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固液界面多层胰高血糖素纤维化的石英晶体微天平研究

Quartz crystal microbalance studies of multilayer glucagon fibrillation at the solid-liquid interface.

作者信息

Hovgaard Mads Bruun, Dong Mingdong, Otzen Daniel Erik, Besenbacher Flemming

机构信息

Interdisciplinary Nanoscience Center and Department of Physics and Astronomy, University of Aarhus, DK-8000 Aarhus C, Denmark.

出版信息

Biophys J. 2007 Sep 15;93(6):2162-9. doi: 10.1529/biophysj.107.109686. Epub 2007 May 18.

DOI:10.1529/biophysj.107.109686
PMID:17513349
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1959527/
Abstract

We have used a quartz crystal microbalance with dissipation (QCM-D) to monitor the changes in layer thickness and viscoelastic properties accompanying multilayer amyloid deposition in situ for the first time. By means of atomic force microscope imaging, an unequivocal correlation is established between the interfacial nucleation and growth of glucagon fibrils and the QCM-D response. The combination of the two techniques allows us to study the temporal evolution of the interfacial fibrillation process. We have modeled the QCM-D data using an extension to the Kelvin-Voigt viscoelastic model. Three phases were observed in the fibrillation process: 1), a rigid multilayer of glucagon monomers forms and slowly rearranges; 2), this multilayer subsequently evolves into a dramatically more viscoelastic layer, containing a polymorphic network of micrometer-long fibrils growing from multiple nucleation sites; and 3), the fibrillar formation effectively stops as a result of the depletion of bulk-phase monomers, although the process can be continued without a lag phase by subsequent addition of fresh monomers. The robustness of the QCM-D technique, consolidated by complementary atomic force microscope studies, should make it possible to combine different components thought to be involved in the plaque formation process and thus build up realistic models of amyloid plaque formation in vitro.

摘要

我们首次使用带耗散监测的石英晶体微天平(QCM-D)原位监测多层淀粉样蛋白沉积过程中层厚度和粘弹性特性的变化。通过原子力显微镜成像,明确建立了胰高血糖素原纤维的界面成核和生长与QCM-D响应之间的相关性。这两种技术的结合使我们能够研究界面纤维化过程的时间演变。我们使用对开尔文-沃伊特粘弹性模型的扩展对QCM-D数据进行了建模。在纤维化过程中观察到三个阶段:1),形成胰高血糖素单体的刚性多层并缓慢重排;2),该多层随后演变成粘弹性显著更高的层,包含从多个成核位点生长的微米级长纤维的多晶网络;3),由于体相单体耗尽,纤维形成有效地停止,尽管通过随后添加新鲜单体可以无滞后阶段地继续该过程。通过互补的原子力显微镜研究巩固的QCM-D技术的稳健性,应该能够组合被认为参与斑块形成过程的不同成分,从而在体外建立淀粉样斑块形成的真实模型。

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本文引用的文献

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