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β-淀粉样蛋白原纤维伸长的动力学分析

Kinetic analysis of beta-amyloid fibril elongation.

作者信息

Cannon Michelle J, Williams Angela D, Wetzel Ronald, Myszka David G

机构信息

Center for Biomolecular Interaction Analysis, University of Utah, Salt Lake City, UT 84132, USA.

出版信息

Anal Biochem. 2004 May 1;328(1):67-75. doi: 10.1016/j.ab.2004.01.014.

Abstract

We used surface plasmon resonance biosensors to evaluate the kinetics associated with the initial events of beta-amyloid (Abeta) fibril elongation. Fibrils were immobilized on the sensor chip surface and extended by exposure to soluble Abeta(1-40) peptide. The fibril surfaces bound Congo red, a marker for beta sheet structures, and exhibited a slow linear background decay that is consistent with fibril depolymerization. Sonicated fibrils supported elongation better than unsonicated fibrils, which is consistent with fibril extension reactions. The kinetic data revealed that peptide association and dissociation occurred in multiple steps. Kinetic rate constants for fibril extension were determined by globally fitting the response data with a three-step polymerization model. In the first step, the soluble peptide binds to the growing fibril tip in a readily reversible reaction. The subsequent steps likely allow bound peptide to be stabilized into the growing fiber through postbinding transitional events. Using a mutant peptide, F19P Abeta(1-40), we illustrate how the biosensor assay can be used to probe structure/function relationships of fibril elongation.

摘要

我们使用表面等离子体共振生物传感器来评估与β-淀粉样蛋白(Aβ)原纤维伸长初始事件相关的动力学。将原纤维固定在传感器芯片表面,并通过暴露于可溶性Aβ(1-40)肽来使其延伸。原纤维表面结合了刚果红,这是β折叠结构的一种标记物,并且呈现出与原纤维解聚一致的缓慢线性背景衰减。超声处理的原纤维比未超声处理的原纤维更有利于伸长,这与原纤维延伸反应一致。动力学数据表明,肽的结合和解离发生在多个步骤中。通过用三步聚合模型对响应数据进行全局拟合来确定原纤维延伸的动力学速率常数。在第一步中,可溶性肽以易于可逆的反应结合到生长的原纤维末端。随后的步骤可能通过结合后过渡事件使结合的肽稳定到生长的纤维中。使用突变肽F19P Aβ(1-40),我们说明了生物传感器测定法可如何用于探究原纤维伸长的结构/功能关系。

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