The MOV10 RNA helicase is a dosage-dependent host restriction factor for LINE1 retrotransposition in mice

Guan, Yongjuan; Gao, Hongyan; Leu, N. Adrian; Vourekas, Anastassios; Alexiou, Panagiotis; Maragkakis, Manolis; Kang, Zhenlong; Mourelatos, Zissimos P.; Liang, Guanxiang; Wang, P. Jeremy

doi:10.1371/journal.pgen.1010566

Cited by 4 publications

(2 citation statements)

References 67 publications

(101 reference statements)

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“…Depending on the genomic and environmental contexts, genetic variation favoring one or the other primary siRNA pathway could have been selected [39][40][41][42] . Research in mammals has shown the importance of dosage of the orthologous MOV10 helicase on retrovirus silencing 43 . We showed here that natural structural variants at the eri-6/7 locus were a major driver of variation in ERGO-1 pathway activity and mRNA levels of its downstream regulated showing the most divergent eri-6/7 region based on SNVs (Fig.…”

Section: Phenotypic Effect Of the Structural Variation At Eri-6/7 On ...mentioning

confidence: 99%

Transposon-mediated genic rearrangements underlie variation in small RNA pathways

Zhang,

Félix,

Andersen

2024

Preprint

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Transposable elements (TEs) are parasitic DNA sequences that insert into the host genome and can cause alterations in host gene structure and expression. Host organisms cope with the often detrimental consequences caused by recent transposition and develop mechanisms that repress TE activities. In the nematode Caenorhabditis elegans, a small interfering RNA (siRNA) pathway dependent on the helicase ERI-6/7 primarily silences long terminal repeat retrotransposons and recent genes of likely viral origin. By studying gene expression variation among wild C. elegans strains, we discovered that structural variants and transposon remnants at the eri-6/7 locus alter its expression in cis and underlie a trans-acting expression quantitative trait locus affecting non-conserved genes and pseudogenes. Multiple insertions of the Polinton DNA transposon (also known as Mavericks) reshuffled the eri-6/7 locus in different configurations, separating the eri-6 and eri-7 exons and causing the inversion of eri-6 as seen in the reference N2 genome. In the inverted configuration, gene function was previously shown to be repaired by unusual trans-splicing mediated by direct repeats flanking the inversion. We show that these direct repeats originated from terminal inverted repeats specific to C. elegans Polintons. This trans-splicing event occurs infrequently compared to cis-splicing to novel downstream exons, thus affecting the production of ERI-6/7. Diverse Polinton-induced structural variations display regulatory effects within the locus and on targets of ERI-6/7-dependent siRNA pathways. Our findings highlight the role of host-transposon interactions in driving rapid host genome diversification among natural populations and shed light on evolutionary novelty in genes and splicing mechanisms.

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Section: Phenotypic Effect Of the Structural Variation At Eri-6/7 On ...mentioning

confidence: 99%

Transposon-mediated genic rearrangements underlie variation in small RNA pathways

Zhang,

Félix,

Andersen

2024

Preprint

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“…In addition, a recent investigation has shown for the first time that Drosophila Fragile X protein is necessary for transposon inactivation in the larval and adult brains of Drosophila "loss of function" dFmr1 mutants [ 65 ]. Results from a study also show that the RNA helicase MOV10 inhibits LINE1 retrotransposition in mice in a dosage-dependent way [ 89 ].…”

Section: Mechanisms Of Transposable Elements Silencingmentioning

confidence: 99%

Transposable elements as essential elements in the control of gene expression

Gebrie

2023

Mobile DNA

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Interspersed repetitions called transposable elements (TEs), commonly referred to as mobile elements, make up a significant portion of the genomes of higher animals. TEs contribute in controlling the expression of genes locally and even far away at the transcriptional and post-transcriptional levels, which is one of their significant functional effects on gene function and genome evolution. There are different mechanisms through which TEs control the expression of genes. First, TEs offer cis-regulatory regions in the genome with their inherent regulatory features for their own expression, making them potential factors for controlling the expression of the host genes. Promoter and enhancer elements contain cis-regulatory sites generated from TE, which function as binding sites for a variety of trans-acting factors. Second, a significant portion of miRNAs and long non-coding RNAs (lncRNAs) have been shown to have TEs that encode for regulatory RNAs, revealing the TE origin of these RNAs. Furthermore, it was shown that TE sequences are essential for these RNAs' regulatory actions, which include binding to the target mRNA. By being a member of cis-regulatory and regulatory RNA sequences, TEs therefore play essential regulatory roles. Additionally, it has been suggested that TE-derived regulatory RNAs and cis-regulatory regions both contribute to the evolutionary novelty of gene regulation. Additionally, these regulatory systems arising from TE frequently have tissue-specific functions. The objective of this review is to discuss TE-mediated gene regulation, with a particular emphasis on the processes, contributions of various TE types, differential roles of various tissue types, based mostly on recent studies on humans.

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Transposon-mediated genic rearrangements underlie variation in small RNA pathways

Zhang,

Félix,

Andersen

2024

Sci. Adv.

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Transposable elements (TEs) can alter host gene structure and expression, whereas host organisms develop mechanisms to repress TE activities. In the nematode Caenorhabditis elegans , a small interfering RNA pathway dependent on the helicase ERI-6/7 primarily silences retrotransposons and recent genes of likely viral origin. By studying gene expression variation among wild C. elegans strains, we found that structural variants and transposon remnants likely underlie expression variation in eri-6/7 and the pathway targets. We further found that multiple insertions of the DNA transposons, Polintons, reshuffled the eri-6/7 locus and induced inversion of eri-6 in some wild strains. In the inverted configuration, gene function was previously shown to be repaired by unusual trans-splicing mediated by direct repeats. We identified that these direct repeats originated from terminal inverted repeats of Polintons . Our findings highlight the role of host-transposon interactions in driving rapid host genome diversification among natural populations and shed light on evolutionary novelty in genes and splicing mechanisms.

show abstract

The MOV10 RNA helicase is a dosage-dependent host restriction factor for LINE1 retrotransposition in mice

Cited by 4 publications

References 67 publications

Transposon-mediated genic rearrangements underlie variation in small RNA pathways

Transposon-mediated genic rearrangements underlie variation in small RNA pathways

Transposable elements as essential elements in the control of gene expression

Transposon-mediated genic rearrangements underlie variation in small RNA pathways

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