Your search keyword '"sendai virus"' showing total 5,973 results

1. Dose-escalation, tolerability, and efficacy of intratumoral and subcutaneous injection of hemagglutinating virus of Japan envelope (HVJ-E) against chemotherapy-resistant malignant pleural mesothelioma: a clinical trial.

Author

Sakura, Kazuma, Kuroyama, Muneyoshi, Shintani, Yasushi, Funaki, Soichiro, Atagi, Shinji, Kadota, Yoshihisa, Kuribayashi, Kozo, Kijima, Takashi, Nakano, Takashi, Nakajima, Toshihiro, Sasai, Masao, Okumura, Meinoshin, and Kaneda, Yasufumi

Subjects

*SENDAI virus, *SUBCUTANEOUS injections, *CLINICAL trials, *DISEASE progression, *MESOTHELIOMA

Abstract

The hemagglutinating virus of Japan envelope (HVJ-E) is an inactivated Sendai virus particle with antitumor effect and inducing antitumor immunity. However, its dosage and efficacy have not been verified. We conducted a phase I clinical study on chemotherapy-resistant malignant pleural mesothelioma (MPM) aiming to determine the recommended dosage for a phase II study through dose-limiting toxicity and evaluate HVJ-E's preliminary efficacy. HVJ-E was administered intratumorally and subcutaneously to the patients with chemotherapy-resistant MPM. While no serious adverse events occurred, known adverse events of HVJ-E were observed. In the preliminary antitumor efficacy using modified response evaluation criteria in solid tumors (RECIST) criteria, three low-dose patients exhibited progressive disease, while all high-dose patients achieved stable disease, yielding disease control rates (DCRs) of 0% and 100%, respectively. Furthermore, the dose-dependent effect of HVJ-E revealed on DCR modified by RECIST and the baseline changes in target lesion size (by CT and SUL-peak; p < 0.05). Comparing targeted lesions receiving intratumoral HVJ-E with non-injected ones, while no clear difference existed at the end of the study, follow-up cases suggested stronger antitumor effects with intratumoral administration. Our findings suggest that HVJ-E could be safely administered to patients with chemotherapy-resistant MPM at both study doses. HVJ-E exhibited some antitumor activity against chemotherapy-resistant MPM, and higher doses tended to have stronger antitumor effects than lower doses. Consequently, a phase II clinical trial with higher HVJ-E doses has been conducted for MPM treatment. Trial registration number: UMIN Clinical Trials Registry (#UMIN000019345). [ABSTRACT FROM AUTHOR]

Published

2024

2. Viral co-detection of influenza virus and other respiratory viruses in hospitalized Brazilian patients during the first three years of the coronavirus disease (COVID)-19 pandemic: an epidemiological profile.

Author

Siqueira, Bianca Aparecida, Bredariol, Ketlyn Oliveira, Boschiero, Matheus Negri, and Lima Marson, Fernando Augusto

Subjects

SARS-CoV-2, EPIDEMIOLOGY, RESPIRATORY syncytial virus, SENDAI virus, VIRUS diseases, INFLUENZA B virus

