Author: Hao, Xinâ€yan; Lv, Qi; Li, Fengâ€di; Xu, Yanâ€feng; Gao, Hong
Title: The characteristics of hDPP4 transgenic mice subjected to aerosol MERS coronavirus infection via an animal noseâ€only exposure device Cord-id: vkjcheaz Document date: 2019_10_30
ID: vkjcheaz
Snippet: BACKGROUND: Middle East respiratory syndrome coronavirus (MERSâ€CoV), which is not fully understood in regard to certain transmission routes and pathogenesis and lacks specific therapeutics and vaccines, poses a global threat to public health. METHODS: To simulate the clinical aerosol transmission route, hDPP4 transgenic mice were infected with MERSâ€CoV by an animal noseâ€only exposure device and compared with instillationâ€inoculated mice. The challenged mice were observed for 14 consecuti
Document: BACKGROUND: Middle East respiratory syndrome coronavirus (MERSâ€CoV), which is not fully understood in regard to certain transmission routes and pathogenesis and lacks specific therapeutics and vaccines, poses a global threat to public health. METHODS: To simulate the clinical aerosol transmission route, hDPP4 transgenic mice were infected with MERSâ€CoV by an animal noseâ€only exposure device and compared with instillationâ€inoculated mice. The challenged mice were observed for 14 consecutive days and necropsied on days 3, 5, 7, and 9 to analyze viral load, histopathology, viral antigen distribution, and cytokines in tissues. RESULTS: MERSâ€CoV aerosolâ€infected mice with an incubation period of 5â€7 days showed weight loss on days 7â€11, obvious lung lesions on day 7, high viral loads in the lungs on days 3â€9 and in the brain on days 7â€9, and 60% survival. MERSâ€CoV instillationâ€inoculated mice exhibited clinical signs on day 1, obvious lung lesions on days 3â€5, continuous weight loss, 0% survival by day 5, and high viral loads in the lungs and brain on days 3â€5. Viral antigen and high levels of proinflammatory cytokines and chemokines were detected in the aerosol and instillation groups. Disease, lung lesion, and viral replication progressions were slower in the MERSâ€CoV aerosolâ€infected mice than in the MERSâ€CoV instillationâ€inoculated mice. CONCLUSION: hDPP4 transgenic mice were successfully infected with MERSâ€CoV aerosols via an animal noseâ€only exposure device, and aerosol†and instillationâ€infected mice simulated the clinical symptoms of moderate diffuse interstitial pneumonia. However, the transgenic mice exposed to aerosol MERSâ€CoV developed disease and lung pathology progressions that more closely resembled those observed in humans.
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