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……中可变剪接的遗传调控 (原文不完整,翻译可能不太准确,需结合完整内容)

The Genetic Regulation of Alternative Splicing in .

作者信息

Noble Jerald D, Balmant Kelly M, Dervinis Christopher, de Los Campos Gustavo, Resende Márcio F R, Kirst Matias, Barbazuk William Brad

机构信息

Plant Molecular and Cellular Biology Graduate Program, University of Florida, Gainesville, FL, United States.

School of Forest Resources and Conservation, University of Florida, Gainesville, FL, United States.

出版信息

Front Plant Sci. 2020 Jun 5;11:590. doi: 10.3389/fpls.2020.00590. eCollection 2020.

Abstract

Alternative splicing (AS) is a mechanism of regulation of the proteome via enabling the production of multiple mRNAs from a single gene. To date, the dynamics of AS and its effects on the protein sequences of individuals in a large and genetically unrelated population of trees have not been investigated. Here we describe the diversity of AS events within a previously genotyped population of 268 individuals of and their putative downstream functional effects. Using a robust bioinformatics pipeline, the AS events and resulting transcript isoforms were discovered and quantified for each individual in the population. Analysis of the AS revealed that, as expected, most AS isoforms are conserved. However, we also identified a substantial collection of new, unannotated splice junctions and transcript isoforms. Heritability estimates for the expression of transcript isoforms showed that approximately half of the isoforms are heritable. The genetic regulators of these AS isoforms and splice junction usage were then identified using a genome-wide association analysis. The expression of AS isoforms was predominately regulated while splice junction usage was generally regulated in . Additionally, we identified 696 genes encoding alternatively spliced isoforms that changed putative protein domains relative to the longest protein coding isoform of the gene, and 859 genes exhibiting this same phenomenon relative to the most highly expressed isoform. Finally, we found that 748 genes gained or lost micro-RNA binding sites relative to the longest protein coding isoform of a given gene, while 940 gained or lost micro-RNA binding sites relative to the most highly expressed isoform. These results indicate that a significant fraction of AS events are genetically regulated and that this isoform usage can result in protein domain architecture changes.

摘要

可变剪接(AS)是一种通过使单个基因产生多个mRNA来调节蛋白质组的机制。迄今为止,尚未研究在一个大型且遗传不相关的树木群体中,可变剪接的动态变化及其对个体蛋白质序列的影响。在这里,我们描述了在一个先前已进行基因分型的包含268个个体的群体中可变剪接事件的多样性及其假定的下游功能效应。使用强大的生物信息学流程,发现并量化了该群体中每个个体的可变剪接事件及产生的转录本异构体。对可变剪接的分析表明,正如预期的那样,大多数可变剪接异构体是保守的。然而,我们也鉴定出了大量新的、未注释的剪接接头和转录本异构体。对转录本异构体表达的遗传力估计表明,大约一半的异构体是可遗传的。然后,使用全基因组关联分析确定了这些可变剪接异构体和剪接接头使用的遗传调节因子。可变剪接异构体的表达主要受调控,而剪接接头的使用在……中通常受调控。此外,我们鉴定出696个编码可变剪接异构体的基因,这些异构体相对于该基因最长的蛋白质编码异构体改变了假定的蛋白质结构域,还有859个基因相对于最高表达的异构体表现出相同的现象。最后,我们发现,相对于给定基因最长的蛋白质编码异构体,748个基因获得或失去了微小RNA结合位点,而相对于最高表达的异构体,940个基因获得或失去了微小RNA结合位点。这些结果表明,相当一部分可变剪接事件受到遗传调控,并且这种异构体的使用可导致蛋白质结构域结构的变化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/edc1/7291814/5675688cc1a3/fpls-11-00590-g001.jpg

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