miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA

The majority of the human genome is made of transposable elements, giving rise to interspaced repeats, including Long INterspersed Element-1s (LINE-1s or L1s). L1s are active human transposable elements involved in genomic diversity and evolution; however, they can also contribute to genomic instabi...

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Autores principales: Fung, Lianna, Guzman, Herlinda, Sevrioukov, Evgueni, Idica, Adam, Park, Eddie, Bochnakian, Aurore, Daugaard, Iben, Jury, Douglas, Mortazavi, Ali, Zisoulis, Dimitrios G., Pedersen, Irene M.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2019
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6515209/
https://www.ncbi.nlm.nih.gov/pubmed/31010097
http://dx.doi.org/10.3390/ijms20081955
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author Fung, Lianna
Guzman, Herlinda
Sevrioukov, Evgueni
Idica, Adam
Park, Eddie
Bochnakian, Aurore
Daugaard, Iben
Jury, Douglas
Mortazavi, Ali
Zisoulis, Dimitrios G.
Pedersen, Irene M.
author_facet Fung, Lianna
Guzman, Herlinda
Sevrioukov, Evgueni
Idica, Adam
Park, Eddie
Bochnakian, Aurore
Daugaard, Iben
Jury, Douglas
Mortazavi, Ali
Zisoulis, Dimitrios G.
Pedersen, Irene M.
author_sort Fung, Lianna
collection PubMed
description The majority of the human genome is made of transposable elements, giving rise to interspaced repeats, including Long INterspersed Element-1s (LINE-1s or L1s). L1s are active human transposable elements involved in genomic diversity and evolution; however, they can also contribute to genomic instability and diseases. L1s require host factors to complete their life cycles, whereas the host has evolved numerous mechanisms to restrict L1-induced mutagenesis. Restriction mechanisms in somatic cells include methylation of the L1 promoter, anti-viral factors and RNA-mediated processes such as small RNAs. microRNAs (miRNAs or miRs) are small non-coding RNAs that post-transcriptionally repress multiple target genes often found in the same cellular pathways. We have recently established that miR-128 functions as a novel restriction factor inhibiting L1 mobilization in somatic cells. We have further demonstrated that miR-128 functions through a dual mechanism; by directly targeting L1 RNA for degradation and indirectly by inhibiting a cellular co-factor which L1 is dependent on to transpose to new genomic locations (TNPO1). Here, we add another piece to the puzzle of the enigmatic L1 lifecycle. We show that miR-128 also inhibits another key cellular factor, hnRNPA1 (heterogeneous nuclear ribonucleoprotein A1), by significantly reducing mRNA and protein levels through direct interaction with the coding sequence (CDS) of hnRNPA1 mRNA. In addition, we demonstrate that repression of hnRNPA1 using hnRNPA1-shRNA significantly decreases de novo L1 retro-transposition and that induced hnRNPA1 expression enhances L1 mobilization. Furthermore, we establish that hnRNPA1 is a functional target of miR-128. Finally, we determine that induced hnRNPA1 expression in miR-128-overexpressing cells can partly rescue the miR-128-induced repression of L1′s ability to transpose to different genomic locations. Thus, we have identified an additional mechanism by which miR-128 represses L1 retro-transposition and mediates genomic stability.
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spelling pubmed-65152092019-05-30 miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA Fung, Lianna Guzman, Herlinda Sevrioukov, Evgueni Idica, Adam Park, Eddie Bochnakian, Aurore Daugaard, Iben Jury, Douglas Mortazavi, Ali Zisoulis, Dimitrios G. Pedersen, Irene M. Int J Mol Sci Article The majority of the human genome is made of transposable elements, giving rise to interspaced repeats, including Long INterspersed Element-1s (LINE-1s or L1s). L1s are active human transposable elements involved in genomic diversity and evolution; however, they can also contribute to genomic instability and diseases. L1s require host factors to complete their life cycles, whereas the host has evolved numerous mechanisms to restrict L1-induced mutagenesis. Restriction mechanisms in somatic cells include methylation of the L1 promoter, anti-viral factors and RNA-mediated processes such as small RNAs. microRNAs (miRNAs or miRs) are small non-coding RNAs that post-transcriptionally repress multiple target genes often found in the same cellular pathways. We have recently established that miR-128 functions as a novel restriction factor inhibiting L1 mobilization in somatic cells. We have further demonstrated that miR-128 functions through a dual mechanism; by directly targeting L1 RNA for degradation and indirectly by inhibiting a cellular co-factor which L1 is dependent on to transpose to new genomic locations (TNPO1). Here, we add another piece to the puzzle of the enigmatic L1 lifecycle. We show that miR-128 also inhibits another key cellular factor, hnRNPA1 (heterogeneous nuclear ribonucleoprotein A1), by significantly reducing mRNA and protein levels through direct interaction with the coding sequence (CDS) of hnRNPA1 mRNA. In addition, we demonstrate that repression of hnRNPA1 using hnRNPA1-shRNA significantly decreases de novo L1 retro-transposition and that induced hnRNPA1 expression enhances L1 mobilization. Furthermore, we establish that hnRNPA1 is a functional target of miR-128. Finally, we determine that induced hnRNPA1 expression in miR-128-overexpressing cells can partly rescue the miR-128-induced repression of L1′s ability to transpose to different genomic locations. Thus, we have identified an additional mechanism by which miR-128 represses L1 retro-transposition and mediates genomic stability. MDPI 2019-04-21 /pmc/articles/PMC6515209/ /pubmed/31010097 http://dx.doi.org/10.3390/ijms20081955 Text en © 2019 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Fung, Lianna
Guzman, Herlinda
Sevrioukov, Evgueni
Idica, Adam
Park, Eddie
Bochnakian, Aurore
Daugaard, Iben
Jury, Douglas
Mortazavi, Ali
Zisoulis, Dimitrios G.
Pedersen, Irene M.
miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title_full miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title_fullStr miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title_full_unstemmed miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title_short miR-128 Restriction of LINE-1 (L1) Retrotransposition Is Dependent on Targeting hnRNPA1 mRNA
title_sort mir-128 restriction of line-1 (l1) retrotransposition is dependent on targeting hnrnpa1 mrna
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6515209/
https://www.ncbi.nlm.nih.gov/pubmed/31010097
http://dx.doi.org/10.3390/ijms20081955
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