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5'-转导 SVA 逆转录转座子群有效地在人类基因组中扩散。

5'-Transducing SVA retrotransposon groups spread efficiently throughout the human genome.

机构信息

Fachgebiet PR2/Retroelemente, Paul-Ehrlich-Institut, D-63225 Langen, Germany.

出版信息

Genome Res. 2009 Nov;19(11):1992-2008. doi: 10.1101/gr.093435.109. Epub 2009 Aug 3.

Abstract

SVA elements represent the youngest family of hominid non-LTR retrotransposons, which alter the human genome continuously. They stand out due to their organization as composite repetitive elements. To draw conclusions on the assembly process that led to the current organization of SVA elements and on their transcriptional regulation, we initiated our study by assessing differences in structures of the 116 SVA elements located on human chromosome 19. We classified SVA elements into seven structural variants, including novel variants like 3'-truncated elements and elements with 5'-flanking sequence transductions. We established a genome-wide inventory of 5'-transduced SVA elements encompassing approximately 8% of all human SVA elements. The diversity of 5' transduction events found indicates transcriptional control of their SVA source elements by a multitude of external cellular promoters in germ cells in the course of their evolution and suggests that SVA elements might be capable of acquiring 5' promoter sequences. Our data indicate that SVA-mediated 5' transduction events involve alternative RNA splicing at cryptic splice sites. We analyzed one remarkably successful human-specific SVA 5' transduction group in detail because it includes at least 32% of all SVA subfamily F members. An ancient retrotransposition event brought an SVA insertion under transcriptional control of the MAST2 gene promoter, giving rise to the primal source element of this group. Members of this group are currently transcribed. Here we show that SVA-mediated 5' transduction events lead to structural diversity of SVA elements and represent a novel source of genomic rearrangements contributing to genomic diversity.

摘要

SVA 元件代表了朊病毒非 LTR 反转录转座子家族中最年轻的成员,它们不断改变人类基因组。由于它们作为复合重复元件的组织方式,它们显得尤为突出。为了得出关于导致 SVA 元件当前组织的组装过程的结论,并对其转录调控进行研究,我们通过评估位于人类 19 号染色体上的 116 个 SVA 元件的结构差异,开始了我们的研究。我们将 SVA 元件分为七种结构变体,包括 3'-截短元件和具有 5'-侧翼序列转导的新型变体。我们建立了一个涵盖大约 8%的人类 SVA 元件的全基因组 5'-转导 SVA 元件的库存。发现的 5'转导事件的多样性表明,在它们的进化过程中,生殖细胞中的多种外部细胞启动子对它们的 SVA 源元件进行转录调控,并表明 SVA 元件可能能够获得 5'启动子序列。我们的数据表明,SVA 介导的 5'转导事件涉及在隐蔽剪接位点的选择性 RNA 剪接。我们详细分析了一个非常成功的人类特异性 SVA 5'转导组,因为它包含至少 32%的所有 SVA 亚家族 F 成员。一个古老的反转座事件将 SVA 插入物置于 MAST2 基因启动子的转录控制之下,产生了该组的原始源元件。该组的成员目前正在转录。在这里,我们表明 SVA 介导的 5'转导事件导致 SVA 元件的结构多样性,并代表导致基因组多样性的基因组重排的新来源。

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Exon-trapping mediated by the human retrotransposon SVA.由人类反转录转座子 SVA 介导的外显子捕获。
Genome Res. 2009 Nov;19(11):1983-91. doi: 10.1101/gr.093153.109. Epub 2009 Jul 27.
2
Active Alu retrotransposons in the human genome.人类基因组中的活跃Alu逆转座子。
Genome Res. 2008 Dec;18(12):1875-83. doi: 10.1101/gr.081737.108. Epub 2008 Oct 3.
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Mobile DNA elements in primate and human evolution.灵长类和人类进化中的移动DNA元件
Am J Phys Anthropol. 2007;Suppl 45:2-19. doi: 10.1002/ajpa.20722.
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Web services at the European bioinformatics institute.欧洲生物信息学研究所的网络服务。
Nucleic Acids Res. 2007 Jul;35(Web Server issue):W6-11. doi: 10.1093/nar/gkm291. Epub 2007 Jun 18.
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Which transposable elements are active in the human genome?哪些转座元件在人类基因组中是活跃的?
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