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基于蛋白质质谱的结构系统发生学:概念验证。

Structural Phylogenetics with Protein Mass Spectrometry: A Proof-of-Concept.

机构信息

Infectious Disease Responses Laboratory, Prince of Wales Clinical Research Sciences, Sydney, NSW, Australia.

出版信息

Protein J. 2024 Oct;43(5):997-1008. doi: 10.1007/s10930-024-10227-8. Epub 2024 Jul 29.

Abstract

It is demonstrated, for the first time, that a mass spectrometry approach (known as phylonumerics) can be successfully implemented for structural phylogenetics investigations to chart the evolution of a protein's structure and function. Illustrated for the compact globular protein myoglobin, peptide masses produced from the proteolytic digestion of the protein across animal species generate trees congruent to the sequence tree counterparts. Single point mutations calculated during the same mass tree building step can be followed along interconnected branches of the tree and represent a viable structural metric. A mass tree built for 15 diverse animal species, easily resolve the birds from mammal species, and the ruminant mammals from the remainder of the animals. Mutations within helix-spanning peptide segments alter both the mass and structure of the protein in these segments. Greater evolution is found in the B-helix over the A, E, F, G and H helices. A further mass tree study, of six more closely related primate species, resolves gorilla from the other primates based on a P22S mutation within the B-helix. The remaining five primates are resolved into two groups based on whether they contain a glycine or serine at position 23 in the same helix. The orangutan is resolved from the gibbon and siamang by its G-helix C110S mutation, while homo sapiens are resolved from chimpanzee based on the Q116H mutation. All are associated with structural perturbations in such helices. These structure altering mutations can be tracked along interconnecting branches of a mass tree, to follow the protein's structure and evolution, and ultimately the evolution of the species in which the proteins are expressed. Those that have the greatest impact on a protein's structure, its function, and ultimately the evolution of the species, can be selectively tracked or monitored.

摘要

首次证明,一种质谱方法(称为 phylonumerics)可成功地用于结构系统发生学研究,以描绘蛋白质结构和功能的进化。以紧凑的球状蛋白肌红蛋白为例,从蛋白质的蛋白水解消化中产生的肽质量在跨越动物物种的情况下生成与序列树相对应的树。在同一质谱树构建步骤中计算的单点突变可以沿着树的互连分支进行跟踪,并代表一种可行的结构度量。为 15 个不同的动物物种构建的质量树很容易将鸟类与哺乳动物物种区分开,将反刍哺乳动物与其余动物区分开。在跨越螺旋肽段的突变会改变这些段中蛋白质的质量和结构。在 B-螺旋中发现的进化大于 A、E、F、G 和 H 螺旋。对六个亲缘关系更密切的灵长类物种进行的进一步质量树研究,根据 B-螺旋内的 P22S 突变将大猩猩与其他灵长类动物区分开。其余五种灵长类动物根据其在同一螺旋中第 23 位是否含有甘氨酸或丝氨酸分为两组。由于 C110S 突变位于 G-螺旋中,猩猩与长臂猿和猩猩分开,而智人则因其 Q116H 突变与黑猩猩分开。所有这些突变都与这些螺旋中的结构扰动有关。这些改变结构的突变可以沿着质谱树的互连分支进行跟踪,以跟踪蛋白质的结构和进化,最终跟踪蛋白质表达的物种的进化。那些对蛋白质结构、功能,最终对物种进化影响最大的突变,可以进行选择性跟踪或监测。

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