Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection

Abstract Background MicroRNAs (miRNAs) control multiple biological processes including the innate immune responses by negative post-transcriptional regulation of gene expression. As there were no studies on the role(s) of miRNAs in viral diseases in Atlantic salmon, we aimed to identify miRNAs respo...

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Main Authors: Rune Andreassen, Nardos Tesfaye Woldemariam, Ine Østråt Egeland, Oleg Agafonov, Hilde Sindre, Bjørn Høyheim
Format: Article
Language:English
Published: BMC 2017-05-01
Series:BMC Genomics
Subjects:
Online Access:http://link.springer.com/article/10.1186/s12864-017-3741-3
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author Rune Andreassen
Nardos Tesfaye Woldemariam
Ine Østråt Egeland
Oleg Agafonov
Hilde Sindre
Bjørn Høyheim
author_facet Rune Andreassen
Nardos Tesfaye Woldemariam
Ine Østråt Egeland
Oleg Agafonov
Hilde Sindre
Bjørn Høyheim
author_sort Rune Andreassen
collection DOAJ
description Abstract Background MicroRNAs (miRNAs) control multiple biological processes including the innate immune responses by negative post-transcriptional regulation of gene expression. As there were no studies on the role(s) of miRNAs in viral diseases in Atlantic salmon, we aimed to identify miRNAs responding to salmonid alphavirus (SAV) infection. Their expression were studied at different time points post infection with SAV isolates associated with different mortalities. Furthermore, the genome sequences of the identified miRNAs were analysed to reveal putative cis-regulatory elements, and, finally, their putative target genes were predicted. Results Twenty differentially expressed miRNAs (DE miRNAs) were identified. The expression of the majority of these increased post infection with maximum levels reached after the viral load were stabilized or decreasing. On the other hand, some miRNAs (e.g. the miRNA-21 family) showed decreased expression at the early time points post infection. There were significant differences in the temporal expression of individual miRNA associated with different SAV isolates. Target gene prediction in SAV responsive immune network genes showed that seventeen of the DE miRNAs could target 24 genes (e.g. IRF3, IRF7). Applying the Atlantic salmon transcriptome as input 28 more immune network genes were revealed as putative targets (e.g. IRF5, IRF4). The majority of the predicted target genes promote inflammatory response. The upstream sequences of the miRNA genes revealed a high density of cis-regulatory sequences known as binding sites for immune network transcription factors (TFs). A high expression in the late phase could therefore be due to increased transcription promoted by immune response activated TFs. Based on the in silico target predictions, we discuss their putative roles as early promotors or late inhibitors of inflammation. We propose that the differences in expressions associated with different SAV isolates could contribute to their differences in mortality rates. Conclusions This study represents the first steps in exploring miRNAs important in viral-host interaction in Atlantic salmon. We identified several miRNAs responding to SAV infection. Some likely to prohibit harmful inflammation while other may promote an early immune response. Their predicted functions need to be validated and further studied in functional assays to fully understand their roles in immune homeostasis.
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spelling doaj.art-e3603a2c2100485aad70ffc5a710a3f42022-12-22T02:41:30ZengBMCBMC Genomics1471-21642017-05-0118111910.1186/s12864-017-3741-3Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infectionRune Andreassen0Nardos Tesfaye Woldemariam1Ine Østråt Egeland2Oleg Agafonov3Hilde Sindre4Bjørn Høyheim5Department of Pharmacy and Biomedical and Laboratory Sciences, Faculty of Health Sciences, Oslo and Akershus University College of Applied SciencesDepartment of Pharmacy and Biomedical and Laboratory Sciences, Faculty of Health Sciences, Oslo and Akershus University College of Applied SciencesDepartment of Pharmacy and Biomedical and Laboratory Sciences, Faculty of Health Sciences, Oslo and Akershus University College of Applied SciencesBioinformatics Core Facility, Department of Core Facilities, Institute of Cancer Research, Radium hospital, part of Oslo University HospitalNorwegian Veterinary InstituteDepartment of Basic Sciences and Aquatic Medicine, School of Veterinary Medicine, Norwegian University of Life SciencesAbstract Background MicroRNAs (miRNAs) control multiple biological processes including the innate immune responses by negative post-transcriptional regulation of gene expression. As there were no studies on the role(s) of miRNAs in viral diseases in Atlantic salmon, we aimed to identify miRNAs responding to salmonid alphavirus (SAV) infection. Their expression were studied at different time points post infection with SAV isolates associated with different mortalities. Furthermore, the genome sequences of the identified miRNAs were analysed to reveal putative cis-regulatory elements, and, finally, their putative target genes were predicted. Results Twenty differentially expressed miRNAs (DE miRNAs) were identified. The expression of the majority of these increased post infection with maximum levels reached after the viral load were stabilized or decreasing. On the other hand, some miRNAs (e.g. the miRNA-21 family) showed decreased expression at the early time points post infection. There were significant differences in the temporal expression of individual miRNA associated with different SAV isolates. Target gene prediction in SAV responsive immune network genes showed that seventeen of the DE miRNAs could target 24 genes (e.g. IRF3, IRF7). Applying the Atlantic salmon transcriptome as input 28 more immune network genes were revealed as putative targets (e.g. IRF5, IRF4). The majority of the predicted target genes promote inflammatory response. The upstream sequences of the miRNA genes revealed a high density of cis-regulatory sequences known as binding sites for immune network transcription factors (TFs). A high expression in the late phase could therefore be due to increased transcription promoted by immune response activated TFs. Based on the in silico target predictions, we discuss their putative roles as early promotors or late inhibitors of inflammation. We propose that the differences in expressions associated with different SAV isolates could contribute to their differences in mortality rates. Conclusions This study represents the first steps in exploring miRNAs important in viral-host interaction in Atlantic salmon. We identified several miRNAs responding to SAV infection. Some likely to prohibit harmful inflammation while other may promote an early immune response. Their predicted functions need to be validated and further studied in functional assays to fully understand their roles in immune homeostasis.http://link.springer.com/article/10.1186/s12864-017-3741-3miRNAVirusAtlantic salmonInnate immune response
spellingShingle Rune Andreassen
Nardos Tesfaye Woldemariam
Ine Østråt Egeland
Oleg Agafonov
Hilde Sindre
Bjørn Høyheim
Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
BMC Genomics
miRNA
Virus
Atlantic salmon
Innate immune response
title Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
title_full Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
title_fullStr Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
title_full_unstemmed Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
title_short Identification of differentially expressed Atlantic salmon miRNAs responding to salmonid alphavirus (SAV) infection
title_sort identification of differentially expressed atlantic salmon mirnas responding to salmonid alphavirus sav infection
topic miRNA
Virus
Atlantic salmon
Innate immune response
url http://link.springer.com/article/10.1186/s12864-017-3741-3
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