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一种估计对重叠基因自然选择强度的简单方法。

A simple method for estimating the strength of natural selection on overlapping genes.

作者信息

Wei Xinzhu, Zhang Jianzhi

机构信息

Department of Ecology and Evolutionary Biology, University of Michigan.

Department of Ecology and Evolutionary Biology, University of Michigan

出版信息

Genome Biol Evol. 2014 Dec 31;7(1):381-90. doi: 10.1093/gbe/evu294.

Abstract

Overlapping genes, where one DNA sequence codes for two proteins with different reading frames, are not uncommon in viruses and cellular organisms. Estimating the direction and strength of natural selection acting on overlapping genes is important for understanding their functionality, origin, evolution, maintenance, and potential interaction. However, the standard methods for estimating synonymous (dS) and nonsynonymous (dN) nucleotide substitution rates are inapplicable here because a nucleotide change can be simultaneously synonymous and nonsynonymous when both reading frames involved are considered. We have developed a simple method that can estimate dN/dS and test for the action of natural selection in each relevant reading frame of the overlapping genes. Our method is an extension of the modified Nei-Gojobori method previously developed for nonoverlapping genes. We confirmed the reliability of our method using extensive computer simulation. Applying this method, we studied the longest human sense-antisense overlapping gene pair, LRRC8E and ENSG00000214248. Although LRRC8E (leucine-rich repeat containing eight family, member E) is known to regulate cell size, the function of ENSG00000214248 is unknown. Our analysis revealed purifying selection on ENSG00000214248 and suggested that it originated in the common ancestor of bony vertebrates.

摘要

重叠基因是指一段DNA序列可编码两种具有不同阅读框的蛋白质,这种情况在病毒和细胞生物中并不罕见。估计作用于重叠基因的自然选择的方向和强度,对于理解它们的功能、起源、进化、维持及潜在相互作用至关重要。然而,估计同义(dS)和非同义(dN)核苷酸替换率的标准方法在此并不适用,因为当考虑两个相关阅读框时,一个核苷酸变化可能同时是同义的和非同义的。我们开发了一种简单方法,可估计dN/dS并检测重叠基因各相关阅读框中自然选择的作用。我们的方法是先前为非重叠基因开发的改良Nei-Gojobori方法的扩展。我们通过广泛的计算机模拟证实了我们方法的可靠性。应用此方法,我们研究了人类最长的正义-反义重叠基因对LRRC8E和ENSG00000214248。尽管已知LRRC8E(富含亮氨酸重复序列8家族成员E)可调节细胞大小,但ENSG00000214248的功能尚不清楚。我们的分析揭示了对ENSG00000214248的纯化选择,并表明它起源于硬骨脊椎动物的共同祖先。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1891/4316641/f15c039cd962/evu294f1p.jpg

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