Abstract

Introduction: In Brazil, few studies were performed regarding the co-detection of respiratory viruses in hospitalized patients. In this way, the study aimed to describe the epidemiological profile of hospitalized patients due to influenza virus infection that presented co-detection with another respiratory virus. Methods: The epidemiological analysis was made by collecting data from Open-Data-SUS. The study comprised patients infected by the influenza A or B virus with positive co-detection of another respiratory virus, such as adenovirus, bocavirus, metapneumovirus, parainfluenza virus (types 1, 2, 3, and 4), rhinovirus, and respiratory syncytial virus (RSV). The markers [gender, age, clinical signs and symptoms, comorbidities, need for intensive care unit (ICU) treatment, and need for ventilatory support] were associated with the chance of death. The data was collected during the first three years of the coronavirus disease (COVID)-19 pandemic--from December 19, 2019, to April 06, 2023. Results: A total of 477 patients were included, among them, the influenza A virus was detected in 400 (83.9%) cases. The co-detection occurred, respectively, for RSV (53.0%), rhinovirus (14.0%), adenovirus (13.4%), parainfluenza virus type 1 (10.7%), parainfluenza virus type 3 (5.2%), metapneumovirus (3.8%), parainfluenza virus type 2 (3.6%), bocavirus (3.4%), and parainfluenza virus type 4 (1.5%). The co-detection rate was higher in the male sex (50.7%), age between 0-12 years of age (65.8%), and white individuals (61.8%). The most common clinical symptoms were cough (90.6%), dyspnea (78.8%), and fever (78.6%). A total of 167 (35.0%) people had at least one comorbidity, mainly cardiopathy (14.3%), asthma (8.4%), and diabetes mellitus (7.3%). The need for ICU treatment occurred in 147 (30.8%) cases, with most of them needing ventilatory support (66.8%), mainly non-invasive ones (57.2%). A total of 33 (6.9%) patients died and the main predictors of death were bocavirus infection (OR = 14.78 [95%CI = 2.84-76.98]), metapneumovirus infection (OR = 8.50 [95%CI = 1.86-38.78]), race (other races vs. white people) (OR = 3.67 [95%CI = 1.39-9.74]), cardiopathy (OR = 3.48 [95%CI = 1.13-10.71]), and need for ICU treatment (OR = 7.64 [95%CI = 2.44-23.92]). Conclusion: Co-detection between the influenza virus and other respiratory viruses occurred, mainly with RSV, rhinovirus, and adenovirus being more common in men, white people, and in the juvenile phase. Co-detection of influenza virus with bocavirus and metapneumovirus was associated with an increased chance of death. Other factors such as race, cardiopathy, and the need for an ICU were also associated with a higher chance of death. [ABSTRACT FROM AUTHOR]

Published

2024

3. Rapid evolution leads to extensive genetic diversification of cattle flu Influenza D virus.

Author

Limaye, Sanket, Lohar, Tejas, Dube, Harita, Ramasamy, Santhamani, Kale, Mohan, Kulkarni-Kale, Urmila, and Kuchipudi, Suresh V.

Subjects

*SENDAI virus, *INFLUENZA viruses, *ANIMAL populations, *RNA viruses, *POPULATION dynamics

Abstract

Influenza D virus (IDV), the cattle flu virus, is a novel multi-host RNA virus, circulating silently worldwide, with widespread seropositivity among US cattle, reaching up to 80% in some areas raising a potential threat of cattle-to-human transmission. Currently, five genetic lineages of IDV have been described, but their evolutionary dynamics have not been studied. Although IDV was first identified in 2011, our comprehensive analysis of all known IDV genomes suggests that the earliest ancestors of IDV likely to have evolved towards the end of the 20th century and D/OK lineage appears to have emerged in 2005. We confirmed a significantly higher substitution rate in IDV than in Influenza C virus, which is consistent with their global distribution and multi-host tropism. We identified multiple sub-populations within the D/OK lineage, highlighting extensive diversification and dissemination. Other findings are evidence for potential reassortment among IDV strains in the USA and transboundary circulation of IDV in Europe with introductions into Danish cattle, some of which potentially originated from France. IDV, an emerging virus with a higher rate of evolution and uncontrolled circulation, could facilitate its adaptation to humans. Our findings underscore the importance of targeted surveillance for IDV in humans and at-risk animal populations. Evolutionary dynamics and population stratification analysis of whole genomes of the cattle flu Influenza D virus reveal its high evolution rate, extensive diversification and global dissemination, stressing the need for targeted surveillance. [ABSTRACT FROM AUTHOR]

