| Literature DB >> 30956044 |
Tania Sultana1, Dominic van Essen1, Oliver Siol2, Marc Bailly-Bechet3, Claude Philippe1, Amal Zine El Aabidine4, Léo Pioger4, Pilvi Nigumann1, Simona Saccani1, Jean-Christophe Andrau4, Nicolas Gilbert5, Gael Cristofari6.
Abstract
L1 retrotransposons are transposable elements and major contributors of genetic variation in humans. Where L1 integrates into the genome can directly impact human evolution and disease. Here, we experimentally induced L1 retrotransposition in cells and mapped integration sites at nucleotide resolution. At local scales, L1 integration is mostly restricted by genome sequence biases and the specificity of the L1 machinery. At regional scales, L1 shows a broad capacity for integration into all chromatin states, in contrast to other known mobile genetic elements. However, integration is influenced by the replication timing of target regions, suggesting a link to host DNA replication. The distribution of new L1 integrations differs from those of preexisting L1 copies, which are significantly reshaped by natural selection. Our findings reveal that the L1 machinery has evolved to efficiently target all genomic regions and underline a predominant role for post-integrative processes on the distribution of endogenous L1 elements.Entities:
Keywords: LINE-1; LINE1; insertion; integration; mobile genetic element; retrotransposition; retrotransposon; transposable elements; transposition; transposon
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Year: 2019 PMID: 30956044 DOI: 10.1016/j.molcel.2019.02.036
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970