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当“内在无序多肽”还是“无序氨基酸聚合物”时:如何研究内在无序多氨基酸链的非构象

When "IUPs" were "BAPs": How to study the nonconformation of intrinsically unfolded polyaminoacid chains.

作者信息

Pastore Annalisa, Temussi Pierandrea

机构信息

National Institute for Medical Research, The Ridgeway, London, NW7 1AA, United Kingdom.

出版信息

Biopolymers. 2013 Nov;100(6):592-600. doi: 10.1002/bip.22363.

Abstract

Ideas often recur. It has been pointed out recently that proteins are not always the well-structured entities we have become accustomed to from crystallographic studies, but may be intrinsically unstructured or contain unstructured regions. This feature, far from making these proteins less interesting, is an essential requirement for their function. Fascinating though it may be, the concept of so-called intrinsically unfolded (or unordered) proteins (IUPs), also often referred to as intrinsically disordered proteins (IDPs), is not new: it directly links back to the 1970s when the attention of many structural biologists was focused on biologically active peptides, which like IUPs lack a specific defined conformation. The recurrent nature of this concept may now be of topical interest since it suggests the transfer, upon suitable adaptation, of old tools to develop new ideas. Here, we review some of the approaches that were developed for the study of peptides and discuss how they could inspire powerful new methodologies for the study of IUPs.

摘要

观点常常反复出现。最近有人指出,蛋白质并不总是我们从晶体学研究中所习惯的结构规整的实体,而是可能本质上无结构或包含无结构区域。这一特征非但使这些蛋白质不那么有趣,反而对其功能来说是一项基本要求。尽管所谓的内在无序(或无规)蛋白质(IUPs),也常被称为内在无序蛋白(IDPs)这一概念可能很吸引人,但它并非新事物:它可以直接追溯到20世纪70年代,当时许多结构生物学家的注意力集中在生物活性肽上,这些生物活性肽与IUPs一样缺乏特定的明确构象。这个概念的反复出现如今可能具有热门意义,因为它表明在适当调整后,旧工具可用于开发新想法。在此,我们回顾一些为研究肽而开发的方法,并讨论它们如何能启发用于研究IUPs的强大新方法。

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