Published

2024

4. Varicella-zoster virus recapitulates its immune evasive behaviour in matured hiPSC-derived neurospheroids.

Author

Govaerts, Jonas, Van Breedam, Elise, De Beuckeleer, Sarah, Goethals, Charlotte, D'Incal, Claudio Peter, Di Stefano, Julia, Van Calster, Siebe, Buyle-Huybrecht, Tamariche, Boeren, Marlies, De Reu, Hans, Paludan, Søren R., Thiry, Marc, Lebrun, Marielle, Sadzot-Delvaux, Catherine, Motaln, Helena, Rogelj, Boris, Van Weyenbergh, Johan, De Vos, Winnok H., Berghe, Wim Vanden, and Ogunjimi, Benson

Subjects

TYPE I interferons, STRESS granules, VARICELLA-zoster virus, SENDAI virus, CENTRAL nervous system

Abstract

Varicella-zoster virus (VZV) encephalitis and meningitis are potential central nervous system (CNS) complications following primary VZV infection or reactivation. With Type-I interferon (IFN) signalling being an important first line cellular defence mechanism against VZV infection by the peripheral tissues, we here investigated the triggering of innate immune responses in a human neurallike environment. For this, we established and characterised 5-month matured hiPSC-derived neurospheroids (NSPHs) containing neurons and astrocytes. Subsequently, NSPHs were infected with reporter strains of VZV (VZVeGFPORF23) or Sendai virus (SeVeGFP), with the latter serving as an immune-activating positive control. Live cell and immunocytochemical analyses demonstrated VZVeGFP-ORF23 infection throughout the NSPHs, while SeVeGFP infection was limited to the outer NSPH border. Next, NanoString digital transcriptomics revealed that SeVeGFP-infected NSPHs activated a clear Type-I IFN response, while this was not the case in VZVeGFP-ORF23-infected NSPHs. Moreover, the latter displayed a strong suppression of genes related to IFN signalling and antigen presentation, as further demonstrated by suppression of IL-6 and CXCL10 production, failure to upregulate Type-I IFN activated anti-viral proteins (Mx1, IFIT2 and ISG15), as well as reduced expression of CD74, a key-protein in the MHC class II antigen presentation pathway. Finally, even though VZVeGFP-ORF23- infection seems to be immunologically ignored in NSPHs, its presence does result in the formation of stress granules upon long-term infection, as well as disruption of cellular integrity within the infected NSPHs. Concluding, in this study we demonstrate that 5-month matured hiPSC-derived NSPHs display functional innate immune reactivity towards SeV infection, and have the capacity to recapitulate the strong immune evasive behaviour towards VZV. [ABSTRACT FROM AUTHOR]

Published

2024

5. Case 29-2024: A 47-Year-Old Man with Confusion and Kidney Failure.

Author

Shah, Sachin J., Price, Melissa C., and Kanjilal, Sanjat

Subjects

*SARS-CoV-2, *SENDAI virus, *MEDICAL societies, *NEMALINE myopathy, *FANCONI'S anemia, *COUGH

Abstract

This article presents a case of a 47-year-old man who was admitted to the hospital with confusion and kidney failure. The patient had experienced fatigue and muscle pain prior to admission, and his symptoms worsened over time. Upon examination, the patient exhibited confusion, difficulty finding words, and garbled speech. Laboratory tests revealed abnormalities in blood and urine, and imaging studies showed consolidation in the right lower lobe of the lung. The article discusses the possible causes of the patient's symptoms, including nontraumatic, nonexertional rhabdomyolysis. It also explores the diagnosis and treatment of Legionella pneumonia, which was ultimately confirmed in this case. The patient's history of living in a converted factory and using dietary supplements, as well as the presence of lung consolidation, suggested a possible diagnosis of legionella infection. The article provides information on the transmission and diagnostic methods of legionella infection, as well as the treatment and prevention strategies. It also highlights the challenges in diagnosing the infection in this particular case due to the patient's altered mental state and poor sample quality. The patient's myopathy may have contributed to the severity of the infection. [Extracted from the article]

Published

2024

6. Zinc-finger CCHC-type containing protein 8 promotes RNA virus replication by suppressing the type-I interferon responses.

