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Structural evaluations of tau protein conformation: methodologies and approaches

机译:TAU蛋白质构象的结构评估:方法和方法

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Protein-misfolding diseases are based on a common principle of aggregation initiated by intra- and inter-molecular contacts. The structural and conformational changes induced by biochemical transformations such as post-translational modifications (PTMs), often lead to protein unfolding and misfolding. Thus, these order-to-disorder or disorder-to-order transitions may regulate cellular function. Tau, a neuronal protein, regulates microtubule (MT) structure and overall cellular integrity. However, misfolded tau modified by PTMs results in MT destabilization, toxic tau aggregate formation, and ultimately cell death, leading to neurodegeneration. Currently, the lack of structural information surrounding tau severely limits understanding of neurodegeneration. This minireview focuses on the current methodologies and approaches aimed at probing tau conformation and the role of conformation in various aspects of tau biochemistry. The recent applications of nuclear magnetic resonance, mass spectrometry, F?rster resonance electron transfer, and molecular dynamics simulations toward structural analysis of conformational landscapes of tau will be described. The strategies developed for structural evaluation of tau may significantly improve our understanding of misfolding diseases.
机译:蛋白质误折叠疾病基于通过内部和分子间接触引发的聚集原理。通过改性后修饰(PTMS)等生物化学转化诱导的结构和构象变化,通常导致蛋白质展开和错误折叠。因此,这些订单到紊乱或无序的转换可能调节蜂窝功能。 TAU,神经元蛋白,调节微管(MT)结构和总体细胞完整性。然而,由PTMS修饰的错误折叠导致MT不稳定,有毒的Tau骨料形成,最终是细胞死亡,导致神经变性。目前,围绕土地的结构信息严重限制了对神经变性的理解。该Minireview专注于目前旨在探测TAU构象的方法和方法以及构象在TAU生物化学各方面的作用。将描述近期核磁共振,质谱法,F?奔跑共振电子转移和朝着陶器构象景观结构分析的分子动力学模拟。对TAU的结构评估制定的策略可能会显着提高我们对错误折叠疾病的理解。

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