Your search keyword '"Rift Valley Fever"' showing total 261 results

1. A Lipid Nanoparticle-Formulated Self-Amplifying RNA Rift Valley Fever Vaccine Induces a Robust Humoral Immune Response in Mice.

Author

Kitandwe, Paul K., Rogers, Paul, Hu, Kai, Nayebare, Owen, Blakney, Anna K., McKay, Paul F., Kaleebu, Pontiano, and Shattock, Robin J.

Subjects

RIFT Valley fever, VENEZUELAN equine encephalomyelitis, HUMORAL immunity, MEMBRANE glycoproteins, ENCEPHALITIS viruses

Abstract

Rift Valley fever (RVF) is a mosquito-borne viral zoonosis that causes high fetal and neonatal mortality rates in ruminants and sometimes severe to fatal complications like encephalitis and hemorrhagic fever in humans. There is no licensed RVF vaccine for human use while approved livestock vaccines have suboptimal safety or efficacy. We designed self-amplifying RNA (saRNA) RVF vaccines and assessed their humoral immunogenicity in mice. Plasmid DNA encoding the Rift Valley fever virus (RVFV) medium (M) segment consensus sequence (WT consensus) and its derivatives mutated to enhance cell membrane expression of the viral surface glycoproteins n (Gn) and c (Gc) were assessed for in vitro expression. The WT consensus and best-expressing derivative (furin-T2A) were cloned into a Venezuelan equine encephalitis virus (VEEV) plasmid DNA replicon and in vitro transcribed into saRNA. The saRNA was formulated in lipid nanoparticles and its humoral immunogenicity in BALB/c mice was assessed. High quantities of dose-dependent RVFV Gn IgG antibodies were detected in the serum of all mice immunized with either WT consensus or furin-T2A saRNA RVF vaccines. Significant RVFV pseudovirus-neutralizing activity was induced in mice immunized with 1 µg or 10 µg of the WT consensus saRNA vaccine. The WT consensus saRNA RVF vaccine warrants further development. [ABSTRACT FROM AUTHOR]

Published

2024

2. A Review of Nonhuman Primate Models of Rift Valley Fever Virus Infection: Progress, Challenge Strains, and Future Directions.

Author

Ebisine, Kimimuepigha, Quist, Darcy, Findlay-Wilson, Stephen, Kennedy, Emma, and Dowall, Stuart

Subjects

RIFT Valley fever, MOSQUITO-borne diseases, CLINICAL trials, ANIMAL diseases, ANIMAL young, MACAQUES

Abstract

Rift Valley fever (RVF) is a mosquito-borne viral disease that primarily affects animals, especially ruminants, but has the capacity to infect humans and result in outbreaks. Infection with the causative agent, RVF virus (RVFV), causes severe disease in domestic animals, especially sheep, resulting in fever, anorexia, immobility, abortion, and high morbidity and mortality rates in neonate animals. Humans become infected through exposure to infected animals and, less frequently, directly via a mosquito bite. A greater awareness of RVFV and its epidemic potential has resulted in increased investment in the development of interventions, especially vaccines. There is currently no substitute for the use of animal models in order to evaluate these vaccines. As outbreaks of RVF disease are difficult to predict or model, conducting Phase III clinical trials will likely not be feasible. Therefore, representative animal model systems are essential for establishing efficacy data to support licensure. Nonhuman primate (NHP) species are often chosen due to their closeness to humans, reflecting similar susceptibility and disease kinetics. This review covers the use of NHP models in RVFV research, with much of the work having been conducted in rhesus macaques and common marmosets. The future direction of RVF work conducted in NHP is discussed in anticipation of the importance of it being a key element in the development and approval of a human vaccine. [ABSTRACT FROM AUTHOR]

Published

2024

3. A Quadruple Gene-Deleted Live BoHV-1 Subunit RVFV Vaccine Vector Reactivates from Latency and Replicates in the TG Neurons of Calves but Is Not Transported to and Shed from Nasal Mucosa.

Author

Pavulraj, Selvaraj, Stout, Rhett W., Paulsen, Daniel B., and Chowdhury, Shafiqul I.

Subjects

*RIFT Valley fever, *ANIMAL herds, *VIRAL shedding, *VACCINE effectiveness, *NERVE endings

Abstract

Bovine herpesvirus type 1 (BoHV-1) establishes lifelong latency in trigeminal ganglionic (TG) neurons following intranasal and ocular infection in cattle. Periodically, the latent virus reactivates in the TG due to stress and is transported anterogradely to nerve endings in the nasal epithelium, where the virus replicates and sheds. Consequently, BoHV-1 is transmitted to susceptible animals and maintained in the cattle population. Modified live BoHV-1 vaccine strains (BoHV-1 MLV) also have a similar latency reactivation. Therefore, they circulate and are maintained in cattle herds. Additionally, they can regain virulence and cause vaccine outbreaks because they mutate and recombine with other circulating field wild-type (wt) strains. Recently, we constructed a BoHV-1 quadruple mutant virus (BoHV-1qmv) that lacks immune evasive properties due to UL49.5 and glycoprotein G (gG) deletions. In addition, it also lacks the gE cytoplasmic tail (gE CT) and Us9 gene sequences designed to make it safe, increase its vaccine efficacy against BoHV-1, and restrict its anterograde neuronal transport noted above. Further, we engineered the BoHV-1qmv-vector to serve as a subunit vaccine against the Rift Valley fever virus (BoHV-1qmv Sub-RVFV) (doi: 10.3390/v15112183). In this study, we determined the latency reactivation and nasal virus shedding properties of BoHV-1qmv (vector) and BoHV-1qmv-vectored subunit RVFV (BoHV-1qmv sub-RVFV) vaccine virus in calves in comparison to the BoHV-1 wild-type (wt) following intranasal inoculation. The real-time PCR results showed that BoHV-1 wt- but not the BoHV-1qmv vector- and BoHV-1qmv Sub-RVFV-inoculated calves shed virus in the nose following dexamethasone-induced latency reactivation; however, like the BoHV-1 wt, both the BoHV-1qmv vector and BoHV-1qmv Sub-RVFV viruses established latency, were reactivated, and replicated in the TG neurons. These results are consistent with the anterograde neurotransport function of the gE CT and Us9 sequences, which are deleted in the BoHV-1qmv and BoHV-1qmv Sub-RVFV. [ABSTRACT FROM AUTHOR]

Published

2024

4. Large-Scale Serological Survey of Crimean-Congo Hemorrhagic Fever Virus and Rift Valley Fever Virus in Small Ruminants in Senegal.

Author

Gahn, Marie Cicille Ba, Diouf, Gorgui, Cissé, Ndjibouyé, Ciss, Mamadou, Bordier, Marion, Ndiaye, Mbengué, Bakhoum, Mame Thierno, Djiba, Mamadou Lamine, Brown, Corrie, Faburay, Bonto, Fall, Assane Gueye, and Lo, Modou Moustapha

Subjects

RIFT Valley fever, ZOONOSES, HEMORRHAGIC fever, IDENTIFICATION of animals, ANIMAL species, PESTE des petits ruminants

Abstract

Crimean-Congo hemorrhagic fever (CCHF) and Rift Valley fever (RVF) are among the list of emerging zoonotic diseases that require special attention and priority. RVF is one of the six priority diseases selected by the Senegalese government. Repeated epidemic episodes and sporadic cases of CCHF and RVF in Senegal motivated this study, involving a national cross-sectional serological survey to assess the distribution of the two diseases in this country throughout the small ruminant population. A total of 2127 sera from small ruminants (goat and sheep) were collected in all regions of Senegal. The overall seroprevalence of CCHF and RVF was 14.1% (IC 95%: 12.5–15.5) and 4.4% (95% CI: 3.5–5.3), respectively. The regions of Saint-Louis (38.4%; 95% CI: 30.4–46.2), Kolda (28.3%; 95% CI: 20.9–35.7), Tambacounda (22.2%; 95% CI: 15.8–28.6) and Kédougou (20.9%; 95% CI: 14.4–27.4) were the most affected areas. The risk factors identified during this study show that the age, species and sex of the animals are key factors in determining exposure to these two viruses. This study confirms the active circulation of CCHF in Senegal and provides important and consistent data that can be used to improve the surveillance strategy of a two-in-one health approach to zoonoses. [ABSTRACT FROM AUTHOR]

Published

2024

5. Exposure to Arboviruses in Cattle: Seroprevalence of Rift Valley Fever, Bluetongue, and Epizootic Hemorrhagic Disease Viruses and Risk Factors in Baringo County, Kenya.

Author

Chiuya, Tatenda, Fèvre, Eric M., Okumu, Noah O., Abdi, Abdullahi M., Junglen, Sandra, and Borgemeister, Christian

Subjects

DISEASE risk factors, ANIMAL herds, RIFT Valley fever, HEMORRHAGIC diseases, BLUETONGUE virus, SERODIAGNOSIS

Abstract

Rift Valley fever virus (RVFV) causes disease outbreaks in livestock and humans; however, its inter-epidemic circulation is poorly understood, similar to other arboviruses affecting cattle such as bluetongue virus (BTV) and epizootic hemorrhagic disease virus (EHDV). Serum samples were collected in Baringo County, Kenya from 400 cattle, accompanied by a risk factor questionnaire. Serological tests were then conducted to determine the exposure of cattle to RVFV, BTV, and EHDV. RVFV, BTV, and EHDV IgG seroprevalence rates were 15.5%, 91.5%, and 91%, respectively. Seropositivity for RVFV, BTV, and EHDV was significantly higher in adult cattle, as well as in females for RVFV. Cattle with herd owners aged between 30–39 years were less likely to be seropositive for RVFV compared to those with owners over the age of 60 years. High seroprevalence of BTV and EHDV in cattle indicates significant exposure and the subclinical circulation of these viruses, presenting a risk of outbreaks to sheep and naïve cattle. Moreover, the detection of RVFV-seropositive young cattle born after the last reported outbreak suggests inter-epidemic circulation of the virus. Overall, monitoring these arboviruses in cattle is crucial in understanding their distribution and seroprevalence during inter-epidemic periods. [ABSTRACT FROM AUTHOR]

Published

2024

6. Genomic Epidemiology of Rift Valley Fever Virus Involved in the 2018 and 2022 Outbreaks in Livestock in Rwanda.

Author

Nsengimana, Isidore, Juma, John, Roesel, Kristina, Gasana, Methode N., Ndayisenga, Fabrice, Muvunyi, Claude M., Hakizimana, Emmanuel, Hakizimana, Jean N., Eastwood, Gillian, Chengula, Augustino A., Bett, Bernard, Kasanga, Christopher J., and Oyola, Samuel O.