Author

Shaoyu Tu, Jiahui Zou, Chuhan Xiong, Chao Dai, Huimin Sun, Didan Luo, Meilin Jin, Huanchun Chen, and Hongbo Zhou

Subjects

*TYPE I interferons, *INTERFERON regulatory factors, *JAPANESE encephalitis viruses, *SENDAI virus, *IMMUNOREGULATION, *INFLUENZA A virus

Abstract

Host cells have evolved an intricate regulatory network to fine tune the type-I interferon responses. However, the full picture of this regulatory network remains to be depicted. In this study, we found that knock out of zinc-finger CCHC-type containing protein 8 (ZCCHC8) impairs the replication of influenza A virus (IAV), Sendai virus (Sev), Japanese encephalitis virus (JEV), and vesicular stomatitis virus (VSV). Further investigation unveiled that ZCCHC8 suppresses the type-I interferon responses by targeting the interferon regulatory factor 3 (IRF3) signaling pathway. Mechanistically, ZCCHC8 associates with phosphorylated IRF3 and disrupts the interaction of IRF3 with the co-activator CREB-binding protein (CBP). Additionally, the direct binding of ZCCHC8 with the IFN-stimulated response element (ISRE) impairs the ISRE-binding of IRF3. Our study contributes to the comprehensive understanding for the negative regulatory network of the type-I interferon responses and provides valuable insights for the control of multiple viruses from a host-centric perspective. IMPORTANCE The innate immune responses serve as the initial line of defense against invading pathogens and harmful substances. Negative regulation of the innate immune responses plays an essential role in avoiding auto-immune diseases and over-activated immune responses. Hence, the comprehensive understanding of the negative regulation network for innate immune responses could provide novel therapeutic insights for the control of viral infections and immune dysfunction. In this study, we report that ZCCHC8 negatively regulates the type-I interferon responses. We illustrate that ZCCHC8 impedes the IRF3-CBP association by interacting with phosphorylated IRF3 and competes with IRF3 for binding to ISRE. Our study demonstrates the role of ZCCHC8 in the replication of multiple RNA viruses and contributes to a deeper understanding of the negative regulation system for the type-I interferon responses. [ABSTRACT FROM AUTHOR]

Published

2024

7. Performance of three multiplex real-time PCR assays for simultaneous detection of 12 infectious pathogens in mice affected with respiratory and digestive diseases.

Author

Hye-young Wang, Jaeil Ahn, Jonghoon Lee, Sang Chul Kang, and Hyunil Kim

Subjects

DIGESTIVE system diseases, RESPIRATORY diseases, PATHOGENIC microorganisms, ANIMAL experimentation, SENDAI virus, MYCOPLASMA, PSEUDOMONADACEAE

Abstract

Introduction: Research quality can be improved with reliable and reproducible experimental results when animal experiments are conducted using laboratory animals with guaranteed microbiological and genetic quality through health monitoring. Therefore, health monitoring requires the rapid and accurate diagnosis of infectious diseases in laboratory animals. Methods: This study presents a performance evaluation of a commercially available multiplex real-time PCR (mRT-PCR) assay for the rapid detection of 12 infectious pathogens (Set 1: Sendai virus [SeV, formally murine respirovirus], Mycoplasma spp., Rodentibacter pneumotropicus, and Rodentibacter heylii; Set 2: Helicobacter spp., Murine norovirus [MNV], Murine hepatitis virus [MHV], and Salmonella spp.; Set 3: Staphylococcus aureus, Streptobacillus moniliformis, Corynebacterium kutscheri, and Pseudomonas aeruginosa). To evaluate the efficacy of the mRT-PCR assay, 102 clinical samples encompassing fecal and cecal specimens were analyzed. The resulting data were then compared with the findings from sequence analysis for validation. Results: The assay’s detection limit ranged from 1 to 100 copies per reaction. Specificity testing involving various viruses and bacteria indicated no crossreactivity between strains. Additionally, the assay exhibited good reproducibility, with mean coefficients of variation for inter- and intra assay variation below 3%. The overall positive rate was 52.9% (n  =  54), with the mRT-PCR assay findings matching sequence analysis results (κ  =  1). MHV (n  =  29, 28.4%) was the most prevalent pathogen, followed by Helicobacter spp. (n  =  28, 27.5%), R. heylii (n  =  18, 17.6%), Mycoplasma spp. (n  =  14, 13.7%), MNV (n  =  12, 11.8%), S. aureus (n  =  9, 8.8%), P. aeruginosa (n  =  4, 3.9%), and R. pneumotropicus (n  =  1, 0.9%). Discussion: This assay offers a rapid turnaround time of 100 min, including 30 min for DNA preparation and 70 min for target DNA/RNA amplification. It ensures accuracy, minimizing false positives or negatives, making it a convenient tool for the simultaneous detection of infectious diseases in many samples. Overall, the propose-d assay holds promise for the effective detection of the most important pathogens in laboratory animal health monitoring. [ABSTRACT FROM AUTHOR]

