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#alpha#-Helix Structure in Alzheimer's disease Aggregates of Tau-Protein

机译:#α-哈尔克斯结构在阿尔茨海默氏症的Tau-蛋白疾病骨料中

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摘要

The discovery of #beta#-sheet structure in Alzheimer's amyloid fibrils, and then in many other disease-related protein fibrils, has led to the widely believed view that #beta#-sheet formation is the general mechanism of aberrant protein aggregation leading to disease. This notion is further reinforced by recent findings, which indicate that normal proteins can be induced to form #beta#-sheet fibrils in vitro. Alzheimer's disease, a paradigm proteopathy, is accompanied by the formation of two distinct aggregates, amyloid fibrils and paired helical filaments (PHFs). Electron microscope images of PHFs show pairs of twisted ribbons with 80 nm periodicity. However, there is little information of the molecular structure of PHFs, as previous studies have failed to identify signs of regular structure. Using far-UV circular dichroism and Fourier-transformed infrared spectroscopy, we find that PHFs are comprised of #alpha#-helices. This is remarkable as tau-protein, PHF's primary constituent, has a high abundance of helix-breaking amino acids and is unstructured in solution. We also find that PHFs are very stable, as judged by their high melting temperature and resistance to protease digestion. PHFs are the first example of pathological aggregation associated to the formation of #alpha#-helix.
机译:在阿尔茨海默氏蛋白原纤维中发现了#beta#-sheet结构,然后在许多其他与疾病相关的蛋白原纤维中导致了广泛认为的观点,即#β#-sheet形成是导致疾病的异常蛋白质聚集的一般机制。最近发现进一步加强了这种观念,表明可以诱导正常蛋白质在体外形成#β-曲面纤维。 Alzheimer的疾病是一种范式蛋白质,伴随着形成两个不同的聚集体,淀粉样蛋白原纤维和配对螺旋丝(PHF)。 PHFS的电子显微镜图像显示扭曲带有80nm周期性的扭曲带。然而,随着以前的研究未能识别常规结构的迹象,PHF的分子结构几乎没有信息。使用FAR-UV圆形二色性和傅里叶变换的红外光谱,我们发现PHFS由#alpha#-helices组成。这是由于Tau-蛋白的PHF的主要成分,具有高丰度的螺旋破碎的氨基酸,并且在溶液中非结构化。我们还发现PHFS非常稳定,通过其高熔点和抗蛋白酶消化来判断。 PHF是与形成#alpha #helix的病理聚集的第一个例子。

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  • 来源
    《Biochemistry 》 |2002年第22期| 共6页
  • 作者单位

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

    Department of Chemistry and Biochemistry and Center for biomolecular Structure and Organization Univerity of Maryland College Park Maryland 20742 Centro de Biologia Molecular Severo Ochoa Universidad Autonoma de Madrid 28049 Madrid Spain and;

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  • 正文语种 eng
  • 中图分类 生物化学 ;
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