Subjects

*RIFT Valley fever, *ZOONOSES, *MOLECULAR cloning, *ANIMAL cloning, *SLAUGHTERING

Abstract

Rift Valley fever (RVF), a mosquito-borne transboundary zoonosis, was first confirmed in Rwanda's livestock in 2012 and since then sporadic cases have been reported almost every year. In 2018, the country experienced its first large outbreak, which was followed by a second one in 2022. To determine the circulating virus lineages and their ancestral origin, two genome sequences from the 2018 outbreak, and thirty-six, forty-one, and thirty-eight sequences of small (S), medium (M), and large (L) genome segments, respectively, from the 2022 outbreak were generated. All of the samples from the 2022 outbreak were collected from slaughterhouses. Both maximum likelihood and Bayesian-based phylogenetic analyses were performed. The findings showed that RVF viruses belonging to a single lineage, C, were circulating during the two outbreaks, and shared a recent common ancestor with RVF viruses isolated in Uganda between 2016 and 2019, and were also linked to the 2006/2007 largest East Africa RVF outbreak reported in Kenya, Tanzania, and Somalia. Alongside the wild-type viruses, genetic evidence of the RVFV Clone 13 vaccine strain was found in slaughterhouse animals, demonstrating a possible occupational risk of exposure with unknown outcome for people working in meat-related industry. These results provide additional evidence of the ongoing wide spread of RVFV lineage C in Africa and emphasize the need for an effective national and international One Health-based collaborative approach in responding to RVF emergencies. [ABSTRACT FROM AUTHOR]

Published

2024

7. Distinct Pathological Changes in Preweaning Mice Infected with Live-Attenuated Rift Valley Fever Virus Strains.

Author

Alkan, Cigdem, Jurado-Cobena, Eduardo, and Ikegami, Tetsuro

Subjects

*RIFT Valley fever, *ENDEMIC diseases, *VACCINE safety, *BRAIN diseases, *PATHOLOGICAL physiology

Abstract

Rift Valley fever (RVF) is a mosquito-borne zoonotic viral disease endemic to Africa and the Middle East. Live-attenuated RVF vaccines have been studied for both veterinary and human use due to their strong immunogenicity and cost-effective manufacturing. The live-attenuated MP-12 vaccine has been conditionally approved for veterinary use in the U.S.A., and next-generation live-attenuated RVF vaccine candidates are being actively researched. Assessing the virulence phenotype of vaccine seeds or lots is crucial for managing vaccine safety. Previously, preweaning 19-day-old outbred CD1 mice have been used to evaluate the MP-12 strain. This study aimed to characterize the relative virulence of three live-attenuated RVF vaccine strains in 19-day-old inbred C57BL/6 mice: the recombinant MP-12 (rMP-12), the RVax-1, and the ∆NSs-∆NSm-rZH501 strains. Although this mouse model did not show dose-dependent pathogenesis, mice that succumbed to the infection exhibited distinct brain pathology. Mice infected with ∆NSs-∆NSm-rZH501 showed an infiltration of inflammatory cells associated with infected neurons, and focal lesions formed around virus-infected cells. In contrast, mice infected with rMP-12 or RVax-1 showed a minimal association of inflammatory cells in the brain, yet the virus spread diffusely. The preweaning model is likely useful for evaluating host responses to attenuated RVFV strains, although further refinement may be necessary to quantitate the virulence among different RVFV strains or vaccine lots. [ABSTRACT FROM AUTHOR]

Published

2024

8. The Development of a Multivalent Capripoxvirus-Vectored Vaccine Candidate to Protect against Sheeppox, Goatpox, Peste des Petits Ruminants, and Rift Valley Fever.

Author

Boshra, Hani, Blyth, Graham A. D., Truong, Thang, Kroeker, Andrea, Kara, Pravesh, Mather, Arshad, Wallace, David, and Babiuk, Shawn

Subjects

LUMPY skin disease, RIFT Valley fever, VIRAL shedding, LIVESTOCK losses, VIRUS diseases, PESTE des petits ruminants, BOVINE viral diarrhea

Abstract

Capripoxviruses are the causative agents of sheeppox, goatpox, and lumpy skin disease (LSD) in cattle, which cause economic losses to the livestock industry in Africa and Asia. Capripoxviruses are currently controlled using several live attenuated vaccines. It was previously demonstrated that a lumpy skin disease virus (LSDV) field isolate from Warmbaths (WB) South Africa, ORF 005 (IL-10) gene-deleted virus (LSDV WB005KO), was able to protect sheep and goats against sheeppox and goatpox. Subsequently, genes encoding the protective antigens for peste des petits ruminants (PPR) and Rift Valley fever (RVF) viruses have been inserted in the LSDV WB005KO construct in three different antigen forms (native, secreted, and fusion). These three multivalent vaccine candidates were evaluated for protection against PPR using a single immunization of 104 TCID50 in sheep. The vaccine candidates with the native and secreted antigens protected sheep against PPR clinical disease and decreased viral shedding, as detected using real-time RT-PCR in oral and nasal swabs. An anamnestic antibody response, measured using PPR virus-neutralizing antibody response production, was observed in sheep following infection. The vaccine candidates with the antigens expressed in their native form were evaluated for protection against RVF using a single immunization with doses of 104 or 105 TCID50 in sheep and goats. Following RVF virus infection, sheep and goats were protected against clinical disease and no viremia was detected in serum compared to control animals, where viremia was detected one day following infection. Sheep and goats developed RVFV-neutralizing antibodies prior to infection, and the antibody responses increased following infection. These results demonstrate that an LSD virus-vectored vaccine candidate can be used in sheep and goats to protect against multiple viral infections. [ABSTRACT FROM AUTHOR]

Published

2024

9. Monoclonal Antibodies for Rift Valley Fever Virus Nucleocapsid: Application in IgG/IgM ELISA for Sero-Diagnosis.

Author

Huang, Jiansheng, Adungo, Ferdinard, Konongoi, Samson Limbaso, Inoue, Shingo, Zhan, Lin, Sang, Rosemary, Ashur, Salame, Kwallah, Allan ole, Mwau, Matilu, Morita, Kouichi, and Yu, Fuxun

Subjects

RIFT Valley fever, ZOONOSES, VIRAL antibodies, SPLEEN, IMMUNOGLOBULIN G, MONOCLONAL antibodies

Abstract

Introduction: Rift Valley fever virus (RVFV) belonging to the Phenuiviridae family is responsible for a zoonotic disease called Rift Valley fever (RVF). Currently, RVFV has spread from Africa to Asia, and due to its ability to cause high mortality rates, it has significantly impacted human health and economic development in many societies. Highly specific and sensitive systems for sero-diagnosis of RVFV infection are needed for clinical use. Method: BALB/c mice were immunized with recombinant RVFV nucleocapsid (rRVFV-N) protein and the spleen cells fused with SP2/0 myeloma cells to create hybridoma cell lines. The secreted monoclonal antibodies (MAbs) were purified and characterized. Enzyme-linked immunosorbent assay (ELISA) systems for the detection of IgG and IgM using the new MAbs were established and evaluated. Serum samples from 96 volunteers and 93 patients of suspected RVF from Kenya were tested compared with the ELISA systems based on inactivated viruses and the rabbit polyclonal antibody. Result: Three monoclonal antibodies against rRVFV-N protein were established. The performance of the MAb-based sandwich IgG ELISA and the IgM capture ELISA perfectly matched the ELISA systems using the inactivated virus or the polyclonal antibody. Conclusions: Recombinant RVFV-N protein-specific MAbs were developed and they offer useful tools for RVFV studies. The MAb-based ELISA systems for detecting IgG and IgM offer safe and useful options for diagnosing RVFV infections in humans. [ABSTRACT FROM AUTHOR]

Published

2024

10. Rift Valley Fever Phlebovirus Reassortment Study in Sheep.

Author

Balaraman, Velmurugan, Indran, Sabarish V., Kim, In Joong, Trujillo, Jessie D., Meekins, David A., Shivanna, Vinay, Zajac, Michelle D., Urbaniak, Kinga, Morozov, Igor, Sunwoo, Sun-Young, Faburay, Bonto, Osterrieder, Klaus, Gaudreault, Natasha N., Wilson, William C., and Richt, Juergen A.

Subjects

*RIFT Valley fever, *SHEEP, *VETERINARY public health, *SHEEP breeds, *AEDES aegypti, *PUBLIC health, *INFECTIOUS disease transmission

Abstract

Rift Valley fever (RVF) in ungulates and humans is caused by a mosquito-borne RVF phlebovirus (RVFV). Live attenuated vaccines are used in livestock (sheep and cattle) to control RVF in endemic regions during outbreaks. The ability of two or more different RVFV strains to reassort when co-infecting a host cell is a significant veterinary and public health concern due to the potential emergence of newly reassorted viruses, since reassortment of RVFVs has been documented in nature and in experimental infection studies. Due to the very limited information regarding the frequency and dynamics of RVFV reassortment, we evaluated the efficiency of RVFV reassortment in sheep, a natural host for this zoonotic pathogen. Co-infection experiments were performed, first in vitro in sheep-derived cells, and subsequently in vivo in sheep. Two RVFV co-infection groups were evaluated: group I consisted of co-infection with two wild-type (WT) RVFV strains, Kenya 128B-15 (Ken06) and Saudi Arabia SA01-1322 (SA01), while group II consisted of co-infection with the live attenuated virus (LAV) vaccine strain MP-12 and a WT strain, Ken06. In the in vitro experiments, the virus supernatants were collected 24 h post-infection. In the in vivo experiments, clinical signs were monitored, and blood and tissues were collected at various time points up to nine days post-challenge for analyses. Cell culture supernatants and samples from sheep were processed, and plaque-isolated viruses were genotyped to determine reassortment frequency. Our results show that RVFV reassortment is more efficient in co-infected sheep-derived cells compared to co-infected sheep. In vitro, the reassortment frequencies reached 37.9% for the group I co-infected cells and 25.4% for the group II co-infected cells. In contrast, we detected just 1.7% reassortant viruses from group I sheep co-infected with the two WT strains, while no reassortants were detected from group II sheep co-infected with the WT and LAV strains. The results indicate that RVFV reassortment occurs at a lower frequency in vivo in sheep when compared to in vitro conditions in sheep-derived cells. Further studies are needed to better understand the implications of RVFV reassortment in relation to virulence and transmission dynamics in the host and the vector. The knowledge learned from these studies on reassortment is important for understanding the dynamics of RVFV evolution. [ABSTRACT FROM AUTHOR]

Published

2024

11. Expanding Understanding of Urban Rift Valley Fever Risk and Associated Vector Ecology at Slaughterhouses in Kisumu, Kenya.

Author

Gerken, Keli Nicole, Owuor, Kevin Omondi, Ndenga, Bryson, Wambua, Sammy, Winter, Christabel, Chemutai, Salome, Omukuti, Rodney, Arabu, Daniel, Miring'u, Irene, Wilson, William C., Mutuku, Francis, Waggoner, Jesse J., Pinsky, Benjamin, Bosire, Carren, and LaBeaud, Angelle Desiree

Subjects

RIFT Valley fever, SLAUGHTERING, URBAN ecology, ANIMAL experimentation, CULEX

Abstract

Rift Valley fever virus (RVFV) is an adaptable arbovirus that can be transmitted by a wide variety of arthropods. Widespread urban transmission of RVFV has not yet occurred, but peri-urban outbreaks of RVFV have recently been documented in East Africa. We previously reported low-level exposure in urban communities and highlighted the risk of introduction via live animal influx. We deployed a slaughtered animal testing framework in response to an early warning system at two urban slaughterhouses and tested animals entering the meat value chain for anti-RVFV IgG and IgM antibodies. We simultaneously trapped mosquitoes for RVFV and bloodmeal testing. Out of 923 animals tested, an 8.5% IgG seroprevalence was identified but no evidence of recent livestock exposure was detected. Mosquito species abundance varied greatly by slaughterhouse site, which explained 52% of the variance in blood meals. We captured many Culex spp., a known RVFV amplifying vector, at one of the sites (p < 0.001), and this species had the most diverse blood meals. No mosquito pools tested positive for RVFV antigen using a rapid VecTOR test. These results expand understanding of potential RVF urban disease ecology, and highlight that slaughterhouses are key locations for future surveillance, modelling, and monitoring efforts. [ABSTRACT FROM AUTHOR]

Published

2024

12. Serological Evidence of Crimean–Congo Haemorrhagic Fever in Livestock in the Omaheke Region of Namibia.

Author

Samkange, Alaster, Mbiri, Pricilla, Matomola, Ophelia Chuma, Zaire, Georgina, Homateni, Anna, Junias, Elifas, Kaatura, Israel, Khaiseb, Siegfried, Ekandjo, Simson, Shoopala, Johannes, Hausiku, Magrecia, Shilongo, Albertina, Mujiwa, Mushabati Linus, Dietze, Klaas, Busch, Frank, Winter, Christian, Matos, Carolina, Weiss, Sabrina, and Chitanga, Simbarashe

Subjects

HEMORRHAGIC fever, ANIMAL herds, ENZYME-linked immunosorbent assay, LIVESTOCK, SHEEP ranches, RIFT Valley fever, SHEEP diseases, CATTLE herding

Abstract

This research examined the positivity ratio of Crimean–Congo haemorrhagic fever (CCHF) antibodies in cattle and sheep within Namibia's Omaheke region after a human disease outbreak in the same geographical area. A total of 200 samples (100 cattle and 100 sheep) were randomly collected from animals brought to two regional auction sites, and then tested using the ID Screen® CCHF Double Antigen Multi-Species Enzyme-Linked Immunosorbent Assay kit. Of the cattle samples, 36% tested positive, while 22% of the sheep samples were seropositive. The cattle had a significantly higher positivity ratio than sheep at the individual animal level (p = 0.0291). At the herd level, 62.5% of cattle herds and 45.5% of sheep flocks had at least one positive animal, but this difference was statistically insignificant (p = 0.2475). The fourteen cattle farms with at least one seropositive animal were dispersed across the Omaheke region. In contrast, the ten sheep farms with seropositive cases were predominantly situated in the southern half of the region. The study concluded that the CCHF is endemic in the Omaheke region and likely in most of Namibia, underscoring the importance of continued surveillance and preventive measures to mitigate the impact of CCHFV on animal health and potential spillover into human populations. [ABSTRACT FROM AUTHOR]

Published

2024

13. Seroprevalence and Risk Factors Associated with Phleboviruses and Crimean–Congo Hemorrhagic Fever Virus among Blood Donors in Central Tunisia.

