Author:
de Carvalho Otávio Valério,Rebouças Santos Marcus,Lopes Rangel Fietto Juliana,Pires Moraes Mauro,de Almeida Márcia Rogéria,Costa Bressan Gustavo,José Pena Lindomar,Silva-Júnior Abelardo
Abstract
Abstract
Background
Canine morbilivirus (canine distemper virus, CDV) is a highly contagious pathogen associated with high morbidity and mortality in susceptible carnivores. Although there are CDV vaccines available, the disease poses a huge threat to dogs and wildlife hosts due to vaccine failures and lack of effective treatment. Thus, the development of therapeutics is an urgent need to achieve rapid outbreak control and reduce mortality in target species. Gene silencing by RNA interference has emerged as a promising therapeutic approach against different human and animal viruses. In this study, plasmid-based short hairpin RNAs (shRNAs) against three different regions in either CDV nucleoprotein (N), or large polymerase (L) genes and recombinant adenovirus-expressing N-specific multi-shRNAs were generated. Viral cytopathic effect, virus titration, plaque-forming unit reduction, and real-time quantitative RT-PCR analysis were used to check the efficiency of constructs against CDV.
Results
In CDV-infected VerodogSLAM cells, shRNA-expressing plasmids targeting the N gene markedly inhibited the CDV replication in a dose-dependent manner, with viral genomes and titers being decreased by over 99%. Transfection of plasmid-based shRNAs against the L gene displayed weaker inhibition of viral RNA level and virus yield as compared to CDV N shRNAs. A combination of shRNAs targeting three sites in the N gene considerably reduced CDV RNA and viral titers, but their effect was not synergistic. Recombinant adenovirus-expressing multiple shRNAs against CDV N gene achieved a highly efficient knockdown of CDV N mRNAs and successful inhibition of CDV replication.
Conclusions
We found that this strategy had strong silencing effects on CDV replication in vitro. Our findings indicate that the delivery of shRNAs using plasmid or adenovirus vectors potently inhibits CDV replication and provides a basis for the development of therapeutic strategies for clinical trials.
Funder
Conselho Nacional de Desenvolvimento Científico e Tecnológico
Coordenação de Aperfeiçoamento de Pessoal de Nível Superior
Publisher
Springer Science and Business Media LLC
Subject
General Veterinary,General Medicine
Reference59 articles.
1. Deem SL, Spelman LH, Yates RA, Montali RJ. Canine distemper in terrestrial carnivores: a review. J Zoo Wildl Med. 2000;31:441–51. https://doi.org/10.1638/1042-7260(2000)031[0441:CDITCA]2.0.CO;2.
2. Maes P, Amarasinghe GK, Ayllón MA, Basler CF, Bavari S. Taxonomy of the order Mononegavirales: second update 2018. Arch Virol. 2019;164:1233–44. https://doi.org/10.1007/s00705-018-04126-4.
3. Appel MJG, Summers BA. Canine distemper: current status. In: Recent advances in infectious diseases. In: Carmichael, L.E, editor. Recent advances in canine infectious diseases. Ithaca: International Veterinary Information Service; 1999.
4. Nagao Y, Nishio Y, Shiomoda H, Tamaru S, Shimojima M, Goto M, et al. An outbreak of canine distemper virus in tigers (Panthera tigris): possible transmission from wild animals to zoo animals. J Vet Med Sci. 2011;74:699–705.
5. Origgi FC, Plattet P, Sattler U, Robert N, Casaubon J, Mavrot F, et al. Emergence of canine distemper virus strains with modified molecular signature and enhanced neuronal tropism leading to high mortality in wild carnivores. Vet Pathol. 2012;49:913–29.
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