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高分辨率光谱学揭示了胰岛素的纤维化抑制途径。

High resolution spectroscopy reveals fibrillation inhibition pathways of insulin.

机构信息

Leibniz Institute of Photonic Technology (IPHT), Albert-Einsteinstr. 9, D-07745 Jena, Germany.

Institute of Physical Chemistry, Friedrich-Schiller-University Jena and Abbe Center of Photonics, Helmholtzweg 4, D-07743 Jena, Germany.

出版信息

Sci Rep. 2016 Dec 23;6:39622. doi: 10.1038/srep39622.

Abstract

Fibril formation implies the conversion of a protein's native secondary structure and is associated with several neurodegenerative diseases. A better understanding of fibrillation inhibition and fibril dissection requires nanoscale molecular characterization of amyloid structures involved. Tip-enhanced Raman scattering (TERS) has already been used to chemically analyze amyloid fibrils on a sub-protein unit basis. Here, TERS in combination with atomic force microscopy (AFM), and conventional Raman spectroscopy characterizes insulin assemblies generated during inhibition and dissection experiments in the presence of benzonitrile, dimethylsulfoxide, quercetin, and β-carotene. The AFM topography indicates formation of filamentous or bead-like insulin self-assemblies. Information on the secondary structure of bulk samples and of single aggregates is obtained from standard Raman and TERS measurements. In particular the high spatial resolution of TERS reveals the surface conformations associated with the specific agents. The insulin aggregates formed under different inhibition and dissection conditions can show a similar morphology but differ in their β-sheet structure content. This suggests different aggregation pathways where the prevention of the β-sheet stacking of the peptide chains plays a major role. The presented approach is not limited to amyloid-related reasearch but can be readily applied to systems requiring extremely surface-sensitive characterization without the need of labels.

摘要

纤维形成意味着蛋白质天然二级结构的转化,并与几种神经退行性疾病有关。更好地理解纤维抑制和纤维分解需要对涉及的淀粉样结构进行纳米级分子特征描述。尖端增强拉曼散射(TERS)已经用于在亚蛋白单元基础上对淀粉样纤维进行化学分析。在这里,TERS 结合原子力显微镜(AFM)和常规拉曼光谱,对苯腈、二甲基亚砜、槲皮素和β-胡萝卜素存在下抑制和分解实验中产生的胰岛素组装体进行了表征。AFM 形貌表明形成了丝状或珠状胰岛素自组装体。来自标准拉曼和 TERS 测量的关于批量样品和单个聚集体的二级结构的信息。特别是,TERS 的高空间分辨率揭示了与特定试剂相关的表面构象。在不同的抑制和分解条件下形成的胰岛素聚集体可以具有相似的形态,但β-折叠结构含量不同。这表明存在不同的聚集途径,其中肽链的β-折叠堆积的阻止起着主要作用。所提出的方法不仅限于与淀粉样蛋白相关的研究,而且可以很容易地应用于需要极其表面敏感表征而无需标记的系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6924/5180225/76ffa7df961c/srep39622-f1.jpg

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