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人类蛋白质组内固有无序的模块性。

Modularity of intrinsic disorder in the human proteome.

机构信息

Department of Biology, Centre for Genomics and Systems Biology, New York University, NY, USA.

出版信息

Proteins. 2010 Jan;78(1):212-21. doi: 10.1002/prot.22504.

Abstract

Predicting regions of disorder has become of increasing interest when determining protein structure and function. With approximately 33% of eukaryotic proteins having significant disordered regions, and an increasing occurrence of disorder in higher organisms, an analysis of the importance of disorder from an evolutionary perspective was clearly warranted. Focusing on the human proteome, we have studied how abundant disorder is and its relevance to protein function and structure. We have shown that disordered regions frequently appear to be independent functional units, and judged by complete association to certain protein domains, may be evolutionarily conserved. Our work also supports previous analyses on association between disorder and alternate splicing and provides support for the modularity of disorder by showing that with respect to splicing events, disordered regions frequently appear to be spliced as whole units.

摘要

预测蛋白质结构和功能的无序区域已成为日益关注的焦点。大约 33%的真核蛋白质具有显著的无序区域,并且无序区域在高等生物中越来越常见,因此从进化角度分析无序区域的重要性是合理的。本文聚焦于人类蛋白质组,研究了无序的丰富程度及其与蛋白质功能和结构的相关性。我们已经表明,无序区域经常似乎是独立的功能单元,并且根据与某些蛋白质结构域的完全关联,可以推断它们在进化上是保守的。我们的工作还支持了以前关于无序与可变剪接之间关联的分析,并通过显示在剪接事件方面,无序区域经常作为整体单元进行剪接,为无序的模块性提供了支持。

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