Research article - Peer-reviewed, 2020
Model of persistent foot-and-mouth disease virus infection in multilayered cells derived from bovine dorsal soft palate
Hagglund, Sara; Laloy, Eve; Naslund, Katarina; Pfaff, Florian; Eschbaumer, Michael; Romey, Aurore; Relmy, Anthony; Rikberg, Annika; Svensson, Anna; Huet, Helene; Gorna, Kamila; Zuehlke, Daniela; Riedel, Katharina; Beer, Martin; Zientara, Stephan; Bakkali-Kassimi, Labib; Blaise-Boisseau, Sandra; Valarcher, Jean FrancoisAbstract
Foot-and-mouth disease virus (FMDV) causes a highly contagious vesicular disease in livestock, with serious consequences for international trade. The virus persists in the nasopharynx of cattle and this slows down the process to obtain an FMDV-free status after an outbreak. To study biological mechanisms, or to identify molecules that can be targeted to diagnose or interfere with persistence, we developed a model of persistent FMDV infection in bovine dorsal soft palate (DSP). Primary DSP cells were isolated after commercial slaughter and were cultured in multilayers at the air-liquid interface. After 5 weeks of culture without further passage, the cells were infected with FMDV strain O/FRA/1/2001. Approximately, 20% of cells still had a polygonal morphology and displayed tight junctions as in stratified squamous epithelia. Subsets of cells expressed cytokeratin and most or all cells expressed vimentin. In contrast to monolayers in medium, multilayers in air demonstrated only a limited cytopathic effect. Integrin alpha(V)beta(6) expression was observed in mono- but not in multilayers. FMDV antigen, FMDV RNA and live virus were detected from day 1 to 28, with peaks at day 1 and 2. The proportion of infected cells was highest at 24 hr (3% and 36% of cells at an MOI of 0.01 and 1, respectively). At day 28 after infection, at a time when animals that still harbour FMDV are considered carriers, FMDV antigen was detected in 0.2%-2.1% of cells, in all layers, and live virus was isolated from supernatants of 6/8 cultures. On the consensus level, the viral genome did not change within the first 24 hr after infection. Only a few minor single nucleotide variants were detected, giving no indication of the presence of a viral quasispecies. The air-liquid interface model of DSP brings new possibilities to investigate FMDV persistence in a controlled manner.Keywords
air-liquid interface models; bovine dorsal soft palate; cattle; epithelial cells; foot-and-mouth disease virus; persistencePublished in
Transboundary and Emerging Diseases2020, volume: 67, number: 1, pages: 133-148
Publisher: WILEY
Authors' information
Swedish University of Agricultural Sciences, Department of Clinical Sciences
Laloy, Eve
Agence Nationale de Securite Sanitaire de lAlimentation, de lEnvironnement du Travail (ANSES)
Näslund, Katarina
Swedish University of Agricultural Sciences, Department of Clinical Sciences
Pfaff, Florian
Friedrich Loeffler Institute
Eschbaumer, Michael
Friedrich Loeffler Institute
Romey, Aurore
Ecole Nationale Veterinaire d'Alfort (ENVA)
Relmy, Anthony
Ecole Nationale Veterinaire d'Alfort (ENVA)
Swedish University of Agricultural Sciences, Department of Clinical Sciences
Swedish University of Agricultural Sciences, Department of Clinical Sciences
Huet, Helene
Ecole Nationale Veterinaire d'Alfort (ENVA)
Gorna, Kamila
Agence Nationale de Securite Sanitaire de lAlimentation, de lEnvironnement du Travail (ANSES)
Zuehlke, Daniela
Ernst Moritz Arndt Universitat Greifswald
Riedel, Katharina
Ernst Moritz Arndt Universitat Greifswald
Beer, Martin
Friedrich Loeffler Institute
Zientara, Stephan
Ecole Nationale Veterinaire d'Alfort (ENVA)
Bakkali-Kassimi, Labib
Ecole Nationale Veterinaire d'Alfort (ENVA)
Blaise-Boisseau, Sandra
Ecole Nationale Veterinaire d'Alfort (ENVA)
Swedish University of Agricultural Sciences, Department of Clinical Sciences
UKÄ Subject classification
Clinical Science
Publication Identifiers
DOI: https://doi.org/10.1111/tbed.13332
URI (permanent link to this page)
https://res.slu.se/id/publ/104355