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反转录基因对人类基因组、蛋白质组和转录组的复杂分析。

Complex Analysis of Retroposed Genes' Contribution to Human Genome, Proteome and Transcriptome.

机构信息

Faculty of Biology, Institute of Human Biology and Evolution, Adam Mickiewicz University, 61-614 Poznań, Poland.

出版信息

Genes (Basel). 2020 May 12;11(5):542. doi: 10.3390/genes11050542.

Abstract

Gene duplication is a major driver of organismal evolution. One of the main mechanisms of gene duplications is retroposition, a process in which mRNA is first transcribed into DNA and then reintegrated into the genome. Most gene retrocopies are depleted of the regulatory regions. Nevertheless, examples of functional retrogenes are rapidly increasing. These functions come from the gain of new spatio-temporal expression patterns, imposed by the content of the genomic sequence surrounding inserted cDNA and/or by selectively advantageous mutations, which may lead to the switch from protein coding to regulatory RNA. As recent studies have shown, these genes may lead to new protein domain formation through fusion with other genes, new regulatory RNAs or other regulatory elements. We utilized existing data from high-throughput technologies to create a complex description of retrogenes functionality. Our analysis led to the identification of human retroposed genes that substantially contributed to transcriptome and proteome. These retrocopies demonstrated the potential to encode proteins or short peptides, act as and - Natural Antisense Transcripts (NATs), regulate their progenitors' expression by competing for the same microRNAs, and provide a sequence to lncRNA and novel exons to existing protein-coding genes. Our study also revealed that retrocopies, similarly to retrotransposons, may act as recombination hot spots. To our best knowledge this is the first complex analysis of these functions of retrocopies.

摘要

基因复制是生物进化的主要驱动力之一。基因复制的主要机制之一是反转录,即 mRNA 首先被转录成 DNA,然后再整合到基因组中。大多数基因反转录本缺乏调控区。然而,功能反转录基因的例子正在迅速增加。这些功能来自于新的时空表达模式的获得,这些模式是由插入 cDNA 周围的基因组序列的内容以及选择性有利的突变所强加的,这可能导致从蛋白质编码到调节 RNA 的转变。正如最近的研究表明,这些基因可能通过与其他基因融合、新的调节 RNA 或其他调节元件形成新的蛋白质结构域。我们利用高通量技术的现有数据,对反转录基因的功能进行了复杂的描述。我们的分析确定了对转录组和蛋白质组有重大贡献的人类反转录基因。这些反转录本表现出编码蛋白质或短肽的潜力,作为 和 - 天然反义转录物(NATs)发挥作用,通过竞争相同的 microRNAs 来调节其前体的表达,并为 lncRNA 和现有蛋白质编码基因提供新的外显子。我们的研究还表明,反转录本与反转录转座子一样,可能作为重组热点。据我们所知,这是对反转录本这些功能的首次综合分析。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/712e/7290577/410805eea214/genes-11-00542-g001.jpg

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