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真菌中的同肽和同密码子水平与 GC/AT 偏向和固有无序性相关,某些氨基酸具有独特的行为。

Homopeptide and homocodon levels across fungi are coupled to GC/AT-bias and intrinsic disorder, with unique behaviours for some amino acids.

机构信息

Department of Biology, McGill University, Montreal, QC, Canada.

出版信息

Sci Rep. 2021 May 11;11(1):10025. doi: 10.1038/s41598-021-89650-1.

Abstract

Homopeptides (runs of one amino-acid type) are evolutionarily important since they are prone to expand/contract during DNA replication, recombination and repair. To gain insight into the genomic/proteomic traits driving their variation, we analyzed how homopeptides and homocodons (which are pure codon repeats) vary across 405 Dikarya, and probed their linkage to genome GC/AT bias and other factors. We find that amino-acid homopeptide frequencies vary diversely between clades, with the AT-rich Saccharomycotina trending distinctly. As organisms evolve, homocodon and homopeptide numbers are majorly coupled to GC/AT-bias, exhibiting a bi-furcated correlation with degree of AT- or GC-bias. Mid-GC/AT genomes tend to have markedly fewer simply because they are mid-GC/AT. Despite these trends, homopeptides tend to be GC-biased relative to other parts of coding sequences, even in AT-rich organisms, indicating they absorb AT bias less or are inherently more GC-rich. The most frequent and most variable homopeptide amino acids favour intrinsic disorder, and there are an opposing correlation and anti-correlation versus homopeptide levels for intrinsic disorder and structured-domain content respectively. Specific homopeptides show unique behaviours that we suggest are linked to inherent slippage probabilities during DNA replication and recombination, such as poly-glutamine, which is an evolutionarily very variable homopeptide with a codon repertoire unbiased for GC/AT, and poly-lysine whose homocodons are overwhelmingly made from the codon AAG.

摘要

同源肽(一种氨基酸类型的重复)在进化上很重要,因为它们在 DNA 复制、重组和修复过程中容易扩展/收缩。为了深入了解驱动它们变异的基因组/蛋白质特征,我们分析了同源肽和同型密码子(纯密码子重复)如何在 405 种担子菌中变化,并探究了它们与基因组 GC/AT 偏倚和其他因素的联系。我们发现,氨基酸同源肽的频率在不同的进化枝之间差异很大,富含 AT 的 Saccharomycotina 明显偏向于富含 AT。随着生物体的进化,同型密码子和同源肽的数量主要与 GC/AT 偏倚相关,与 AT 或 GC 偏倚的程度呈双分叉相关。中 GC/AT 基因组往往明显较少,仅仅是因为它们处于中 GC/AT 水平。尽管存在这些趋势,但同源肽相对于编码序列的其他部分往往偏向 GC,即使在富含 AT 的生物体中也是如此,这表明它们吸收 AT 偏倚较少,或者本身更富含 GC。最频繁和最易变的同源肽氨基酸倾向于固有无序,固有无序和结构域含量与同源肽水平之间存在相反的相关性和反相关性。特定的同源肽表现出独特的行为,我们认为这些行为与 DNA 复制和重组过程中的固有滑移概率有关,例如多谷氨酰胺,它是一种进化上非常可变的同源肽,其密码子库不受 GC/AT 的影响,多赖氨酸的同型密码子几乎全部由 AAG 密码子组成。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e9b7/8113271/709b05619212/41598_2021_89650_Fig1_HTML.jpg

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