A bovine respiratory syncytial virus model with high clinical expression in calves with specific passive immunity

被引:30
作者
Blodorn, Krister
Hagglund, Sara
Gavier-Widen, Dolores [1 ,2 ]
Eleouet, Jean-Francois [3 ]
Riffault, Sabine [3 ]
Pringle, John
Taylor, Geraldine [4 ]
Valarcher, Jean Francois [1 ,5 ]
机构
[1] Natl Vet Inst, Dept Pathol & Wildlife Dis, S-75007 Uppsala, Sweden
[2] Swedish Univ Agr Sci, Dept Biomed Sci & Vet Publ Hlth, Uppsala, Sweden
[3] INRA, Unite Virol & Immunol Mol, Jouy en Josas, France
[4] Pirbright Inst, Pirbright, Surrey, England
[5] Natl Vet Inst, Dept Virol, Immunol & Parasitol, S-75007 Uppsala, Sweden
基金
英国生物技术与生命科学研究理事会; 瑞典研究理事会;
关键词
Bovine respiratory syncytial virus; Experimental infection model; Calves; Maternal immunity; Aerosol; FORCED OSCILLATION TECHNIQUE; AGE-DEPENDENT DIFFERENCES; T-LYMPHOCYTE SUBSETS; EXPERIMENTAL-INFECTION; CELL RESPONSES; BRSV INFECTION; CALF PNEUMONIA; VACCINE; REPLICATION; PROTECTION;
D O I
10.1186/s12917-015-0389-6
中图分类号
S85 [动物医学(兽医学)];
学科分类号
0906 ;
摘要
Background: Bovine respiratory syncytial virus (BRSV) is a major cause of respiratory disease in cattle worldwide. Calves are particularly affected, even with low to moderate levels of BRSV-specific maternally derived antibodies (MDA). Available BRSV vaccines have suboptimal efficacy in calves with MDA, and published infection models in this target group are lacking in clinical expression. Here, we refine and characterize such a model. Results: In a first experiment, 2 groups of 3 calves with low levels of MDA were experimentally inoculated by inhalation of aerosolized BRSV, either: the Snook strain, passaged in gnotobiotic calves (BRSV-Snk), or isolate no. 9402022 Denmark, passaged in cell culture (BRSV-Dk). All calves developed clinical signs of respiratory disease and shed high titers of virus, but BRSV-Snk induced more severe disease, which was then reproduced in a second experiment in 5 calves with moderate levels of MDA. These 5 calves shed high titers of virus and developed severe clinical signs of disease and extensive macroscopic lung lesions (mean+/-SD, 48.3+/-12.0% of lung), with a pulmonary influx of inflammatory cells, characterized by interferon gamma secretion and a marked effect on lung function. Conclusions: We present a BRSV-infection model, with consistently high clinical expression in young calves with low to moderate levels of BRSV-specific MDA, that may prove useful in studies into disease pathogenesis, or evaluations of vaccines and antivirals. Additionally, refined tools to assess the outcome of BRSV infection are described, including passive measurement of lung function and a refined system to score clinical signs of disease. Using this cognate host calf model might also provide answers to elusive questions about human RSV (HRSV), a major cause of morbidity in children worldwide.
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页数:14
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