Hazara virus infection is lethal for adult type I interferon receptor-knockout mice and may act as a surrogate for infection with the human-pathogenic Crimean–Congo hemorrhagic fever virus

Author:

Dowall Stuart D.1,Findlay-Wilson Stephen1,Rayner Emma1,Pearson Geoff1,Pickersgill Janice1,Rule Antony1,Merredew Natasha1,Smith Hazel1,Chamberlain John1,Hewson Roger1

Affiliation:

1. Health Protection Agency, Porton Down, Salisbury, Wiltshire SP4 0JG, UK

Abstract

Hazara virus (HAZV) is closely related to the Crimean–Congo hemorrhagic fever virus (CCHFV). HAZV has not been reported to cause human disease; work with infectious material can be carried out at containment level (CL)-2. By contrast, CCHFV causes a haemorrhagic fever in humans and requires CL-4 facilities. A disease model of HAZV infection in mice deficient in the type I interferon receptor is reported in this study. Dose–response effects were seen with higher doses, resulting in a shorter time to death and earlier detection of viral loads in organs. The lowest dose of 10 p.f.u. was still lethal in over 50 % of the mice. Histopathological findings were identified in the liver, spleen and lymph nodes, with changes similar to a recent mouse model of CCHFV infection. The findings demonstrate that inoculation of mice with HAZV may act as a useful surrogate model for the testing of antiviral agents against CCHFV.

Publisher

Microbiology Society

Subject

Virology

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