类别。我们发现,由野生型和突变型小鼠重组 PrP(23-231)形成的纤维具有非常低的轴向弹性模量(0.1-1.4 GPa)。我们证明,即使是这些纤维的蛋白酶 K 抗性核心也具有类似的低固有刚度。使用一种称为 AM-FM 模式的新型原子力显微镜,我们估计 PrP 纤维的径向模量约为 0.6 GPa,与使用集合方法得出的轴向模量一致。我们的结果对理解基于蛋白质的感染性和设计淀粉样生物材料具有深远的意义。

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