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长末端重复序列赋予哺乳动物卵母细胞和受精卵中基因和基因表达程序的演化动力。

Long terminal repeats power evolution of genes and gene expression programs in mammalian oocytes and zygotes.

机构信息

Bioinformatics Group, Division of Molecular Biology, Department of Biology, Faculty of Science, University of Zagreb, 10000, Zagreb, Croatia.

Institute of Molecular Genetics, Academy of Sciences of the Czech Republic, 142 20 Prague 4, Czech Republic.

出版信息

Genome Res. 2017 Aug;27(8):1384-1394. doi: 10.1101/gr.216150.116. Epub 2017 May 18.

Abstract

Retrotransposons are "copy-and-paste" insertional mutagens that substantially contribute to mammalian genome content. Retrotransposons often carry long terminal repeats (LTRs) for retrovirus-like reverse transcription and integration into the genome. We report an extraordinary impact of a group of LTRs from the mammalian endogenous retrovirus-related ERVL retrotransposon class on gene expression in the germline and beyond. In mouse, we identified more than 800 LTRs from ORR1, MT, MT2, and MLT families, which resemble mobile gene-remodeling platforms that supply promoters and first exons. The LTR-mediated gene remodeling also extends to hamster, human, and bovine oocytes. The LTRs function in a stage-specific manner during the oocyte-to-embryo transition by activating transcription, altering protein-coding sequences, producing noncoding RNAs, and even supporting evolution of new protein-coding genes. These functions result, for example, in recycling processed pseudogenes into mRNAs or lncRNAs with regulatory roles. The functional potential of the studied LTRs is even higher, because we show that dormant LTR promoter activity can rescue loss of an essential upstream promoter. We also report a novel protein-coding gene evolution--in which an MT LTR provided a promoter and the 5' exon with a functional start codon while the bulk of the protein-coding sequence evolved through a CAG repeat expansion. Altogether, ERVL LTRs provide molecular mechanisms for stochastically scanning, rewiring, and recycling genetic information on an extraordinary scale. ERVL LTRs thus offer means for a comprehensive survey of the genome's expression potential, tightly intertwining with gene expression and evolution in the germline.

摘要

逆转录转座子是“复制粘贴”插入诱变剂,它们极大地促进了哺乳动物基因组的内容。逆转录转座子通常带有长末端重复序列(LTRs),用于类似于逆转录病毒的逆转录和整合到基因组中。我们报告了一组来自哺乳动物内源性逆转录病毒相关 ERVL 逆转录转座子类的 LTR 对生殖系和其他基因表达的非凡影响。在小鼠中,我们从 ORR1、MT、MT2 和 MLT 家族中鉴定了 800 多个 LTR,它们类似于提供启动子和第一外显子的移动基因重塑平台。LTR 介导的基因重塑也扩展到了仓鼠、人类和牛卵母细胞。LTR 以在卵母细胞到胚胎过渡过程中特定的阶段发挥作用,通过激活转录、改变蛋白质编码序列、产生非编码 RNA,甚至支持新蛋白质编码基因的进化。这些功能导致例如将加工后的假基因回收为具有调节作用的 mRNA 或 lncRNA。所研究的 LTR 的功能潜力甚至更高,因为我们表明休眠的 LTR 启动子活性可以挽救必需上游启动子的丧失。我们还报告了一种新的蛋白质编码基因进化,其中 MT LTR 提供了一个启动子和具有功能起始密码子的 5'外显子,而蛋白质编码序列的大部分则通过 CAG 重复扩展进化而来。总的来说,ERVL LTR 为随机扫描、重新布线和以非凡规模回收遗传信息提供了分子机制。ERVL LTR 因此提供了一种全面调查基因组表达潜力的手段,与生殖系中的基因表达和进化紧密交织。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/24ff/5538554/f2c6bde93a6e/1384f01.jpg

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