Literature DB >> 27715458

Alternative splicing of a viral mirtron differentially affects the expression of other microRNAs from its cluster and of the host transcript.

Perrine Rasschaert1, Thomas Figueroa1, Ginette Dambrine1, Denis Rasschaert1, Sylvie Laurent1,2.   

Abstract

Interplay between alternative splicing and the Microprocessor may have differential effects on the expression of intronic miRNAs organized into clusters. We used a viral model - the LAT long non-coding RNA (LAT lncRNA) of Marek's disease oncogenic herpesvirus (MDV-1), which has the mdv1-miR-M8-M6-M7-M10 cluster embedded in its first intron - to assess the impact of splicing modifications on the biogenesis of each of the miRNAs from the cluster. Drosha silencing and alternative splicing of an extended exon 2 of the LAT lncRNA from a newly identified 3' splice site (SS) at the end of the second miRNA of the cluster showed that mdv1-miR-M6 was a 5'-tailed mirtron. We have thus identified the first 5'-tailed mirtron within a cluster of miRNAs for which alternative splicing is directly associated with differential expression of the other miRNAs of the cluster, with an increase in intronic mdv1-miR-M8 expression and a decrease in expression of the exonic mdv1-miR-M7, and indirectly associated with regulation of the host transcript. According to the alternative 3SS used for the host intron splicing, the mdv1-miR-M6 is processed as a mirtron by the spliceosome, dispatching the other miRNAs of the cluster into intron and exon, or as a canonical miRNA by the Microprocessor complex. The viral mdv1-miR-M6 mirtron is the first mirtron described that can also follow the canonical pathway.

Entities:  

Keywords:  Cluster of microRNAs; Marek's disease virus; long non-coding RNA; mirtron; splicing

Mesh:

Substances:

Year:  2016        PMID: 27715458      PMCID: PMC5207378          DOI: 10.1080/15476286.2016.1244600

Source DB:  PubMed          Journal:  RNA Biol        ISSN: 1547-6286            Impact factor:   4.652


  36 in total

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5.  Transcriptome-wide N6-methyladenosine modification profiling of long non-coding RNAs during replication of Marek's disease virus in vitro.

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6.  Epigenetic Silencing of MicroRNA-126 Promotes Cell Growth in Marek's Disease.

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