Author

Ayari, Rym, Chaouch, Houda, Findlay-Wilson, Stephen, Hachfi, Wissem, Ben Lasfar, Nadia, Bellazreg, Foued, Dowall, Stuart, Hannachi, Neila, and Letaief, Amel

Subjects

HEMORRHAGIC fever, BLOOD donors, RIFT Valley fever, SEROPREVALENCE, CITIES & towns

Abstract

The aim of this study was to determine the prevalence of six viruses, from two families of the order Bunyavirales, in the general population of central Tunisia. Sera collected from 377 asymptomatic blood donors were serologically assayed for Rift Valley fever virus (RVFV), Crimean–Congo hemorrhagic fever virus (CCHFV), and four sandfly-borne phleboviruses: Toscana virus (TOSV), sandfly fever Naples virus (SFNV), sandfly fever Sicilian virus (SFSV), and sandfly fever Cyprus virus (SFCV). Of the 377 subjects enrolled in this study, 17.3% were IgG positive for at least one of the viruses tested. The most frequently detected antibodies were against TOSV (13.3%), followed by SFCV (2.9%), RVFV (1.9%), SFSV (1.3%), and SFNV (1.1%). Only one sample was IgG positive for CCHFV. Dual reactivity was observed in nine cases: SFSV + SFCV in three cases (0.8%) and TOSV + SFNV, TOSV + SFCV, and TOSV + RVFV in two cases (0.5%) each. 15.9% of donors were IgG positive against sandfly-borne phleboviruses. Among the 65 donors IgG positive for phleboviruses, 50.8% were from rural areas compared to 12.3% from urban areas (p < 0.001); 92.3% had animals in their living quarters (p = 0.009); and 70.8% lived in the vicinity of stagnant water (p = 0.062). Seroprevalence was significantly higher among donors living with chronic diseases (p = 0.039). Furthermore, the seroprevalence of phleboviruses was higher in Kairouan, the central governorate, than in the two coastal governorates: Monastir and Sousse, with 33.4%, 24.2%, and 14.9%, respectively. The presence of antibodies in the general population needs further investigation to better assess the extent of these viruses. Only TOSV was known to have an extensive circulation in Tunisia and in North Africa. Continued surveillance and interventions are necessary to detect the emergence of all arboviruses and to prevent further transmission. [ABSTRACT FROM AUTHOR]

Published

2024

14. Rift Valley Fever Virus: An Overview of the Current Status of Diagnostics.

Author

Lapa, Daniele, Pauciullo, Silvia, Ricci, Ida, Garbuglia, Anna Rosa, Maggi, Fabrizio, Scicluna, Maria Teresa, and Tofani, Silvia

Subjects

RIFT Valley fever, LYME disease, HEMORRHAGIC fever, SYMPTOMS, ZOONOSES, VECTOR-borne diseases

Abstract

Rift Valley fever is a vector-borne zoonotic disease caused by the Rift Valley fever virus (Phlebovirus genus) listed among the eight pathogens included in the Bluepoint list by the WHO. The transmission is mainly vehicled by Aedes and Culex mosquito species. Symptoms of the disease are varied and non-specific, making clinical diagnosis often challenging, especially in the early stages. Due to the difficulty in distinguishing Rift Valley fever from other viral hemorrhagic fevers, as well as many other diseases that cause fever, an early diagnosis of the infection is important to limit its spread and to provide appropriate care to patients. To date, there is no validated point-of-care diagnostic tool. The virus can only be detected in the blood for a brief period, suggesting that molecular methods alone are not sufficient for case determination. For this, it is preferable to combine both molecular and serological tests. The wide distribution of competent vectors in non-endemic areas, together with global climate change, elicit the spread of RVFV to continents other than Africa, making surveillance activities vital to prevent or to limit the impact of human outbreaks and for a rapid identification of positive cases, making diagnosis a key factor for this achievement. [ABSTRACT FROM AUTHOR]

Published

2024

15. Evaluation of a Combined Live Attenuated Vaccine against Lumpy Skin Disease, Contagious Bovine Pleuropneumonia and Rift Valley Fever.

Author

Bamouh, Zohra, Elarkam, Amal, Elmejdoub, Soufiane, Hamdi, Jihane, Boumart, Zineb, Smith, Greg, Suderman, Matthew, Teffera, Mahder, Wesonga, Hezron, Wilson, Stephen, Watts, Douglas M., Babiuk, Shawn, Pickering, Brad, and Elharrak, Mehdi

Subjects

LUMPY skin disease, RIFT Valley fever, COMBINED vaccines, RESOURCE-limited settings, CERCOPITHECUS aethiops

Abstract

The use of effective vaccines is among the most important strategies for the prevention and progressive control of transboundary infectious animal diseases. However, the use of vaccine is often impeded by the cost, a lack of cold chains and other factors. In resource-limited countries in Africa, one approach to improve coverage and reduce cost is to vaccinate against multiple diseases using combined vaccines. Therefore, the objective of this study was to evaluate a combined vaccine for the prevention and control of Lumpy Skin Disease (LSD), Contagious Bovine Pleuropneumonia (CBPP) and Rift Valley fever (RVF). The LSD and CBPP were formulated as a combined vaccine, and the RVF was formulated separately as live attenuated vaccines. These consisted of a Mycoplasma MmmSC T1/44 strain that was propagated in Hayflick-modified medium, RVF virus vaccine, C13T strain prepared in African green monkey cells (Vero), and the LSDV Neethling vaccine strain prepared in primary testis cells. The vaccines were tested for safety via the subcutaneous route in both young calves and pregnant heifers with no side effect, abortion or teratogenicity. The vaccination of calves induced seroconversions for all three vaccines starting from day 7 post-vaccination (PV), with rates of 50% for LSD, 70% for CBPP and 100% for RVF, or rates similar to those obtained with monovalent vaccines. The challenge of cattle vaccinated with the LSD/CBPP and the RVF vaccine afforded full protection against virulent strains of LSDV and RVFV. A satisfactory level of protection against a CBPP challenge was observed, with 50% of protection at 6 months and 81% at 13 months PV. A mass vaccination trial was performed in four regions of Burkina Faso that confirmed safety and specific antibody responses induced by the vaccines. The multivalent LSD/CBPP+RVF vaccine provides a novel and beneficial approach to the control of the three diseases through one intervention and, therefore, reduces the cost and improves vaccination coverage. [ABSTRACT FROM AUTHOR]

Published

2024

16. Recent Advances in the Epidemiology of Pathogenic Agents.

Author

Chen, Wei-Chuan and Lin, Yusen Eason

Subjects

EPIDEMIOLOGY, CORONAVIRUS disease treatment, MIDDLE East respiratory syndrome, RIFT Valley fever, SARS disease

Abstract

The article discusses recent advances in the epidemiology of pathogenic agents, with a focus on various studies and findings. It highlights the resurgence of syphilis and the global spread of antibiotic resistance, emphasizing the need for improved diagnostic methods and treatment strategies. Other studies explore the genomic structure of SARS-CoV-2 and its receptor-binding mechanisms, providing insights into disease transmission dynamics and potential cross-species transfer. The article also discusses the prevalence of bacterial and fungal co-infections in COVID-19 patients, the complex nature of pathogen co-infections in diarrheal episodes, and the importance of considering genetic predispositions in patients with COVID-19. Additionally, it mentions the World Health Organization's efforts to update the list of priority pathogens and the need for ongoing surveillance and research in the field of epidemiology. [Extracted from the article]

Published

2024

17. An Entomological Investigation during a Recent Rift Valley Fever Epizootic/Epidemic Reveals New Aspects of the Vectorial Transmission of the Virus in Madagascar.

Author

Tantely, Luciano Michaël, Andriamandimby, Soa Fy, Ambinintsoa, Maminirina Fidelis, Raharinirina, Manou Rominah, Rafisandratantsoa, Jean Théophile, Ravalohery, Jean-Pierre, Harimanana, Aina, Ranoelison, Nirina Nantenaina, Irinantenaina, Judickaelle, Ankasitrahana, Miamina Fidy, Ranoaritiana, Dany Bakoly, Randrianasolo, Laurence, Randremanana, Rindra Vatosoa, Lacoste, Vincent, Dussart, Philippe, and Girod, Romain

Subjects

RIFT Valley fever, AEDES aegypti, INSECT traps, AEDES albopictus, MOSQUITO nets, CULEX, EPIDEMICS

Abstract

A Rift Valley fever (RVF) outbreak occurred in at least five regions of Madagascar in 2021. The aim of this study was to provide an overview of the richness, abundance, ecology, and trophic preferences of mosquitoes in the Mananjary district and to investigate the distribution of mosquitoes that were RT-PCR-positive for RVFV. Three localities were prospected from 26 April to 4 May 2021, using light traps, BG-Sentinel traps baited with an artificial human odor, Muirhead-Thomson pit traps, and indoor pyrethroid spray catches. A total of 2806 mosquitoes belonging to at least 26 species were collected. Of 512 monospecific pools of mosquitoes tested with real-time RT-PCR, RVFV was detected in 37 pools representing 10 mosquito species. The RVFV-positive species were as follows: Aedes albopictus, Ae. argenteopunctatus, Anopheles coustani, An. gambiae s.l., An. mascarensis, An. squamosus/cydippis, Culex antennatus, Cx. decens, Cx. Tritaeniorhynchus, and Uranotaenia spp. Of the 450 tested engorged females, 78.7% had taken a blood meal on humans, 92.9% on cattle, and 71.6% had taken mixed (human–cattle) blood meals. This investigation suggests the potential role of mosquitoes in RVFV transmission within this epizootic/epidemic context and that the human populations at the three study sites were highly exposed to mosquitoes. Therefore, the use of impregnated mosquito nets as an appropriate prevention method is recommended. [ABSTRACT FROM AUTHOR]

Published

2024

18. The Re-Emergence of Rift Valley Fever in Mananjary District, Madagascar in 2021: A Call for Action.

Author

Harimanana, Aina Nirina, Andriamandimby, Soa Fy, Ranoaritiana, Dany Bakoly, Randrianasolo, Laurence, Irinantenaina, Judickaelle, Ranoelison, Nirina Nantenaina, Rafisandrantatsoa, Jean Théophile, Ankasitrahana, Miamina Fidy, Raherinandrasana, Antso Hasina, Andriamahatana, Manuela Vololoniaina, Tantely, Michael Luciano, Girod, Romain, Dussart, Philippe, Lacoste, Vincent, and Randremanana, Rindra Vatosoa

