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An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
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An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
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An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility

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An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility
Paper

An endogenous retroviral element co-opts an upstream regulatory sequence to achieve somatic expression and mobility

2025
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Overview
Retrotransposons, multi-copy sequences that propagate via copy-and-paste mechanisms involving an RNA intermediate, occupy large portions of all eukaryotic genomes. A great majority of their manifold copies remain silenced in somatic cells, nevertheless, some are transcribed, often in a tissue specific manner, and a small fraction retains its ability to mobilize. Retrotransposon expression or mobility are increasingly recognized to contribute to normal development and tissue homeostasis, as well as to aging and disease. While it is well characterized that retrotransposon sequences may provide cis regulatory elements for neighboring genes, how their own expression and mobility are achieved in different somatic contexts is not well understood. Here, using long-read DNA sequencing, we characterize somatic retrotransposition in the Drosophila intestine. We show that retroelement mobility does not change significantly upon aging and is limited to very few active sub-families of retrotransposons. Importantly, we identify a polymorphic donor locus of an endogenous LTR retroviral element rover, active in the intestinal tissue. We reveal that gut activity of the rover donor copy depends on its genomic environment. Without affecting local gene expression, the copy co-opts its upstream enhancer sequence, rich in transcription factor binding sites, for somatic expression. Further we show that escargot, a snail-type transcription factor critical for gut progenitor cell function, can drive transcriptional activity of the active rover copy. These data provide new insights into how locus-specific features allow active retrotransposons to produce functional transcripts and mobilize in a somatic lineage.Competing Interest StatementThe authors have declared no competing interest.