Rift Valley fever virus targets the maternal-foetal interface in ovine and human placentas

Oymans, Judith; Schreur, Paul J. Wichgers; Keulen, Lucien van; Kant, Jet; Kortekaas, Jeroen

doi:10.1371/journal.pntd.0007898

Cited by 40 publications

(67 citation statements)

References 29 publications

(31 reference statements)

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“…RVFV virus replicates efficiently in maternal placental epithelial cells before the virus infects foetal trophoblasts. The virus has also been shown to bypass the maternal epithelial cell layer by directly targeting foetal trophoblasts in the haemophagous zone, a region of the ovine placenta where maternal blood is in direct contact with foetal cells [26] . Thus, the two lambs with fore limb malformations and one lamb with a deformed tail born during the first trimester of pregnancy in this study were consistent with transplacental virus infection, suggesting that the malformation could be attributed to infection by the RVFV arMP-12ΔNSm21/384 vaccine virus.…”

Section: Discussionmentioning

confidence: 99%

“…However, one report claimed that the MP-12 vaccine caused abortions in sheep and foetal malformation, but this alleged observation has not been confirmed [15] . The MP-12 parent vaccine virus was used to develop a recombinant arMP-12ΔNSm21/384 vaccine candidate with nucleotides deleted from the genes that encoded for the non-structural M protein [26] . Experimental studies including pregnant sheep and calves demonstrated that this recombinant vaccine was safe, efficacious and non-teratogenic [16] , [17] , [18] .…”

Section: Introductionmentioning

confidence: 99%

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Safety and immunogenicity of the Rift Valley fever arMP-12 ΔNSm21/384 candidate vaccine in pregnant ewes

Boumart¹,

Bamouh²,

Hamdi³

et al. 2020

Vaccine: X

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Highlights Rift Valley fever virus causes abortion, teratogenicity and mortality in domestic ruminants. Safety and immunogenicity RVFV arMP-12ΔNSm21/384 vaccine was determined in pregnant ewes. Vaccine was safe and immunogenic last stages of pregnancy, but may caused malformed lambs early stage. Pregnant sheep should not be vaccinated with the RVFV vaccine during the first month of gestation.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Safety and immunogenicity of the Rift Valley fever arMP-12 ΔNSm21/384 candidate vaccine in pregnant ewes

Boumart¹,

Bamouh²,

Hamdi³

et al. 2020

Vaccine: X

View full text Add to dashboard Cite

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“…All dilutions and suspensions were prepared in complete medium. After 48 h, an immunoperoxidase monolayer assay (IPMA) was performed as described previously using the rabbit antisera as primary antibodies and anti-goat-HRP (Dako, Agilent, Santa Clara, CA, USA) as a secondary antibody [37]. A well was scored positive for neutralization if less than 50% of the cells were stained, the negative control (without serum) was used as 100% cell staining.…”

Section: Virus Neutralization Testmentioning

confidence: 99%

“…All growth curves were performed in triplicate and each sample was titrated in triplicate using end-point dilution assay as described previously [38]. An immunoperoxidase monolayer assay (IPMA) was performed as described using the rabbit antisera as primary antibodies and anti-rabbit-HRP (Dako, Agilent, Santa Clara, CA, USA) as a secondary antibody [37]. Titres were determined using the Spearman-Kärber algorithm and were expressed as TCID 50 /mL.…”

Section: Growth Curvesmentioning

confidence: 99%

Reverse Genetics System for Shuni Virus, an Emerging Orthobunyavirus with Zoonotic Potential

Oymans

Schreur

Oort

et al. 2020

Viruses

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The genus Orthobunyavirus (family Peribunyaviridae, order Bunyavirales) comprises over 170 named mosquito- and midge-borne viruses, several of which cause severe disease in animals or humans. Their three-segmented genomes enable reassortment with related viruses, which may result in novel viruses with altered host or tissue tropism and virulence. One such reassortant, Schmallenberg virus (SBV), emerged in north-western Europe in 2011. Shuni virus (SHUV) is an orthobunyavirus related to SBV that is associated with neurological disease in horses in southern Africa and recently caused an outbreak manifesting with neurological disease and birth defects among ruminants in Israel. The zoonotic potential of SHUV was recently underscored by its association with neurological disease in humans. We here report a reverse genetics system for SHUV and provide first evidence that the non-structural (NSs) protein of SHUV functions as an antagonist of host innate immune responses. We furthermore report the rescue of a reassortant containing the L and S segments of SBV and the M segment of SHUV. This novel reverse genetics system can now be used to study SHUV virulence and tropism, and to elucidate the molecular mechanisms that drive reassortment events.

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“…Each placentome contains maternal and foetal tissues, which are separated by several cell layers. The maternal epithelium and foetal trophoblasts form the actual barrier between mother and foetus in the synepitheliochorial part of the placenta, whereas in the so-called haemophagous zones, foetal trophoblasts are in direct contact with stagnant pools of maternal blood [19].…”

Section: Wslv Replicates In the Ovine Placentamentioning

confidence: 99%

Early Pathogenesis of Wesselsbron Disease in Pregnant Ewes

et al. 2020

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Wesselsbron virus (WSLV) is a neglected, mosquito-borne flavivirus that is endemic to the African continent. The virus is teratogenic to ruminants and causes a self-limiting febrile illness in humans. Wesselsbron disease manifests with similar clinical signs and occurs in the same areas under the same climatic conditions as Rift Valley fever, which is therefore included in the differential diagnosis. Although the gross pathology of WSLV infection in pregnant ewes is reported in literature, the pathogenesis that leads to stillbirths, congenital malformations and abortion has remained undescribed. In the present study, pregnant ewes were inoculated with WSLV and subjected to detailed clinical- and histopathology 8 days later. The virus was mainly detected in foetal trophoblasts of the placenta and in neural progenitor cells, differentiated neurons, oligodendrocytes, microglia and astrocytes. Our study demonstrates that WSLV efficiently crosses the maternal–foetal interface and is highly neuroinvasive in the ovine foetus.

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Rift Valley fever virus targets the maternal-foetal interface in ovine and human placentas

Cited by 40 publications

References 29 publications

Safety and immunogenicity of the Rift Valley fever arMP-12 ΔNSm21/384 candidate vaccine in pregnant ewes

Safety and immunogenicity of the Rift Valley fever arMP-12 ΔNSm21/384 candidate vaccine in pregnant ewes

Reverse Genetics System for Shuni Virus, an Emerging Orthobunyavirus with Zoonotic Potential

Early Pathogenesis of Wesselsbron Disease in Pregnant Ewes

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