Subjects

RIFT Valley fever, FEVER, IMMUNOGLOBULIN M

Abstract

An epizootic of rift valley fever (RVF) was suspected on 21 February 2021 in various districts of Madagascar, with a lab confirmation on 1 April 2021. A cross-sectional survey aiming to detect cases of RVF in humans and to study the circulation of rift valley fever virus (RVFV) in animals was conducted from 22 April to 4 May 2021 in the district of Mananjary. Blood samples from cattle and humans were tested using serological and molecular techniques. In cattle, the circulation of RVFV was confirmed between 5 February and 4 May 2021. The positivity rates of anti-RVFV IgG and IgM were 60% and 40%, respectively. In humans, the circulation of RVFV was observed from 1 April to 5 May 2021. The positivity rate of RVFV was estimated to be 11.7% by combining the results of the molecular and serological approaches. Of the 103 individuals who agreed to participate in the survey, 3 were determined to be positive by RT-PCR, and 10 had anti-RVFV IgM. Among them, one was positive for both. Given that previous studies have reported the circulation of RVFV during inter-epidemic periods and the occurrence of outbreaks due to imported RVFV in Madagascar, our findings suggest the importance of strengthening RVF surveillance from a "One Health" perspective by conducting syndromic and risk-based surveillance at the national and regional levels. [ABSTRACT FROM AUTHOR]

Published

2024

19. Emergence of Crimean–Congo Hemorrhagic Fever Virus in Eastern Senegal in 2022.

Author

Sene, Ousseynou, Sagne, Samba Niang, Ngom, Déthié, Diagne, Moussa Moise, Badji, Aminata, Khoulé, Aliou, Ndiaye, El Hadji, Sankhe, Safietou, Loucoubar, Cheikh, Diallo, Mawlouth, Weidmann, Manfred, Dia, Ndongo, Simon-Lorière, Etienne, Sall, Yoro, Diop, Boly, Ndiaye, Mamadou, Sakuntabhai, Anavaj, Sall, Amadou Alpha, Faye, Ousmane, and Faye, Oumar

Subjects

*HEMORRHAGIC fever, *GENETIC variation, *RANGELANDS, *RIFT Valley fever, *NUCLEOTIDE sequencing, *SEQUENCE analysis, *TICK infestations

Abstract

Crimean–Congo hemorrhagic fever (CCHF), the most widespread tick-borne viral human infection, poses a threat to global health. In this study, clinical samples collected through national surveillance systems were screened for acute CCHF virus (CCHFV) infection using RT-PCR and for exposure using ELISA. For any CCHF-positive sample, livestock and tick samples were also collected in the neighborhood of the confirmed case and tested using ELISA and RT-PCR, respectively. Genome sequencing and phylogenetic analyses were also performed on samples with positive RT-PCR results. In Eastern Senegal, two human cases and one Hyalomma tick positive for CCHF were identified and a seroprevalence in livestock ranging from 9.33% to 45.26% was detected. Phylogenetic analyses revealed that the human strain belonged to genotype I based on the available L segment. However, the tick strain showed a reassortant profile, with the L and M segments belonging to genotype I and the S segment belonging to genotype III. Our data also showed that our strains clustered with strains isolated in different countries, including Mauritania. Therefore, our findings confirmed the high genetic variability inside the CCHF genotypes and their introduction to Senegal from other countries. They also indicate an increasing CCHF threat in Senegal and emphasize the need to reinforce surveillance using a one-health approach. [ABSTRACT FROM AUTHOR]

Published

2024

20. Evaluation of Inactivation Methods for Rift Valley Fever Virus in Mouse Microglia.

Author

Rangel, Margarita V., Bourguet, Feliza A., Hall, Carolyn I., and Weilhammer, Dina R.

Subjects

RIFT Valley fever, VIRUS inactivation, MICE, MICROGLIA, EVALUATION methodology, AEDES aegypti, FLOW cytometry, PATHOGENIC viruses

Abstract

Rift Valley fever phlebovirus (RVFV) is a highly pathogenic mosquito-borne virus with bioweapon potential due to its ability to be spread by aerosol transmission. Neurological symptoms are among the worst outcomes of infection, and understanding of pathogenesis mechanisms within the brain is limited. RVFV is classified as an overlap select agent by the CDC and USDA; therefore, experiments involving fully virulent strains of virus are tightly regulated. Here, we present two methods for inactivation of live virus within samples derived from mouse microglia cells using commercially available kits for the preparation of cells for flow cytometry and RNA extraction. Using the flow cytometry protocol, we demonstrate key differences in the response of primary murine microglia to infection with fully virulent versus attenuated RVFV. [ABSTRACT FROM AUTHOR]

Published

2024

21. Safety and Efficacy upon Infection in Sheep with Rift Valley Fever Virus ZH548-rA2, a Triple Mutant Rescued Virus.

Author

Moreno, Sandra, Lorenzo, Gema, López-Valiñas, Álvaro, de la Losa, Nuria, Alonso, Celia, Charro, Elena, Núñez, José I., Sánchez-Cordón, Pedro J., Borrego, Belén, and Brun, Alejandro

Subjects

*RIFT Valley fever, *SHEEP, *VIRAL genes, *VIRAL antigens, *VIRUS diseases, *SHEEP diseases

Abstract

The introduction of three single nucleotide mutations into the genome of the virulent RVFV ZH548 strain allows for the rescue of a fully attenuated virus in mice (ZH548-rA2). These mutations are located in the viral genes encoding the RdRp and the non-structural protein NSs. This paper shows the results obtained after the subcutaneous inoculation of ZH548-rA2 in adult sheep and the subsequent challenge with the parental virus (ZH548-rC1). Inoculation with the ZH548-rA2 virus caused no detectable clinical or pathological effect in sheep, whereas inoculation of the parental rC1 virus caused lesions compatible with viral infection characterised by the presence of scattered hepatic necrosis. Viral infection was confirmed via immunohistochemistry, with hepatocytes within the necrotic foci appearing as the main cells immunolabelled against viral antigen. Furthermore, the inoculation of sheep with the rA2 virus prevented the liver damage expected after rC1 virus inoculation, suggesting a protective efficacy in sheep which correlated with the induction of both humoral and cell-mediated immune responses. [ABSTRACT FROM AUTHOR]

Published

2024

22. Computer-Selected Antiviral Compounds: Assessing In Vitro Efficacies against Rift Valley Fever Virus.

Author

Alkan, Cigdem, O'Brien, Terrence, Kenyon, Victor, and Ikegami, Tetsuro

Subjects

*RIFT Valley fever, *ANTIVIRAL agents, *HIGH throughput screening (Drug development), *ZOONOSES, *VIRUS diseases, *VACCINE approval

Abstract

Rift Valley fever is a zoonotic viral disease transmitted by mosquitoes, impacting both humans and livestock. Currently, there are no approved vaccines or antiviral treatments for humans. This study aimed to evaluate the in vitro efficacy of chemical compounds targeting the Gc fusion mechanism. These compounds were identified through virtual screening of millions of commercially available small molecules using a structure-based artificial intelligence bioactivity predictor. In our experiments, a pretreatment with small molecule compounds revealed that 3 out of 94 selected compounds effectively inhibited the replication of the Rift Valley fever virus MP-12 strain in Vero cells. As anticipated, these compounds did not impede viral RNA replication when administered three hours after infection. However, significant inhibition of viral RNA replication occurred upon viral entry when cells were pretreated with these small molecules. Furthermore, these compounds exhibited significant inhibition against Arumowot virus, another phlebovirus, while showing no antiviral effects on tick-borne bandaviruses. Our study validates AI-based virtual high throughput screening as a rational approach for identifying effective antiviral candidates for Rift Valley fever virus and other bunyaviruses. [ABSTRACT FROM AUTHOR]

Published

2024

23. Brilacidin as a Broad-Spectrum Inhibitor of Enveloped, Acutely Infectious Viruses.

Author

Anderson, Carol A., Barrera, Michael D., Boghdeh, Niloufar A., Smith, Miata, Alem, Farhang, and Narayanan, Aarthi

Subjects

ALPHAVIRUSES, VENEZUELAN equine encephalomyelitis, RIFT Valley fever, ENCEPHALITIS viruses, CERCOPITHECUS aethiops, HEMORRHAGIC fever

Abstract

Alphaviruses, belonging to the Togaviridae family, and bunyaviruses, belonging to the Paramyxoviridae family, are globally distributed and lack FDA-approved vaccines and therapeutics. The alphaviruses Venezuelan equine encephalitis virus (VEEV) and eastern equine encephalitis virus (EEEV) are known to cause severe encephalitis, whereas Sindbis virus (SINV) causes arthralgia potentially persisting for years after initial infection. The bunyavirus Rift Valley Fever virus (RVFV) can lead to blindness, liver failure, and hemorrhagic fever. Brilacidin, a small molecule that was designed de novo based on naturally occurring host defensins, was investigated for its antiviral activity against these viruses in human small airway epithelial cells (HSAECs) and African green monkey kidney cells (Veros). This testing was further expanded into a non-enveloped Echovirus, a Picornavirus, to further demonstrate brilacidin's effect on early steps of the viral infectious cycle that leads to inhibition of viral load. Brilacidin demonstrated antiviral activity against alphaviruses VEEV TC-83, VEEV TrD, SINV, EEEV, and bunyavirus RVFV. The inhibitory potential of brilacidin against the viruses tested in this study was dependent on the dosing strategy which necessitated compound addition pre- and post-infection, with addition only at the post-infection stage not eliciting a robust inhibitory response. The inhibitory activity of brilacidin was only modest in the context of the non-enveloped Picornavirus Echovirus, suggesting brilacidin may be less potent against non-enveloped viruses. [ABSTRACT FROM AUTHOR]

Published

2024

24. Mosquito-Borne Arboviruses Occurrence and Distribution in the Last Three Decades in Central Africa: A Systematic Literature Review.

Author

Poungou, Natacha, Sevidzem, Silas Lendzele, Koumba, Aubin Armel, Koumba, Christophe Roland Zinga, Mbehang, Phillipe, Onanga, Richard, Zahouli, Julien Zahouli Bi, Maganga, Gael Darren, Djogbénou, Luc Salako, Borrmann, Steffen, Adegnika, Ayola Akim, Becker, Stefanie C., Mavoungou, Jacques François, and Nguéma, Rodrigue Mintsa

Subjects

ARBOVIRUSES, RIFT Valley fever, MOSQUITO control, WEST Nile virus, YELLOW fever, MOSQUITO vectors, CHIKUNGUNYA virus

Abstract

Arboviruses represent a real public health problem globally and in the Central African subregion in particular, which represents a high-risk zone for the emergence and re-emergence of arbovirus outbreaks. Furthermore, an updated review on the current arbovirus burden and associated mosquito vectors is lacking for this region. To contribute to filling this knowledge gap, the current study was designed with the following objectives: (i) to systematically review data on the occurrence and distribution of arboviruses and mosquito fauna; and (ii) to identify potential spillover mosquito species in the Central African region in the last 30 years. A web search enabled the documentation of 2454 articles from different online databases. The preferred reporting items for systematic reviews and meta-analyses (PRISMA) and the quality of reporting of meta-analyses (QUORUM) steps for a systematic review enabled the selection of 164 articles that fulfilled our selection criteria. Of the six arboviruses (dengue virus (DENV), chikungunya virus (CHIKV), yellow fever virus (YFV), Zika virus (ZIKV), Rift Valley fever virus (RVFV), and West Nile virus (WNV)) of public health concern studied, the most frequently reported were chikungunya and dengue. The entomological records showed >248 species of mosquitoes regrouped under 15 genera, with Anopheles (n = 100 species), Culex (n = 56 species), and Aedes (n = 52 species) having high species diversity. Three genera were rarely represented, with only one species included, namely, Orthopodomyia, Lutzia, and Verrallina, but individuals of the genera Toxorhinchites and Finlayas were not identified at the species level. We found that two Aedes species (Ae. aegypti and Ae. albopictus) colonised the same microhabitat and were involved in major epidemics of the six medically important arboviruses, and other less-frequently identified mosquito genera consisted of competent species and were associated with outbreaks of medical and zoonotic arboviruses. The present study reveals a high species richness of competent mosquito vectors that could lead to the spillover of medically important arboviruses in the region. Although epidemiological studies were found, they were not regularly documented, and this also applies to vector competence and transmission studies. Future studies will consider unpublished information in dissertations and technical reports from different countries to allow their information to be more consistent. A regional project, entitled "Ecology of Arboviruses" (EcoVir), is underway in three countries (Gabon, Benin, and Cote d'Ivoire) to generate a more comprehensive epidemiological and entomological data on this topic. [ABSTRACT FROM AUTHOR]

Published

2024

25. Emerging Zoonotic Diseases among Pastoral Communities of Caia and Búzi Districts, Sofala, Mozambique: Evidence of Antibodies against Brucella, Leptospira, Rickettsia, and Crimean-Congo Hemorrhagic Fever Virus.

