4.6 Article

NSG-Mice Reveal the Importance of a Functional Innate and Adaptive Immune Response to Overcome RVFV Infection

Journal

VIRUSES-BASEL
Volume 14, Issue 2, Pages -

Publisher

MDPI
DOI: 10.3390/v14020350

Keywords

Rift Valley fever; immunodeficiency; innate immunity; adaptive immunity; virus persistence

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The interferon type 1 response is critical for controlling RVFV replication and disease, while functional NK cells, macrophages, and lymphocytes are essential for virus clearance during RVFV infection.
Rift Valley fever (RVF) is a zoonotic disease caused by RVF Phlebovirus (RVFV). The RVFV MP-12 vaccine strain is known to exhibit residual virulence in the case of a deficient interferon type 1 response. The hypothesis of this study is that virus replication and severity of lesions induced by the MP-12 strain in immunocompromised mice depend on the specific function of the disturbed pathway. Therefore, 10 strains of mice with deficient innate immunity (B6-IFNAR(tmAgt), C.129S7(B6)-Ifng(tm1Ts)/J, B6-TLR3(tm1Flv), B6-TLR7(tm1Aki), NOD/ShiLtJ), helper T-cell- (CD4(tm1Mak)), cytotoxic T-cell- (CD8(atm1Mak)), B-cell- (Igh-J(tm1Dhu)N?+N2), combined T- and B-cell- (NU/J) and combined T-, B-, natural killer (NK) cell- and macrophage-mediated immunity (NOD.Cg-Prkdc(scid)Il2rg(tm1WjI)/SzJ (NSG) mice) were subcutaneously infected with RVFV MP-12. B6-IFNAR(tmAgt) mice were the only strain to develop fatal disease due to RVFV-induced severe hepatocellular necrosis and apoptosis. Notably, no clinical disease and only mild multifocal hepatocellular necrosis and apoptosis were observed in NSG mice, while immunohistochemistry detected the RVFV antigen in the liver and the brain. No or low virus expression and no lesions were observed in the other mouse strains. Conclusively, the interferon type 1 response is essential for early control of RVFV replication and disease, whereas functional NK cells, macrophages and lymphocytes are essential for virus clearance.

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