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How disordered is my protein and what is its disorder for? A guide through the “dark side” of the protein universe

机译:如何无序是我的蛋白质,它是什么障碍?蛋白质的宇宙

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摘要

In the last 2 decades it has become increasingly evident that a large number of proteins are either fully or partially disordered. Intrinsically disordered proteins lack a stable 3D structure, are ubiquitous and fulfill essential biological functions.Their conformational heterogeneity is encoded in their amino acid sequences, thereby allowing intrinsically disordered proteins or regions to be recognized based on properties of these sequences. The identification of disordered regions facilitates thefunctional annotation of proteins and is instrumental for delineating boundaries of protein domains amenable to structural determination with X-ray crystallization. This article discusses a comprehensive selection of databases and methods currently employed to disseminate experimental and putative annotations of disorder, predict disorder and identify regions involved in induced folding. It also provides a set of detailed instructions that should be followed to perform computational analysis of disorder.
机译:在过去的2年已成为越来越多明显,大量的蛋白质要么全部或部分无序。内在无序蛋白质缺乏稳定3 d结构,是无处不在的,满足重要的生物功能。构象异构性是他们的编码氨基酸序列,从而允许内在无序蛋白质或地区基于属性的识别序列。地区促进thefunctional注释的蛋白质和描述工具边界的蛋白质域服从与x射线结构测定结晶。综合数据库的选择和方法目前用来传播实验和假定的注释的障碍,预测障碍和识别区域参与诱导折叠。应遵循执行的指令计算分析的障碍。

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