Author

Oludele, John, Alho, Pascoal, Chongo, Inocêncio, Maholela, Plácida, Magaia, Vlademiro, Muianga, Argentina, Melchior, Bibiana, Isaías, Telma, Gatambire, Aline, Zimba, Edna, Nhavoto, Emídio, Notiço, Paulo, Inguana, Pedro, Cantoria, Juma, António, Virgílio, Monteiro, Vanessa, Ali, Sádia, Inlamea, Osvaldo, and Samo Gudo, Eduardo

Subjects

*RICKETTSIA, *HEMORRHAGIC fever, *LEPTOSPIRA, *BRUCELLA, *ZOONOSES, *RIFT Valley fever, *IMMUNOGLOBULINS

Abstract

Background: Emerging zoonotic diseases are an increasing threat to public health. There is little data on the seroprevalence of zoonotic diseases among pastoralists in the country. We aim to carry out a cross-sectional study on the prevalence of major zoonotic diseases among pastoral communities in the Caia and Búzi districts. Methods: Between January and December 2018, a questionnaire was used to solicit socio-demographic data from consenting pastoralists with the collection of blood samples in the Caia and Búzi districts of the Sofala province. All samples were tested using ELISA commercial reagents for the detection of IgM antibodies against Brucella and Leptospira. Likewise, IgM and IgG antibodies against Rickettsia and CCHFV were determined using ELISA kits. Results: A total of 218 samples were tested, of which 43.5% (95/218) were from the district of Caia and 56.4% (123/218) from the Búzi district. Results from both districts showed that the seroprevalence of IgM antibodies against Brucella and Leptospira was 2.7% (6/218) and 30.3% (67/218), respectively. Positivity rates for IgM and IgG anti-Rickettsia and CCHFV were 8.7% (19/218), 2.7% (6/218), 4.1% (9/218), and 0.9% (2/218), respectively. Conclusions: Results from our study showed evidence of antibodies due to exposure to Brucella, Leptospira, Rickettsia, and CCHFV with antibodies against Leptospira and Rickettsia being the most prevalent. Hence, laboratory diagnosis of zoonotic diseases is essential in the early detection of outbreaks, the identification of silent transmission, and the etiology of non-febrile illness in a pastoral community. There is a need to develop public health interventions that will reduce the risk of transmission. [ABSTRACT FROM AUTHOR]

Published

2023

26. Pathogenesis of Rift Valley Fever Virus in a BALB/c Mouse Model Is Affected by Virus Culture Conditions and Sex of the Animals.

Author

Graham, Victoria A., Easterbrook, Linda, Kennedy, Emma, Rayner, Emma, Findlay-Wilson, Stephen, Flett, Lucy, Wise, Emma Louise, Treagus, Samantha, Fotheringham, Susan, Kempster, Sarah, Almond, Neil, and Dowall, Stuart

Subjects

*RIFT Valley fever, *LABORATORY mice, *MICE, *ANIMAL disease models, *VIRAL tropism, *PATHOGENESIS

Abstract

Rift Valley fever virus (RVFV) is a mosquito-borne zoonotic pathogen causing disease in livestock and humans. Whilst initially restricted to the African continent, recent spread to the Arabian Peninsula has highlighted the likelihood of entry into new regions. Due to the absence of a regulatory-approved human vaccine, work is ongoing to develop and assess countermeasures. As such, small animal models play a pivotal role in providing information on disease pathogenesis and elucidating which intervention strategies confer protection. To develop and establish the BALB/c mouse model, we challenged mice with RVFV grown from two separate cell lines: one derived from mosquitoes (C6/36) and the other mammalian derived (Vero E6). Following infection, we assessed the clinical course of disease progression at days 1 and 3 post-challenge and evaluated viral tropism and immune analytes. The results demonstrated that RVFV infection was affected by the cell line used to propagate the challenge virus, with those grown in insect cells resulting in a more rapid disease progression. The lowest dose that caused uniform severe disease remained the same across both virus preparations. In addition, to demonstrate reproducibility, the lowest dose was used for a subsequent infection study using male and female animals. The results further demonstrated that male mice succumbed to infection more rapidly than their female counterparts. Our results establish an RVFV mouse model and key parameters that affect the course of disease progression in BALB/c mice. [ABSTRACT FROM AUTHOR]

Published

2023

27. Rapid On-Site Detection of Arboviruses by a Direct RT-qPCR Assay.

Author

Mhamadi, Moufid, Mencattelli, Giulia, Gaye, Alioune, Ndiaye, El Hadji, Sow, Aïssatou Aïcha, Faye, Martin, Ndione, Marie Henriette Dior, Diagne, Moussa Moïse, Mhamadi, Moundhir, Faye, Ousmane, Weidmann, Manfred, Faye, Oumar, Diallo, Mawlouth, and Diagne, Cheikh Tidiane

Subjects

RIFT Valley fever, ARBOVIRUS diseases, ARBOVIRUSES, VIRAL transmission, POLYMERASE chain reaction, COMMUNICABLE diseases

Abstract

Arthropod-borne diseases currently constitute a source of major health concerns worldwide. They account for about 50% of global infectious diseases and cause nearly 700,000 deaths every year. Their rapid increase and spread constitute a huge challenge for public health, highlighting the need for early detection during epidemics, to curtail the virus spread, and to enhance outbreak management. Here, we compared a standard quantitative polymerase chain reaction (RT-qPCR) and a direct RT-qPCR assay for the detection of Zika (ZIKV), Chikungunya (CHIKV), and Rift Valley Fever (RVFV) viruses from experimentally infected-mosquitoes. The direct RT-qPCR could be completed within 1.5 h and required 1 µL of viral supernatant from homogenized mosquito body pools. Results showed that the direct RT-qPCR can detect 85.71%, 89%, and 100% of CHIKV, RVFV, and ZIKV samples by direct amplifications compared to the standard method. The use of 1:10 diluted supernatant is suggested for CHIKV and RVFV direct RT-qPCR. Despite a slight drop in sensitivity for direct PCR, our technique is more affordable, less time-consuming, and provides a better option for qualitative field diagnosis during outbreak management. It represents an alternative when extraction and purification steps are not possible because of insufficient sample volume or biosecurity issues. [ABSTRACT FROM AUTHOR]

Published

2023

28. New Trends in Vaccine Characterization, Formulations, and Development.

Author

Kumar, Ravinder

Subjects

PEPTIDE vaccines, VACCINES, LUMPY skin disease, RIFT Valley fever, HEALTH attitudes

Abstract

This document is a list of references cited in various scientific articles related to vaccine development and delivery. The articles cover a wide range of topics, including the use of yeast-based virus-like particles as a platform for vaccine development, trends in COVID-19 vaccine development, and evaluation of a combined live attenuated vaccine for multiple diseases. Other topics include T cell vaccinology, protein subunit vaccines against COVID-19, and the acceptance and attitudes toward COVID-19 vaccines. The document also includes information on the use of yeast as a carrier for drug delivery and vaccine construction, antifungal vaccines, thermostable vaccines, and the global distribution of COVID-19 vaccines. It is important to note that the statements, opinions, and data in the publications are the responsibility of the individual authors and contributors, not the publisher. [Extracted from the article]

Published

2024

29. Identification of Host Factors for Rift Valley Fever Phlebovirus.

Author

Balaraman, Velmurugan, Indran, Sabarish V., Li, Yonghai, Meekins, David A., Jakkula, Laxmi U. M. R., Liu, Heidi, Hays, Micheal P., Souza-Neto, Jayme A., Gaudreault, Natasha N., Hardwidge, Philip R., Wilson, William C., Weber, Friedemann, and Richt, Juergen A.

Subjects

*RIFT Valley fever, *BUNYAVIRUSES, *ENCEPHALITIS viruses, *VIRAL genes, *VIRAL replication, *ANTIVIRAL agents

Abstract

Rift Valley fever phlebovirus (RVFV) is a zoonotic pathogen that causes Rift Valley fever (RVF) in livestock and humans. Currently, there is no licensed human vaccine or antiviral drug to control RVF. Although multiple species of animals and humans are vulnerable to RVFV infection, host factors affecting susceptibility are not well understood. To identify the host factors or genes essential for RVFV replication, we conducted CRISPR-Cas9 knockout screening in human A549 cells. We then validated the putative genes using siRNA-mediated knock-downs and CRISPR-Cas9-mediated knock-out studies. The role of a candidate gene in the virus replication cycle was assessed by measuring intracellular viral RNA accumulation, and the virus titers were analyzed using plaque assay or TCID50 assay. We identified approximately 900 genes with potential involvement in RVFV infection and replication. Further evaluation of the effect of six genes on viral replication using siRNA-mediated knock-downs revealed that silencing two genes (WDR7 and LRP1) significantly impaired RVFV replication. For further analysis, we focused on the WDR7 gene since the role of the LRP1 gene in RVFV replication was previously described in detail. WDR7 knockout A549 cell lines were generated and used to dissect the effect of WRD7 on a bunyavirus, RVFV, and an orthobunyavirus, La Crosse encephalitis virus (LACV). We observed significant effects of WDR7 knockout cells on both intracellular RVFV RNA levels and viral titers. At the intracellular RNA level, WRD7 affected RVFV replication at a later phase of its replication cycle (24 h) when compared with the LACV replication, which was affected in an earlier replication phase (12 h). In summary, we identified WDR7 as an essential host factor for the replication of two different viruses, RVFV and LACV, both of which belong to the Bunyavirales order. Future studies will investigate the mechanistic role through which WDR7 facilitates phlebovirus replication. [ABSTRACT FROM AUTHOR]

Published

2023

30. A Novel Quadruple Gene-Deleted BoHV-1-Vectored RVFV Subunit Vaccine Induces Humoral and Cell-Mediated Immune Response against Rift Valley Fever in Calves.

Author

Pavulraj, Selvaraj, Stout, Rhett W., Barras, Elise D., Paulsen, Daniel B., and Chowdhury, Shafiqul I.

Subjects

*RIFT Valley fever, *GRANULOCYTE-macrophage colony-stimulating factor, *MONONUCLEAR leukocytes, *BOVINE viral diarrhea virus, *CALVES, *VIRAL vaccines, *HEMORRHAGIC fever

Abstract

Rift Valley fever virus (RVFV) is considered to be a high biodefense priority based on its threat to livestock and its ability to cause human hemorrhagic fever. RVFV-infected livestock are also a significant risk factor for human infection by direct contact with contaminated blood, tissues, and aborted fetal materials. Therefore, livestock vaccination in the affected regions has the direct dual benefit and one-health approach of protecting the lives of millions of animals and eliminating the risk of severe and sometimes lethal human Rift Valley fever (RVF) disease. Recently, we have developed a bovine herpesvirus type 1 (BoHV-1) quadruple gene mutant virus (BoHV-1qmv) vector that lacks virulence and immunosuppressive properties due to the deletion of envelope proteins UL49.5, glycoprotein G (gG), gE cytoplasmic tail, and US9 coding sequences. In the current study, we engineered the BoHV-1qmv further by incorporating a chimeric gene sequence to express a proteolytically cleavable polyprotein: RVFV envelope proteins Gn ectodomain sequence fused with bovine granulocyte-macrophage colony-stimulating factor (GMCSF) and Gc, resulting in a live BoHV-1qmv-vectored subunit vaccine against RVFV for livestock. In vitro, the resulting recombinant virus, BoHV-1qmv Sub-RVFV, was replicated in cell culture with high titers. The chimeric Gn-GMCSF and Gc proteins expressed by the vaccine virus formed the Gn–Gc complex. In calves, the BoHV-1qmv Sub-RVFV vaccination was safe and induced moderate levels of the RVFV vaccine strain, MP12-specific neutralizing antibody titers. Additionally, the peripheral blood mononuclear cells from the vaccinated calves had six-fold increased levels of interferon-gamma transcription compared with that of the BoHV-1qmv (vector)-vaccinated calves when stimulated with heat-inactivated MP12 antigen in vitro. Based on these findings, we believe that a single dose of BoHV-1qmv Sub-RVFV vaccine generated a protective RVFV-MP12-specific humoral and cellular immune response. Therefore, the BoHV-1qmv sub-RVFV can potentially be a protective subunit vaccine for cattle against RVFV. [ABSTRACT FROM AUTHOR]

Published

2023

31. Dishevelled Has Anti-Viral Activity in Rift Valley Fever Virus Infected Aedes aegypti.

Author

Smith, Christian B., Hodges, Natasha F., Kading, Rebekah C., and Campbell, Corey L.

