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Reading the tea leaves: Dead transposon copies reveal novel host and transposon biology

机译:阅读茶叶:死亡的转座子副本揭示了新颖的寄主和转座子生物学

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Transposable elements comprise a huge portion of most animal genomes. Unlike many pathogens, these elements leave a mark of their impact via their insertion into host genomes. With proper teasing, these sequences can relay information about the evolutionary history of transposons and their hosts. In a new publication, Larson and colleagues describe a previously unappreciated density of long interspersed element-1 (LINE-1) sequences that have been spliced (LINE-1 and other reverse transcribing elements are necessarily intronless). They provide data to suggest that the retention of these potentially deleterious splice sites in LINE-1 results from the sites’ overlap with an important transcription factor binding site. These spliced LINE-1s (i.e., spliced integrated retrotransposed elements [SpiREs]) lose their ability to replicate, suggesting they are evolutionary dead ends. However, the lethality of this splicing could be an efficient means of blocking continued replication of LINE-1. In this way, the record of inactive LINE-1 sequences in the human genome revealed a new, though infrequent, event in the LINE-1 replication cycle and motivates future studies to test whether splicing might be another weapon in the anti-LINE-1 arsenal of host genomes.
机译:转座因子占大多数动物基因组的很大一部分。与许多病原体不同,这些元素通过插入宿主基因组而留下了影响的印记。通过适当的戏弄,这些序列可以传递有关转座子及其宿主进化史的信息。在新的出版物中,Larson及其同事描述了以前拼接的长的散布的element-1(LINE-1)序列以前未曾意识到的密度(LINE-1和其他反转录元素必须是无内含子的)。他们提供的数据表明,这些潜在的有害剪接位点在LINE-1中的保留是由于这些位点与重要的转录因子结合位点重叠而导致的。这些拼接的LINE-1(即拼接的整合逆转座子[SpiRE])失去了复制能力,表明它们是进化的死胡同。但是,这种剪接的杀伤力可能是阻止LINE-1继续复制的有效手段。这样,人类基因组中无活性的LINE-1序列的记录揭示了LINE-1复制周期中的一个新事件,尽管很少发生,并激发了未来的研究以测试剪接是否可能是抗LINE-1的另一种武器宿主基因组库。

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