MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells

MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells

Abstract Background Bovine ephemeral fever virus (BEFV), the causative agent of bovine ephemeral fever, is an economically important pathogen of cattle and water buffalo. MicroRNAs (miRNAs) are endogenous 21-23 nt small non-coding RNA molecules that binding to a multiple of target mRNAs and function...

Full description

Bibliographic Details
Main Authors: Peili Hou, Hongmei Wang, Guimin Zhao, Guixue Hu, Xianzhu Xia, Hongbin He
Format: Article
Language:English
Published: BMC 2018-12-01
Series:BMC Microbiology
Subjects:
Bovine ephemeral fever virus (BEFV)
MiR-3470b
Mitochondrial antiviral signaling protein (MAVS)
Virus replication
Online Access:http://link.springer.com/article/10.1186/s12866-018-1366-6
id doaj-2dc527466f5045968b51f5486bbd56fc
record_format Article
spelling doaj-2dc527466f5045968b51f5486bbd56fc2020-11-25T00:26:52ZengBMCBMC Microbiology1471-21802018-12-0118111010.1186/s12866-018-1366-6MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cellsPeili Hou0Hongmei Wang1Guimin Zhao2Guixue Hu3Xianzhu Xia4Hongbin He5College of Animal Science and Technology, Jilin Agricultural UniversityKey Laboratory of Animal Resistant Biology of Shandong, Ruminant Diseases Research Center, College of Life Sciences, Shandong Normal UniversityKey Laboratory of Animal Resistant Biology of Shandong, Ruminant Diseases Research Center, College of Life Sciences, Shandong Normal UniversityCollege of Animal Science and Technology, Jilin Agricultural UniversityKey Laboratory of Jilin Province for Zoonosis Prevention and Control, Institute of Military Veterinary, Academy of Military Medical SciencesKey Laboratory of Animal Resistant Biology of Shandong, Ruminant Diseases Research Center, College of Life Sciences, Shandong Normal UniversityAbstract Background Bovine ephemeral fever virus (BEFV), the causative agent of bovine ephemeral fever, is an economically important pathogen of cattle and water buffalo. MicroRNAs (miRNAs) are endogenous 21-23 nt small non-coding RNA molecules that binding to a multiple of target mRNAs and functioning in the regulation of viral replication including the miRNA-mediated antiviral defense. However, the reciprocal interaction between bovine ephemeral fever virus replication and host miRNAs still remain poorly understood. The aim of our study herein was to investigate the exact function of miR-3470b and its molecular mechanisms during BEFV infection. Results In this study, we found a set of microRNAs induced by BEFV infection using small RNA deep sequencing, and further identified BEFV infection could significantly up-regulate the miR-3470b expression in Baby Hamster Syrian Kidney cells (BHK-21) after 24 h and 48 h post-infection (pi) compared to normal BHK-21 cells without BEFV infection. Additionally, the target association between miR-3470b and mitochondrial antiviral signaling protein (MAVS) was predicted by target gene prediction tools and further validated using a dual-luciferase reporter assay, and the expression of MAVS mRNA and protein levels was negatively associated with miR-3470b levels. Furthermore, the miR-3470b mimic transfection significantly contributed to increase the BEFV N mRNA, G protein level and viral titer, respectively, whereas the miR-3470b inhibitor had the opposite effect on BEFV replication. Moreover, the overexpression of MAVS or silencing of miR-3470b by its inhibitors suppressed BEFV replication, and knockdown of MAVS by small interfering RNA also promoted the replication of BEFV. Conclusions Our findings is the first to reveal that miR-3470b as a novel host factor regulates BEFV replication via directly targeting the MAVS gene in BHK-21 cells and may provide a potential strategy for developing effective antiviral therapy.http://link.springer.com/article/10.1186/s12866-018-1366-6Bovine ephemeral fever virus (BEFV)MiR-3470bMitochondrial antiviral signaling protein (MAVS)Virus replication
collection DOAJ
language English
format Article
sources DOAJ
author Peili Hou
Hongmei Wang
Guimin Zhao
Guixue Hu
Xianzhu Xia
Hongbin He
spellingShingle Peili Hou
Hongmei Wang
Guimin Zhao
Guixue Hu
Xianzhu Xia
Hongbin He
MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
BMC Microbiology
Bovine ephemeral fever virus (BEFV)
MiR-3470b
Mitochondrial antiviral signaling protein (MAVS)
Virus replication
author_facet Peili Hou
Hongmei Wang
Guimin Zhao
Guixue Hu
Xianzhu Xia
Hongbin He
author_sort Peili Hou
title MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
title_short MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
title_full MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
title_fullStr MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
title_full_unstemmed MiR-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (MAVS) in baby hamster Syrian kidney cells
title_sort mir-3470b promotes bovine ephemeral fever virus replication via directly targeting mitochondrial antiviral signaling protein (mavs) in baby hamster syrian kidney cells
publisher BMC
series BMC Microbiology
issn 1471-2180
publishDate 2018-12-01
description Abstract Background Bovine ephemeral fever virus (BEFV), the causative agent of bovine ephemeral fever, is an economically important pathogen of cattle and water buffalo. MicroRNAs (miRNAs) are endogenous 21-23 nt small non-coding RNA molecules that binding to a multiple of target mRNAs and functioning in the regulation of viral replication including the miRNA-mediated antiviral defense. However, the reciprocal interaction between bovine ephemeral fever virus replication and host miRNAs still remain poorly understood. The aim of our study herein was to investigate the exact function of miR-3470b and its molecular mechanisms during BEFV infection. Results In this study, we found a set of microRNAs induced by BEFV infection using small RNA deep sequencing, and further identified BEFV infection could significantly up-regulate the miR-3470b expression in Baby Hamster Syrian Kidney cells (BHK-21) after 24 h and 48 h post-infection (pi) compared to normal BHK-21 cells without BEFV infection. Additionally, the target association between miR-3470b and mitochondrial antiviral signaling protein (MAVS) was predicted by target gene prediction tools and further validated using a dual-luciferase reporter assay, and the expression of MAVS mRNA and protein levels was negatively associated with miR-3470b levels. Furthermore, the miR-3470b mimic transfection significantly contributed to increase the BEFV N mRNA, G protein level and viral titer, respectively, whereas the miR-3470b inhibitor had the opposite effect on BEFV replication. Moreover, the overexpression of MAVS or silencing of miR-3470b by its inhibitors suppressed BEFV replication, and knockdown of MAVS by small interfering RNA also promoted the replication of BEFV. Conclusions Our findings is the first to reveal that miR-3470b as a novel host factor regulates BEFV replication via directly targeting the MAVS gene in BHK-21 cells and may provide a potential strategy for developing effective antiviral therapy.
topic Bovine ephemeral fever virus (BEFV)
MiR-3470b
Mitochondrial antiviral signaling protein (MAVS)
Virus replication
url http://link.springer.com/article/10.1186/s12866-018-1366-6
work_keys_str_mv AT peilihou mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
AT hongmeiwang mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
AT guiminzhao mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
AT guixuehu mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
AT xianzhuxia mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
AT hongbinhe mir3470bpromotesbovineephemeralfevervirusreplicationviadirectlytargetingmitochondrialantiviralsignalingproteinmavsinbabyhamstersyriankidneycells
_version_ 1725342071876747264

Similar Items