Subjects

*RIFT Valley fever, *AEDES aegypti, *GENE expression, *CULEX, *INFECTIOUS disease transmission, *INSECTICIDE resistance, *MOSQUITO control

Abstract

Mosquitoes in the genera Aedes and Culex are vectors of Rift Valley fever virus (RVFV), which emerges in periodic epidemics in Africa and Saudi Arabia. Factors that influence the transmission dynamics of RVFV are not well characterized. To address this, we interrogated mosquito host-signaling responses through analysis of differentially expressed genes (DEGs) in two mosquito species with marked differences in RVFV vector competence: Aedes aegypti (Aae, low competence) and Culex tarsalis (Cxt, high competence). Mosquito–host transcripts related to three different signaling pathways were investigated. Selected genes from the Wingless (Wg, WNT-beta-catenin) pathway, which is a conserved regulator of cell proliferation and differentiation, were assessed. One of these, dishevelled (DSH), differentially regulates progression/inhibition of the WNT and JNK (c-Jun N-terminal Kinase) pathways. A negative regulator of the JNK-signaling pathway, puckered, was also assessed. Lastly, Janus kinase/signal transducers and activators of transcription (JAK-STAT) are important for innate immunity; in this context, we tested domeless levels. Here, individual Aae and Cxt were exposed to RVFV MP-12 via oral bloodmeals and held for 14 days. Robust decreases in DEGs in both Aae and Cxt were observed. In particular, Aae DSH expression, but not Cxt DSH, was correlated to the presence/absence of viral RNA at 14 days post-challenge (dpc). Moreover, there was an inverse relationship between the viral copy number and aaeDSH expression. DSH silencing resulted in increased viral copy numbers compared to controls at 3 dpc, consistent with a role for aaeDSH in antiviral immunity. Analysis of cis-regulatory regions for the genes of interest revealed clues to upstream regulation of these pathways. [ABSTRACT FROM AUTHOR]

Published

2023

32. Arthropod-Borne Viruses in Mauritania: A Literature Review.

Author

El Ghassem, Abdallahi, Abdoullah, Bedia, Deida, Jemila, Ould Lemrabott, Mohamed Aly, Ouldabdallahi Moukah, Mohamed, Ould Ahmedou Salem, Mohamed Salem, Briolant, Sébastien, Basco, Leonardo K., Ould Brahim, Khyarhoum, and Ould Mohamed Salem Boukhary, Ali

Subjects

ARBOVIRUS diseases, RIFT Valley fever, ARBOVIRUSES, LITERATURE reviews, WEST Nile fever, ZOONOSES, INSECTICIDE resistance

Abstract

During the past four decades, recurrent outbreaks of various arthropod-borne viruses have been reported in Mauritania. This review aims to consolidate the current knowledge on the epidemiology of the major arboviruses circulating in Mauritania. Online databases including PubMed and Web of Science were used to retrieve relevant published studies. The results showed that numerous arboviral outbreaks of variable magnitude occurred in almost all 13 regions of Mauritania, with Rift Valley fever (RVF), Crimean–Congo hemorrhagic fever (CCHF), and dengue (DEN) being the most common infections. Other arboviruses causing yellow fever (YF), chikungunya (CHIK), o'nyong-nyong (ONN), Semliki Forest (SF), West Nile fever (WNF), Bagaza (BAG), Wesselsbron (WSL), and Ngari (NRI) diseases have also been found circulating in humans and/or livestock in Mauritania. The average case fatality rates of CCHF and RVF were 28.7% and 21.1%, respectively. RVF outbreaks have often occurred after unusually heavy rainfalls, while CCHF epidemics have mostly been reported during the dry season. The central and southeastern regions of the country have carried the highest burden of RVF and CCHF. Sheep, cattle, and camels are the main animal reservoirs for the RVF and CCHF viruses. Culex antennatus and Cx. poicilipes mosquitoes and Hyalomma dromedarii, H. rufipes, and Rhipicephalus everesti ticks are the main vectors of these viruses. DEN outbreaks occurred mainly in the urban settings, including in Nouakchott, the capital city, and Aedes aegypti is likely the main mosquito vector. Therefore, there is a need to implement an integrated management strategy for the prevention and control of arboviral diseases based on sensitizing the high-risk occupational groups, such as slaughterhouse workers, shepherds, and butchers for zoonotic diseases, reinforcing vector surveillance and control, introducing rapid point-of-care diagnosis of arboviruses in high-risk areas, and improving the capacities to respond rapidly when the first signs of disease outbreak are identified. [ABSTRACT FROM AUTHOR]

Published

2023

33. Surveillance, Prevention, Evolution and Control of Emerging Viruses: A 2022 Editorial Update.

Author

Vaslin, Maite Freitas Silva, Arruda, Luciana de Barros, and Campos, Fabricio Souza

Subjects

*AVIAN influenza A virus, *POULTRY farms, *ANIMAL communities, *RESPIRATORY diseases, *ANIMAL tracks, *LUMPY skin disease, *RIFT Valley fever

Abstract

The novel virus called the Peixe-Boi virus (PBV) corroborates the circulation of henipa-like viruses far from Africa, Asia, and Australia. Also, new isolates of high pathogenic H5N1 influenza virus, epizootic hemorrhagic disease virus strain (EHDV), and Lumpy skin disease virus (LSDV) were reported in wild birds and poultry, cattle, and yaks [[5], [7]]. The Special Issue "Emerging Viruses: Surveillance, Prevention, Evolution and Control" has been published annually by I Viruses i , since 2019, highlighting the increasing effort of the scientific community for the surveillance and further research of new emerging or re-emerging viruses. Using 74 primer pairs matching the three genomic segments of the entire Rift Valley fever virus (RVFV) (genus I Phlebovirus i , family I Phenuiviridae i ) genome, they obtained around 80-90% of the genome covering of the virus from not enriched samples. [Extracted from the article]

Published

2023

34. Novel Antiviral Agents: Synthesis, Molecular Modelling Studies and Biological Investigation.

Author

Brogi, Simone

Subjects

*ANTIVIRAL agent synthesis, *CXCR4 receptors, *VIRUS diseases, *MIDDLE East respiratory syndrome, *RIFT Valley fever

Abstract

Therefore, it is critical to identify novel antiviral drugs, vaccines, therapeutic strategies primarily based on the repurposing of marketed drugs, and early diagnostic and prevention strategies, considering the likelihood of future outbreaks. Mohammad and colleagues developed a virtual screening protocol for identifying possible antiviral agents targeting SARS-CoV-2 NSP3 macrodomain-1, which plays a crucial role in viruses' attack on the innate immune system. The findings showed that MST is an extremely accurate method for investigating protein-ligand and/or protein-protein interactions in anti-coronavirus drug discovery, indicating that it is a perfect technique for examining viral variations to develop effective antivirals. Studies are being conducted to determine if effective antiviral treatment with direct-acting antiviral drugs will result in improved survival in individuals with advanced CKD [[14]]. [Extracted from the article]

Published

2023

35. Melittin-Related Peptides Interfere with Sandfly Fever Naples Virus Infection by Interacting with Heparan Sulphate.

Author

Chianese, Annalisa, Zannella, Carla, Palma, Francesca, Di Clemente, Laura, Monti, Alessandra, Doti, Nunzianna, De Filippis, Anna, and Galdiero, Massimiliano

Subjects

VIRUS diseases, PEPTIDES, RIFT Valley fever, FEVER, SULFATES

Abstract

Emerging viruses pose an important global public health challenge, and early action is needed to control their spread. The Bunyaviridae family contains a great number of arboviruses which are potentially pathogenic for humans. For example, phleboviruses affect a large range of hosts, including humans and animals. Some infections usually have an asymptomatic course, but others lead to severe complications, such as Toscana virus, which is able to cause meningitis and encephalitis. Unfortunately, to date, no vaccines or antiviral treatments have been found. In the present study, we evaluated the effect of melittin-related peptides, namely the frog-derived RV-23 and AR-23, on sandfly fever Naples virus infection in vitro. Both peptides exhibited a strong antiviral activity by targeting the viral particles and blocking the virus–cell interaction. Their action was directed to an early phase of SFNV infection, in particular at viral adsorption on host cells, by interfering with the binding of common glycosaminoglycan receptors. Given the better antimicrobial behavior of AR-23 and RV-23 compared to melittin in terms of selectivity, our studies expand our understanding of the potential of these peptides as antimicrobials and stimulate further investigations in the direction of novel antiviral strategies against phlebovirus infection. [ABSTRACT FROM AUTHOR]

Published

2023

36. Rift Valley Fever Virus—Infection, Pathogenesis and Host Immune Responses.

Author

Nair, Niranjana, Osterhaus, Albert D. M. E., Rimmelzwaan, Guus F., and Prajeeth, Chittappen Kandiyil

Subjects

RIFT Valley fever, IMMUNE response, INFECTION prevention, FEVER, PREVENTIVE medicine, PESTE des petits ruminants, ANIMAL species, T cells

Abstract

Rift Valley Fever Virus is a mosquito-borne phlebovirus causing febrile or haemorrhagic illness in ruminants and humans. The virus can prevent the induction of the antiviral interferon response through its NSs proteins. Mutations in the NSs gene may allow the induction of innate proinflammatory immune responses and lead to attenuation of the virus. Upon infection, virus-specific antibodies and T cells are induced that may afford protection against subsequent infections. Thus, all arms of the adaptive immune system contribute to prevention of disease progression. These findings will aid the design of vaccines using the currently available platforms. Vaccine candidates have shown promise in safety and efficacy trials in susceptible animal species and these may contribute to the control of RVFV infections and prevention of disease progression in humans and ruminants. [ABSTRACT FROM AUTHOR]

Published

2023

37. Zoo-Sanitary Situation Assessment, an Initial Step in Country Disease Prioritization Process: Systematic Review and Meta-Analysis from 2000 to 2020 in Cameroon.

