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硫氧还蛋白家族中折叠速率的非守恒性揭示了祖先无辅助折叠的降解。

Non-conservation of folding rates in the thioredoxin family reveals degradation of ancestral unassisted-folding.

机构信息

Departamento de Quimica Fisica, Facultad de Ciencias, Unidad de Excelencia de Química Aplicada a Biomedicina y Medioambiente (UEQ), Universidad de Granada, 18071 Granada, Spain.

Department of Biology, Georgia State University, Atlanta, GA 30303, U.S.A.

出版信息

Biochem J. 2019 Dec 12;476(23):3631-3647. doi: 10.1042/BCJ20190739.

Abstract

Evolution involves not only adaptation, but also the degradation of superfluous features. Many examples of degradation at the morphological level are known (vestigial organs, for instance). However, the impact of degradation on molecular evolution has been rarely addressed. Thioredoxins serve as general oxidoreductases in all cells. Here, we report extensive mutational analyses on the folding of modern and resurrected ancestral bacterial thioredoxins. Contrary to claims from recent literature, in vitro folding rates in the thioredoxin family are not evolutionarily conserved, but span at least a ∼100-fold range. Furthermore, modern thioredoxin folding is often substantially slower than ancestral thioredoxin folding. Unassisted folding, as probed in vitro, thus emerges as an ancestral vestigial feature that underwent degradation, plausibly upon the evolutionary emergence of efficient cellular folding assistance. More generally, our results provide evidence that degradation of ancestral features shapes, not only morphological evolution, but also the evolution of individual proteins.

摘要

进化不仅涉及适应,还涉及多余特征的退化。许多形态水平退化的例子是已知的(例如退化器官)。然而,退化对分子进化的影响很少被涉及。硫氧还蛋白在所有细胞中作为通用的氧化还原酶。在这里,我们报告了对现代和复活的祖先细菌硫氧还蛋白折叠的广泛突变分析。与最近文献中的说法相反,在硫氧还蛋白家族中,体外折叠速率在进化上没有保守,而是跨越至少 100 倍的范围。此外,现代硫氧还蛋白折叠通常比祖先硫氧还蛋白折叠慢得多。因此,在体外探测到的无辅助折叠,作为一个古老的退化特征出现,很可能是在有效的细胞折叠辅助进化出现后退化的。更一般地说,我们的结果提供了证据,表明祖先特征的退化不仅塑造了形态进化,而且塑造了单个蛋白质的进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/68b1/6906118/7071b9f51d85/BCJ-476-3631-g0001.jpg

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