Interferonogenic activity of the strain BH-3 duck hepatitis virus type I (Picornaviridae: Avihepatovirus: Avihepatovirus A)

Introduction. Duck viral hepatitis type I (DVH-I) is a poorly studied contagious disease caused by RNA-containing duck (Anatinae) hepatitis virus type I (Picornaviridae: Avihepatovirus: Avihepatovirus A). This infection is widespread in many countries, including Russia, and causes significant damage to industrial duck breeding. The study of interferonogenic activity of its etiologic agent strains is of great importance in solving the problem of developing effective means to control the disease.Material and methods. Strain BH-3 of duck hepatitis virus type I isolated from the liver of sick ducklings was used in the study. The strain was adapted to developing 10–12 day old duck embryos, to the cell culture of chicken and duck fibroblasts and deposited in the State Collection of Viruses of the D.I. Ivanovsky Institute of Virology of FSBI «National Research Centre for Epidemiology and Microbiology named after the honorary academician N.F. Gamaleya» of the Ministry of Health of Russia. Experiments were performed using the standard tissue culture method.Results and discussion. Data on the ability of the viral strain BH-3 to induce interferon (IFN) and its sensitivity to the action of exogenous interferon in the culture of duck fibroblasts are presented. It has been shown that the interferonogenic activity of this strain of the hepatitis virus is in direct proportion to the multiplicity of infection. The maximum induction of IFN (1 : 256 CEPD50) was observed at a dose of 1.0 TCD50/cell in 72–96 hrs after inoculation of the cell culture. Exogenous IFN at a dose of 1 : 128 completely suppressed the cytopathic effect and death of duck embryos infected with hepatitis virus at a dose of 100 TCD50/cell.Conclusion. The data obtained allow us to state that the vaccine strain BH-3 of duck hepatitis virus type I has a pronounced interferonogenic activity and sensitivity to the action of exogenous IFN. This may have implications for the development of effective therapeutic agents against DVH-I.

Ferritin heavy polypeptide 1 mediates apoptosis-related gene expression of duck (Anas platyrhynchos domesticus)

Duck hepatitis virus type 1 (DHV-1) infection of ducklings causes hepatitis and is associated with high morbidity and mortality. Virus infection may induce apoptosis and inhibit proliferation. In humans, ferritin heavy polypeptide 1 (FTH1) has been reported to affect the development of hepatitis and inhibit apoptosis. However, the effect of duck FTH1 (duFTH1) on apoptosis in DHV-1 infected ducklings has not been investigated. Therefore, we measured duFHT1 expression in tissues of DHV-1 infected ducklings and characterized the functional effects of ectopic overexpression and endogenous downregulation of FTH1 in duck embryo fibroblasts (DEF) to elucidate possible mechanisms involved. In the present study, the expression of duFTH1 was decreased in liver and spleen after DHV-1 infection. The effects of altered FTH1 expression on expression of pro- and anti-apoptotic genes were evaluated by qPCR arrays. Decreased expressions of Caspase-3 and Caspase-8 were observed in FTH1-overexpressing DEF cells, while decreased expression of Bcl-2 was detected in FTH1 knocked down DEF cells. Our findings suggest that the regulation of FTH1 expression indirectly mediated the expression of apoptosis-related genes; the protective effect of FTH1 was associated with the inhibition of apoptosis in DEF.