Author

Mouliom Mouiche, Mohamed Moctar, Nguemou Wafo, Eugenie Elvire, Mpouam, Serge Eugene, Moffo, Frédéric, Kameni Feussom, Jean Marc, Njayou Ngapagna, Arouna, Mfopit, Youssouf Mouliom, Saegerman, Claude, and Abdoulmoumini, Mamoudou

Subjects

PESTE des petits ruminants, RIFT Valley fever, ANIMAL disease control, AFRICAN swine fever, ANIMAL diseases

Abstract

To prevent and/or control infectious diseases in animal and human health, an appropriate surveillance system based on suitable up-to-date epidemiological data is required. The systematic review protocol was designed according to the PRISMA statement to look at the available data on infectious diseases of livestock in Cameroon from 2000–2020. Data were searched through online databases. Grey literature was comprised of dissertations and theses from veterinary higher education institutions in Cameroon. A random-effects model was used to calculate pooled prevalence using Comprehensive Meta-Analysis Software. Based on disease prevalence, major infectious diseases of livestock in Cameroon were gastrointestinal parasitosis (57.4% in cattle, 67.2% in poultry, 88% in pigs), hemoparasites (21.6% in small ruminants, 19.7% in cattle), bovine pasteurellosis (55.5%), fowl salmonellosis (48.2%), small ruminant plague (39.7%), foot-and-mouth disease (34.5% in cattle), and African swine fever (18.9%). Furthermore, other important endemic zoonoses in the country included: Rift Valley fever (10.9% in cattle, 3.7% in small ruminants), brucellosis (7% in cattle, 8% in pigs), bovine tuberculosis (4.7% in cattle), hepatitis E virus (8.4% in pigs) and bovine leptospirosis (2.5%). Most of the retrieved research were carried out in the Adamawa, Northwest, and West regions of Cameroon. The evaluation of existing data as evidence, albeit publication-specific, is an important step towards the process of prioritizing animal diseases, including zoonoses. [ABSTRACT FROM AUTHOR]

Published

2023

38. Detection of Anti-Rift Valley Fever Virus Antibodies in Serum Samples of Patients with Suspected Arbovirus Infection.

Author

Lapa, Daniele, Specchiarello, Eliana, Francalancia, Massimo, Girardi, Enrico, Maggi, Fabrizio, and Garbuglia, Anna Rosa

Subjects

COCCIDIOIDOMYCOSIS, VIRAL antibodies, ARBOVIRUS diseases, RIFT Valley fever, IMMUNOGLOBULINS, COMMUNICABLE diseases, IMMUNOGLOBULIN M

Abstract

The definitive diagnosis of the Rift Valley fever virus (RVFV) requires a form of testing that is available only in reference laboratories. It includes indirect immunofluorescence assay (IFA), the serum neutralization assay (NA), and real-time PCR. Therefore, often, no attempts are made to detect it, even among travelers from endemic areas. In this study, the presence of anti-RVFV IgG and IgM was retrospectively screened in stored serum samples from people who were admitted with arbovirus symptoms at the National Institute for Infectious Diseases (INMI) L. Spallanzani, Rome, Italy. Overall, 80 residual serum samples were anonymized, and sub-aliquots were prepared and tested for anti-RVFV IgG and IgM. A serum neutralization assay was used as a confirmatory test. There was a positive result in eight out of 80 samples (10%) for anti-RVFV IgG, with titers ranging from 1:40 up to 1:1280. Three of eight (2.6%) samples were confirmed as seropositive through an in-house serum neutralization assay, with antibody titers ranging from 1:10 to 1:160. All samples resulted negative for anti-RVFV IgM and RVFV RNA when tested by IFA and real-time RT-PCR, respectively. Our data highlight that several RVFV infections can possibly escape routine virological diagnosis, which suggests RVFV testing should be set up in order to monitor virus prevalence. [ABSTRACT FROM AUTHOR]

Published

2023

39. Alternative Splicing of RIOK3 Engages the Noncanonical NFκB Pathway during Rift Valley Fever Virus Infection.

Author

Bisom, Thomas Charles, Smelser, Hope, Lanchy, Jean-Marc, and Lodmell, J. Stephen

Subjects

*RIFT Valley fever, *ALTERNATIVE RNA splicing, *VIRUS diseases, *RNA virus infections, *TYPE I interferons, *INTERFERONS

Abstract

Although the noncanonical NFκB pathway was originally identified as a cellular pathway contributing to lymphoid organogenesis, in the past 20 years, its involvement in innate immunity has become more appreciated. In particular, the noncanonical NFκB pathway has been found to be activated and even exploited by some RNA viruses during infection. Intriguingly, activation of this pathway has been shown to have a role in disrupting transcription of type 1 interferon (IFN), suggesting a rationale for why this response could be co-opted by some viruses. Rift Valley fever virus (RVFV) is a trisegmented ambisense RNA virus that poses a considerable threat to domestic livestock and human health. Previously, we showed the atypical kinase RIOK3 is important for mounting an IFN response to RVFV infection of human epithelial cells, and shortly following infection with RVFV (MP12 strain), RIOK3 mRNA is alternatively spliced to its X2 isoform that encodes a truncated RIOK3 protein. Alternative splicing of RIOK3 mRNA has an inhibitory effect on the IFN response but also stimulates an NFκB-mediated inflammatory response. Here, we demonstrate alternative splicing of RIOK3 mRNA is associated with activation of the noncanonical NFκB pathway and suggest this pathway is co-opted by RVFV (MP12) to enhance viral success during infection. [ABSTRACT FROM AUTHOR]

Published

2023

40. Evidence of Rift Valley Fever Virus Circulation in Livestock and Herders in Southern Ghana.

Author

Johnson, Sherry Ama Mawuko, Asmah, Richard, Awuni, Joseph Adongo, Tasiame, William, Mensah, Gloria Ivy, Paweska, Janusz T., Weyer, Jacqueline, Hellferscee, Orienka, and Thompson, Peter N.

Subjects

*RIFT Valley fever, *VETERINARY virology, *HERDERS, *IMMUNOGLOBULINS, *ZOONOSES, *LIVESTOCK farms

Abstract

Rift Valley fever (RVF) is a re-emerging zoonotic disease of domestic ruminants and humans. While neighbouring countries have reported outbreaks of RVF, Ghana has not yet identified any cases. The aim of this study was to determine whether RVF virus (RVFV) was circulating in livestock and herders in the southern part of Ghana, to estimate its seroprevalence, and to identify associated risk factors. The study surveyed 165 livestock farms randomly selected from two districts in southern Ghana. Serum samples of 253 goats, 246 sheep, 220 cattle, and 157 herdsmen were tested to detect IgG and IgM antibodies against RVFV. The overall seroprevalence of anti-RVF antibodies in livestock was 13.1% and 30.9% of farms had RVFV seropositive animals. The species-specific prevalence was 24.1% in cattle, 8.5% in sheep, and 7.9% in goats. A RVFV IgG seroprevalence of 17.8% was found among the ruminant herders, with 8.3% of all herders being IgM positive. RVFV was shown, for the first time, to have been circulating in southern Ghana, with evidence of a recent outbreak in Kwahu East; however, it was clinically undetected despite significant recent human exposure. A One Health approach is recommended to better understand RVF epidemiology and socio-economic impact in Ghana. [ABSTRACT FROM AUTHOR]

Published

2023

41. Latest Advances in Arbovirus Diagnostics.

Author

Varghese, Jano, De Silva, Imesh, and Millar, Douglas S.

Subjects

WEST Nile virus, RIFT Valley fever, JAPANESE encephalitis viruses, YELLOW fever, ARBOVIRUS diseases, DENGUE viruses

Abstract

Arboviruses are a diverse family of vector-borne pathogens that include members of the Flaviviridae, Togaviridae, Phenuviridae, Peribunyaviridae, Reoviridae, Asfarviridae, Rhabdoviridae, Orthomyxoviridae and Poxviridae families. It is thought that new world arboviruses such as yellow fever virus emerged in the 16th century due to the slave trade from Africa to America. Severe disease-causing viruses in humans include Japanese encephalitis virus (JEV), yellow fever virus (YFV), dengue virus (DENV), West Nile virus (WNV), Zika virus (ZIKV), Crimean–Congo hemorrhagic fever virus (CCHFV), severe fever with thrombocytopenia syndrome virus (SFTSV) and Rift Valley fever virus (RVFV). Numerous methods have been developed to detect the presence of these pathogens in clinical samples, including enzyme-linked immunosorbent assays (ELISAs), lateral flow assays (LFAs) and reverse transcriptase–polymerase chain reaction (RT-PCR). Most of these assays are performed in centralized laboratories due to the need for specialized equipment, such as PCR thermal cyclers and dedicated infrastructure. More recently, molecular methods have been developed which can be performed at a constant temperature, termed isothermal amplification, negating the need for expensive thermal cycling equipment. In most cases, isothermal amplification can now be carried out in as little as 5–20 min. These methods can potentially be used as inexpensive point of care (POC) tests and in-field deployable applications, thus decentralizing the molecular diagnosis of arboviral disease. This review focuses on the latest developments in isothermal amplification technology and detection techniques that have been applied to arboviral diagnostics and highlights future applications of these new technologies. [ABSTRACT FROM AUTHOR]

Published

2023

42. Mechanism of Immune Evasion in Mosquito-Borne Diseases.

Author

Bhattacharjee, Swagato, Ghosh, Debanjan, Saha, Rounak, Sarkar, Rima, Kumar, Saurav, Khokhar, Manoj, and Pandey, Rajan Kumar

Subjects

RIFT Valley fever, WEST Nile fever, ZIKA virus infections, NON-communicable diseases, JAPANESE B encephalitis, MOSQUITO control

Abstract

In recent decades, mosquito-borne illnesses have emerged as a major health burden in many tropical regions. These diseases, such as malaria, dengue fever, chikungunya, yellow fever, Zika virus infection, Rift Valley fever, Japanese encephalitis, and West Nile virus infection, are transmitted through the bite of infected mosquitoes. These pathogens have been shown to interfere with the host's immune system through adaptive and innate immune mechanisms, as well as the human circulatory system. Crucial immune checkpoints such as antigen presentation, T cell activation, differentiation, and proinflammatory response play a vital role in the host cell's response to pathogenic infection. Furthermore, these immune evasions have the potential to stimulate the human immune system, resulting in other associated non-communicable diseases. This review aims to advance our understanding of mosquito-borne diseases and the immune evasion mechanisms by associated pathogens. Moreover, it highlights the adverse outcomes of mosquito-borne disease. [ABSTRACT FROM AUTHOR]

Published

2023

43. Rift Valley Fever Virus Primes Immune Responses in Aedes aegypti Cells.

Author

Laureti, Mathilde, Lee, Rui-Xue, Bennett, Amelia, Wilson, Lucas Aladar, Sy, Victoria Elena, Kohl, Alain, and Dietrich, Isabelle

Subjects

RIFT Valley fever, AEDES aegypti, IMMUNE response, PATTERN perception receptors, RNA interference, INSECTICIDE resistance, MOSQUITO control, AVIAN influenza

Abstract

The ongoing global emergence of arthropod-borne (arbo) viruses has accelerated research into the interactions of these viruses with the immune systems of their vectors. Only limited information exists on how bunyaviruses, such as Rift Valley fever virus (RVFV), are sensed by mosquito immunity or escape detection. RVFV is a zoonotic phlebovirus (Bunyavirales; Phenuiviridae) of veterinary and human public health and economic importance. We have shown that the infection of mosquitoes with RVFV triggers the activation of RNA interference pathways, which moderately restrict viral replication. Here, we aimed to better understand the interactions between RVFV and other vector immune signaling pathways that might influence RVFV replication and transmission. For this, we used the immunocompetent Aedes aegypti Aag2 cell line as a model. We found that bacteria-induced immune responses restricted RVFV replication. However, virus infection alone did not alter the gene expression levels of immune effectors. Instead, it resulted in the marked enhancement of immune responses to subsequent bacterial stimulation. The gene expression levels of several mosquito immune pattern recognition receptors were altered by RVFV infection, which may contribute to this immune priming. Our findings imply that there is a complex interplay between RVFV and mosquito immunity that could be targeted in disease prevention strategies. [ABSTRACT FROM AUTHOR]

Published

2023

44. Influence of RVFV Infection on Olfactory Perception and Behavior in Drosophila melanogaster.

Author

Bergmann, Stella, Bohn, Maja C., Dornbusch, Susann, Becker, Stefanie C., and Stern, Michael

Subjects

OLFACTORY perception, DROSOPHILA melanogaster, RIFT Valley fever, FLIES as carriers of disease, NITRIC-oxide synthases, ODORS, MOSQUITOES, AEDES aegypti

Abstract

In blood-feeding dipterans, olfaction plays a role in finding hosts and, hence, in spreading pathogens. Several pathogens are known to alter olfactory responses and behavior in vectors. As a mosquito-borne pathogen, Rift Valley Fever Virus (RVFV) can affect humans and cause great losses in livestock. We test the influence of RVFV infection on sensory perception, olfactory choice behavior and activity on a non-biting insect, Drosophila melanogaster, using electroantennograms (EAG), Y-maze, and locomotor activity monitor. Flies were injected with RVFV MP12 strain. Replication of RVFV and its persistence for at least seven days was confirmed by quantitative reverse transcription-PCR (RT-qPCR). One day post injection, infected flies showed weaker EAG responses towards 1-hexanol, vinegar, and ethyl acetate. In the Y-maze, infected flies showed a significantly lower response for 1-hexanol compared to uninfected flies. At days six or seven post infection, no significant difference between infected and control flies could be found in EAG or Y-maze anymore. Activity of infected flies was reduced at both time points. We found an upregulation of the immune-response gene, nitric oxide synthase, in infected flies. An infection with RVFV is able to transiently reduce olfactory perception and attraction towards food-related odors in Drosophila, while effects on activity and immune effector gene expression persist. A similar effect in blood-feeding insects could affect vector competence in RVFV transmitting dipterans. [ABSTRACT FROM AUTHOR]

Published

2023

45. Mosquito-Borne Diseases and Their Control Strategies: An Overview Focused on Green Synthesized Plant-Based Metallic Nanoparticles.

