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Widespread roles of enhancer-like transposable elements in cell identity and long-range genomic interactions.


ABSTRACT: A few families of transposable elements (TEs) have been shown to evolve into cis-regulatory elements (CREs). Here, to extend these studies to all classes of TEs in the human genome, we identified widespread enhancer-like repeats (ELRs) and find that ELRs reliably mark cell identities, are enriched for lineage-specific master transcription factor binding sites, and are mostly primate-specific. In particular, elements of MIR and L2 TE families whose abundance co-evolved across chordate genomes, are found as ELRs in most human cell types examined. MIR and L2 elements frequently share long-range intra-chromosomal interactions and binding of physically interacting transcription factors. We validated that eight L2 and nine MIR elements function as enhancers in reporter assays, and among 20 MIR-L2 pairings, one MIR repressed and one boosted the enhancer activity of L2 elements. Our results reveal a previously unappreciated co-evolution and interaction between two TE families in shaping regulatory networks.

SUBMITTER: Cao Y 

PROVIDER: S-EPMC6314169 | biostudies-literature | 2019 Jan

REPOSITORIES: biostudies-literature

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Widespread roles of enhancer-like transposable elements in cell identity and long-range genomic interactions.

Cao Yaqiang Y   Chen Guoyu G   Wu Gang G   Zhang Xiaoli X   McDermott Joseph J   Chen Xingwei X   Xu Chi C   Jiang Quanlong Q   Chen Zhaoxiong Z   Zeng Yingying Y   Ai Daosheng D   Huang Yi Y   Han Jing-Dong J JJ  

Genome research 20181119 1


A few families of transposable elements (TEs) have been shown to evolve into <i>cis</i>-regulatory elements (CREs). Here, to extend these studies to all classes of TEs in the human genome, we identified widespread enhancer-like repeats (ELRs) and find that ELRs reliably mark cell identities, are enriched for lineage-specific master transcription factor binding sites, and are mostly primate-specific. In particular, elements of MIR and L2 TE families whose abundance co-evolved across chordate geno  ...[more]

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