4.6 Article

Rift Valley Fever Virus Non-Structural Protein S Is Associated with Nuclear Translocation of Active Caspase-3 and Inclusion Body Formation

Journal

VIRUSES-BASEL
Volume 14, Issue 11, Pages -

Publisher

MDPI
DOI: 10.3390/v14112487

Keywords

caspase-3; Rift Valley fever; apoptosis; inclusion bodies

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This study investigates the pathomechanism of intranuclear inclusion body formation in severe Rift Valley fever using a mouse model. The results suggest that the intranuclear accumulation of RVFV NSs is involved in the nuclear translocation of active caspase-3, and both nuclear NSs and active caspase-3 are involved in the formation of visible inclusion bodies. This research is important for understanding severe complications caused by Rift Valley fever virus.
Rift Valley fever phlebovirus (RVFV) causes Rift Valley fever (RVF), an emerging zoonotic disease that causes abortion storms and high mortality rates in young ruminants as well as severe or even lethal complications in a subset of human patients. This study investigates the pathomechanism of intranuclear inclusion body formation in severe RVF in a mouse model. Liver samples from immunocompetent mice infected with virulent RVFV 35/74, and immunodeficient knockout mice that lack interferon type I receptor expression and were infected with attenuated RVFV MP12 were compared to livers from uninfected controls using histopathology and immunohistochemistry for RVFV nucleoprotein, non-structural protein S (NSs) and pro-apoptotic active caspase-3. Histopathology of the livers showed virus-induced, severe hepatic necrosis in both mouse strains. However, immunohistochemistry and immunofluorescence revealed eosinophilic, comma-shaped, intranuclear inclusions and an intranuclear (co-)localization of RVFV NSs and active caspase-3 only in 35/74-infected immunocompetent mice, but not in MP12-infected immunodeficient mice. These results suggest that intranuclear accumulation of RVFV 35/74 NSs is involved in nuclear translocation of active caspase-3, and that nuclear NSs and active caspase-3 are involved in the formation of the light microscopically visible inclusion bodies.

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