Tracing the birth and intrinsic disorder of loops and domains in protein evolution.

IF 4.9 Q1 BIOPHYSICS
Biophysical reviews Pub Date : 2024-11-20 eCollection Date: 2024-12-01 DOI:10.1007/s12551-024-01251-0
Gustavo Caetano-Anollés, Fizza Mughal, M Fayez Aziz, Kelsey Caetano-Anollés
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引用次数: 0

Abstract

Protein loops and structural domains are building blocks of molecular structure. They hold evolutionary memory and are largely responsible for the many functions and processes that drive the living world. Here, we briefly review two decades of phylogenomic data-driven research focusing on the emergence and evolution of these elemental architects of protein structure. Phylogenetic trees of domains reconstructed from the proteomes of organisms belonging to all three superkingdoms and viruses were used to build chronological timelines describing the origin of each domain and its embedded loops at different levels of structural abstraction. These timelines consistently recovered six distinct evolutionary phases and a most parsimonious evolutionary progression of cellular life. The timelines also traced the birth of domain structures from loops, which allowed to model their growth ab initio with AlphaFold2. Accretion decreased the disorder of the growing molecules, suggesting disorder is molecular size-dependent. A phylogenomic survey of disorder revealed that loops and domains evolved differently. Loops were highly disordered, disorder increased early in evolution, and ordered and moderate disordered structures were derived. Gradual replacement of loops with α-helix and β-strand bracing structures over time paved the way for the dominance of more disordered loop types. In contrast, ancient domains were ordered, with disorder evolving as a benefit acquired later in evolution. These evolutionary patterns explain inverse correlations between disorder and sequence length of loops and domains. Our findings provide a deep evolutionary view of the link between structure, disorder, flexibility, and function.

追踪蛋白质进化中环和结构域的诞生和内在紊乱。
蛋白质环和结构域是分子结构的组成部分。它们拥有进化记忆,并在很大程度上负责驱动生命世界的许多功能和过程。在这里,我们简要回顾了二十年来系统基因组数据驱动的研究,重点关注这些蛋白质结构的基本建筑师的出现和进化。从属于所有三个超级王国和病毒的生物体的蛋白质组中重建的结构域的系统发育树被用来建立时间轴,描述每个结构域的起源及其在不同结构抽象水平上的嵌入回路。这些时间线一致地恢复了六个不同的进化阶段和细胞生命最简约的进化进程。时间线还追踪了环域结构的诞生,这使得用AlphaFold2从头开始模拟它们的生长成为可能。增积降低了生长分子的无序性,表明无序性与分子大小有关。一项疾病的系统基因组调查显示,环路和结构域的进化方式不同。环路高度无序,在进化早期无序度增加,并衍生出有序和中度无序结构。随着时间的推移,α-螺旋和β-链支撑结构逐渐取代环,为更无序的环类型的主导地位铺平了道路。相反,古代的域是有序的,无序的进化是在进化的后期获得的好处。这些进化模式解释了环和结构域的无序程度与序列长度之间的负相关关系。我们的发现为结构、紊乱、灵活性和功能之间的联系提供了一个深刻的进化观点。
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来源期刊
Biophysical reviews
Biophysical reviews Biochemistry, Genetics and Molecular Biology-Biophysics
CiteScore
8.90
自引率
0.00%
发文量
93
期刊介绍: Biophysical Reviews aims to publish critical and timely reviews from key figures in the field of biophysics. The bulk of the reviews that are currently published are from invited authors, but the journal is also open for non-solicited reviews. Interested authors are encouraged to discuss the possibility of contributing a review with the Editor-in-Chief prior to submission. Through publishing reviews on biophysics, the editors of the journal hope to illustrate the great power and potential of physical techniques in the biological sciences, they aim to stimulate the discussion and promote further research and would like to educate and enthuse basic researcher scientists and students of biophysics. Biophysical Reviews covers the entire field of biophysics, generally defined as the science of describing and defining biological phenomenon using the concepts and the techniques of physics. This includes but is not limited by such areas as: - Bioinformatics - Biophysical methods and instrumentation - Medical biophysics - Biosystems - Cell biophysics and organization - Macromolecules: dynamics, structures and interactions - Single molecule biophysics - Membrane biophysics, channels and transportation
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