Author

Onen, Hudson, Luzala, Miryam M., Kigozi, Stephen, Sikumbili, Rebecca M., Muanga, Claude-Josué K., Zola, Eunice N., Wendji, Sébastien N., Buya, Aristote B., Balciunaitiene, Aiste, Viškelis, Jonas, Kaddumukasa, Martha A., and Memvanga, Patrick B.

Subjects

*MOSQUITO control, *RIFT Valley fever, *POISONS, *YELLOW fever, *PREVENTIVE medicine, *BIOLOGICAL insecticides

Abstract

Simple Summary: Mosquitoes are the carrier of pathogens that cause common human diseases such as malaria, Dengue, Chikungunya, yellow fever, Zika, and West Nile. The use of chemical and biological insecticides is among the key control tools for reducing mosquito populations at different life stages (i.e., eggs, larvae, pupae, and adults). The weaknesses of these tools, especially those with chemicals, are the high cost of production, and their negative effects on other beneficial organisms such as bees and water-dwelling invasive species. Thus, researchers and academics are searching for new safe and environmentally friendly forms of insecticides. Of late, green synthesized plant-based metallic nanoparticles have attracted great interest as an alternative to traditional insecticides. Typically using metal salts in combination with aqueous plant extracts, the synthesis of these nanoparticles is eco-friendly and relatively cheap. This review aims to report on the currently available knowledge on the development of green synthesized metallic nanoparticles and their performance as repellent, ovicidal, larvicidal, pupicidal, and adulticidal agents against different mosquito species. Mosquitoes act as vectors of pathogens that cause most life-threatening diseases, such as malaria, Dengue, Chikungunya, Yellow fever, Zika, West Nile, Lymphatic filariasis, etc. To reduce the transmission of these mosquito-borne diseases in humans, several chemical, biological, mechanical, and pharmaceutical methods of control are used. However, these different strategies are facing important and timely challenges that include the rapid spread of highly invasive mosquitoes worldwide, the development of resistance in several mosquito species, and the recent outbreaks of novel arthropod-borne viruses (e.g., Dengue, Rift Valley fever, tick-borne encephalitis, West Nile, yellow fever, etc.). Therefore, the development of novel and effective methods of control is urgently needed to manage mosquito vectors. Adapting the principles of nanobiotechnology to mosquito vector control is one of the current approaches. As a single-step, eco-friendly, and biodegradable method that does not require the use of toxic chemicals, the green synthesis of nanoparticles using active toxic agents from plant extracts available since ancient times exhibits antagonistic responses and broad-spectrum target-specific activities against different species of vector mosquitoes. In this article, the current state of knowledge on the different mosquito control strategies in general, and on repellent and mosquitocidal plant-mediated synthesis of nanoparticles in particular, has been reviewed. By doing so, this review may open new doors for research on mosquito-borne diseases. [ABSTRACT FROM AUTHOR]

Published

2023

46. Molecular Tracking of the Origin of Vesicular Stomatitis Outbreaks in 2004 and 2018, Ecuador.

Author

Vasco-Julio, David, Aguilar, Dayana, Maldonado, Alexander, de la Torre, Euclides, Cisneros-Montufar, Maria Soledad, Bastidas-Caldes, Carlos, Navarro, Juan-Carlos, and de Waard, Jacobus H.

Subjects

VESICULAR stomatitis, ZOONOSES, PRODUCTION losses, RIFT Valley fever, VIRUS diseases, MAXIMUM likelihood statistics, PLANT viruses

Abstract

Simple Summary: Vesicular stomatitis (VS) is a viral disease that primarily affects cattle, horses and swine. In affected livestock, the VS virus (VSV) causes painful blister-like lesions in the mouth, on the tongue, lips, nostrils, hooves, and teats and infected animals usually refuse to eat and drink, causing livestock production losses. VS is also a zoonotic disease and can cause influenza-like symptoms in humans. In 2018, Ecuador experienced an outbreak of VS affecting cattle in most of the provinces of the country. Here we determined the phylogenetic relationship among the virus strains isolated in that year. Our analysis suggests different transmission patterns in the major geographic regions of Ecuador; several small and independent outbreaks, most probably transmitted by vectors in the Amazon, and an outbreak caused by the movement of livestock and/or fomites in the Andean and Coastal regions. For better control of future outbreaks, we recommend more research into vectors and vertebrate reservoirs in Ecuador. This can further elucidate the mechanisms of the emergence and re-emergence of the virus. The Vesicular Stomatitis Virus (VSV) is an arbovirus causing vesicular stomatitis (VS) in livestock. There are two serotypes recognized: New Jersey (VSNJV) and Indiana (VSIV). The virus can be transmitted directly by contact or by vectors. In 2018, Ecuador experienced an outbreak of Vesicular Stomatitis (VS) in cattle, caused by VSNJV and VSVIV, with 399 cases reported distributed over 18 provinces. We determined the phylogenetic relationships among 67 strains. For the construction of phylogenetic trees, the viral phosphoprotein gene was sequenced, and trees were constructed based on the Maximum Likelihood method using 2004 outbreak strains from Ecuador (GenBank) and the 2018 sequences (this article). We built a haplotype network for VSNJV to trace the origin of the 2004 and 2018 epizootics through topology and mutation connections. These analyses suggest two different origins, one related to the 2004 outbreak and the other from a transmission source in 2018. Our analysis also suggests different transmission patterns; several small and independent outbreaks, most probably transmitted by vectors in the Amazon, and another outbreak caused by the movement of livestock in the Andean and Coastal regions. We recommend further research into vectors and vertebrate reservoirs in Ecuador to clarify the mechanisms of the reemergence of the virus. [ABSTRACT FROM AUTHOR]

Published

2023

47. Perspectives of Next-Generation Live-Attenuated Rift Valley Fever Vaccines for Animal and Human Use.

Author

Wichgers Schreur, Paul J., Bird, Brian H., Ikegami, Tetsuro, Bermúdez-Méndez, Erick, and Kortekaas, Jeroen

Subjects

RIFT Valley fever, REVERSE genetics, VACCINES, VACCINE safety, VACCINATION, HUMORAL immunity

Abstract

Live-attenuated Rift Valley fever (RVF) vaccines transiently replicate in the vaccinated host, thereby effectively initiating an innate and adaptive immune response. Rift Valley fever virus (RVFV)-specific neutralizing antibodies are considered the main correlate of protection. Vaccination with classical live-attenuated RVF vaccines during gestation in livestock has been associated with fetal malformations, stillbirths, and fetal demise. Facilitated by an increased understanding of the RVFV infection and replication cycle and availability of reverse genetics systems, novel rationally-designed live-attenuated candidate RVF vaccines with improved safety profiles have been developed. Several of these experimental vaccines are currently advancing beyond the proof-of-concept phase and are being evaluated for application in both animals and humans. We here provide perspectives on some of these next-generation live-attenuated RVF vaccines and highlight the opportunities and challenges of these approaches to improve global health. [ABSTRACT FROM AUTHOR]

Published

2023

48. The Use of Drones to Deliver Rift Valley Fever Vaccines in Rwanda: Perceptions and Recommendations.

Author

Griffith, Evan F., Schurer, Janna M., Mawindo, Billy, Kwibuka, Rita, Turibyarive, Thierry, and Amuguni, Janetrix Hellen

Subjects

RIFT Valley fever, VACCINE effectiveness, VACCINES, SUPPLY chains, ANIMAL health

Abstract

Given the recent emergence of Rift Valley Fever (RVF) in Rwanda and its profound impact on livelihoods and health, improving RVF prevention and control strategies is crucial. Vaccinating livestock is one of the most sustainable strategies to mitigate the impact of RVF on health and livelihoods. However, vaccine supply chain constraints severely limit the effectiveness of vaccination programs. In the human health sector, unmanned aerial vehicles, i.e., drones, are increasingly used to improve supply chains and last-mile vaccine delivery. We investigated perceptions of whether delivering RVF vaccines by drone in Rwanda might help to overcome logistical constraints in the vaccine supply chain. We conducted semi-structured interviews with stakeholders in the animal health sector and Zipline employees in Nyagatare District in the Eastern Province of Rwanda. We used content analysis to identify key themes. We found that stakeholders in the animal health sector and Zipline employees believe that drones could improve RVF vaccination in Nyagatare. The primary benefits study participants identified included decreased transportation time, improved cold chain maintenance, and cost savings. [ABSTRACT FROM AUTHOR]

Published

2023

49. Special Issue: "Innate Immunity to Virus Infection, 1st Edition".

Author

Wang, Congcong, Ma, Feng, and Sun, Caijun

Subjects

*VIRUS diseases, *NATURAL immunity, *PORCINE reproductive & respiratory syndrome, *PORCINE epidemic diarrhea virus, *WEST Nile fever, *RIFT Valley fever

Abstract

The research article by Zhang et al. investigated multiple PRR-mediated signaling pathways involved in the anti-PEDV responses. Frequent outbreaks of emerging and re-emerging pathogenic viruses have become one of the major challenges for global public health. These results show that multiple porcine PRR-mediated signaling pathways are involved in PEDV recognition and defense, expanding our understanding of innate immunity responses to PEDV infection. [Extracted from the article]

Published

2023

50. Whole Genome Sequencing Analysis of African Orthobunyavirus Isolates Reveals Naturally Interspecies Segments Recombinations between Bunyamwera and Ngari Viruses.

Author

Mhamadi, Moufid, Dieng, Idrissa, Dolgova, Anna S., Touré, Cheikh Talibouya, Ndiaye, Mignane, Diagne, Moussa Moïse, Faye, Babacar, Gladkikh, Anna S., Dedkov, Vladimir G., Sall, Amadou Alpha, Faye, Ousmane, and Faye, Oumar

Subjects

*WHOLE genome sequencing, *RIFT Valley fever, *SEQUENCE analysis, *GENETIC recombination, *HEMORRHAGIC fever, *ARENAVIRUSES, *REVERSE genetics, *RNA viruses

Abstract

Bunyamwera virus is the prototype of the Bunyamwera serogroup, which belongs to the order Bunyavirales of the Orthobunyavirus genus in the Peribunyaviridae family. Bunyamwera is a negative-sense RNA virus composed of three segments S, M, and L. Genetic recombination is possible between members of this order as it is already documented. Additionally, it can lead to pathogenic or host range improvement, if it occurs with viruses of public health and agricultural importance such as Rift Valley fever virus and Crimea–Congo hemorrhagic fever virus. Here, we characterize five African Orthobunyavirus viruses from different geographical regions. Our results suggest that the five newly characterized strains are identified as Bunyamwera virus strains. Furthermore, two of the five strains sequenced in this study are recombinant strains, as fragments of their segments are carried by Ngari and Bunyamwera strains. Further investigations are needed to understand the functional impact of these recombinations. [ABSTRACT FROM AUTHOR]

Published

2023