On Protein Loops, Prior Molecular States and Common Ancestors of Life

IF 2.1 3区 生物学 Q4 BIOCHEMISTRY & MOLECULAR BIOLOGY
Kelsey Caetano-Anollés, M. Fayez Aziz, Fizza Mughal, Gustavo Caetano-Anollés
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Abstract

The principle of continuity demands the existence of prior molecular states and common ancestors responsible for extant macromolecular structure. Here, we focus on the emergence and evolution of loop prototypes – the elemental architects of protein domain structure. Phylogenomic reconstruction spanning superkingdoms and viruses generated an evolutionary chronology of prototypes with six distinct evolutionary phases defining a most parsimonious evolutionary progression of cellular life. Each phase was marked by strategic prototype accumulation shaping the structures and functions of common ancestors. The last universal common ancestor (LUCA) of cells and viruses and the last universal cellular ancestor (LUCellA) defined stem lines that were structurally and functionally complex. The evolutionary saga highlighted transformative forces. LUCA lacked biosynthetic ribosomal machinery, while the pivotal LUCellA lacked essential DNA biosynthesis and modern transcription. Early proteins therefore relied on RNA for genetic information storage but appeared initially decoupled from it, hinting at transformative shifts of genetic processing. Urancestral loop types suggest advanced folding designs were present at an early evolutionary stage. An exploration of loop geometric properties revealed gradual replacement of prototypes with α-helix and β-strand bracing structures over time, paving the way for the dominance of other loop types. AlphFold2-generated atomic models of prototype accretion described patterns of fold emergence. Our findings favor a ‛processual’ model of evolving stem lines aligned with Woese’s vision of a communal world. This model prompts discussing the ‘problem of ancestors’ and the challenges that lie ahead for research in taxonomy, evolution and complexity.

Abstract Image

论蛋白质环、先验分子状态和生命的共同祖先
连续性原则要求存在先前的分子状态和负责现存大分子结构的共同祖先。在这里,我们重点研究了环原型--蛋白质结构域的基本架构师--的出现和进化。横跨超王国和病毒的系统发生组学重建生成了一个原型进化年表,其中有六个不同的进化阶段,定义了细胞生命最合理的进化进程。每个阶段都以塑造共同祖先结构和功能的战略原型积累为标志。细胞和病毒的最后一个普遍共同祖先(LUCA)和最后一个普遍细胞祖先(LUCellA)定义了结构和功能复杂的干系。进化传奇凸显了变革力量。LUCA 缺乏生物合成核糖体机制,而关键的 LUCellA 则缺乏必要的 DNA 生物合成和现代转录。因此,早期蛋白质依赖于 RNA 来存储遗传信息,但最初似乎与 RNA 脱钩,这暗示了遗传处理过程的转变。星状环类型表明在早期进化阶段就存在先进的折叠设计。对环路几何特性的研究表明,随着时间的推移,α螺旋和β链支撑结构逐渐取代了原型结构,为其他环路类型占据主导地位铺平了道路。AlphFold2 生成的原型增殖原子模型描述了折叠出现的模式。我们的研究结果倾向于茎线进化的 "过程 "模型,这与 Woese 的共同世界愿景一致。这一模型促使我们讨论 "祖先问题 "以及分类学、进化和复杂性研究面临的挑战。
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来源期刊
Journal of Molecular Evolution
Journal of Molecular Evolution 生物-进化生物学
CiteScore
5.50
自引率
2.60%
发文量
36
审稿时长
3 months
期刊介绍: Journal of Molecular Evolution covers experimental, computational, and theoretical work aimed at deciphering features of molecular evolution and the processes bearing on these features, from the initial formation of macromolecular systems through their evolution at the molecular level, the co-evolution of their functions in cellular and organismal systems, and their influence on organismal adaptation, speciation, and ecology. Topics addressed include the evolution of informational macromolecules and their relation to more complex levels of biological organization, including populations and taxa, as well as the molecular basis for the evolution of ecological interactions of species and the use of molecular data to infer fundamental processes in evolutionary ecology. This coverage accommodates such subfields as new genome sequences, comparative structural and functional genomics, population genetics, the molecular evolution of development, the evolution of gene regulation and gene interaction networks, and in vitro evolution of DNA and RNA, molecular evolutionary ecology, and the development of methods and theory that enable molecular evolutionary inference, including but not limited to, phylogenetic methods.
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