Published

2024

8. Characterization of Influenza D Virus Reassortant Strain in Swine from Mixed Pig and Beef Farm, France.

Author

Gorin, Stéphane, Richard, Gautier, Hervé, Séverine, Eveno, Eric, Blanchard, Yannick, Jardin, Agnès, Rose, Nicolas, and Simon, Gaëlle

Subjects

*SENDAI virus, *SWINE farms, *SWINE influenza, *SWINE, *BINDING sites

Abstract

Influenza D virus was isolated from pigs on a mixed pig and beef farm in France. Investigation suggested bullto-pig transmission and spread among pigs. The swine influenza D virus recovered was a reassortant of D/660 and D/OK lineages. Reported mutations in the receptor binding site might be related to swine host adaptation. [ABSTRACT FROM AUTHOR]

Published

2024

9. Comparison of the calcium signaling alterations in GABA-ergic medium spiny neurons produced from iPSCs of different origins.

Author

Oshkolova, Arina A., Grekhnev, Dmitriy A., Kruchinina, Anna A., Belikova, Lilia D., Volovikov, Egor A., Lebedeva, Olga S., Bogomazova, Alexandra N., Vigont, Vladimir A., Lagarkova, Maria A., and Kaznacheyeva, Elena V.

Subjects

*MEDIUM spiny neurons, *CALCIUM channels, *INDUCED pluripotent stem cells, *CALCIUM, *NUCLEUS accumbens, *SENDAI virus, *SOMATIC cells

Abstract

Disease models based on induced pluripotent stem cells (iPSCs) are in high demand because of their physiological adequacy and well-reproducibility of the pathological phenotype. Nowadays, the most common approach to generate iPSCs is the reprogramming of somatic cells using vectors based on lentivirus or Sendai virus. We have previously shown impairments of calcium signaling including store-operated calcium entry in Huntington's disease-specific iPSCs-based GABA-ergic medium spiny neurons. However, different approaches for iPSCs generation make it difficult to compare the models since the mechanism of reprogramming may influence the electrophysiological properties of the terminally differentiated neurons. Here, we have studied the features of calcium homeostasis in GABA-ergic medium spiny neurons differentiated from iPSCs obtained from fibroblasts of the same donor using different methods. Our data demonstrated that there were no significant differences neither in calcium influx through the store-operated channels, nor in the levels of proteins activating this type of calcium entry in neurons differentiated from iPSCs generated with lenti- and Sendai viruses-based approaches. We also found no differences in voltage-gated calcium entry for these neurons. Thus, we clearly showed that various methods of cell reprogramming result in similar deregulations in neuronal calcium signaling which substantiates the ability to combine the experimental data on functional studies of ion channels in models based on iPSCs obtained by different methods and expands the prospects for the use of biobanking. • Different methods of iPSCs generation result in similar neuronal calcium signaling. • Data obtained with different iPSCs-based models can be combined. • Calcium alterations in HD-specific neurons do not depend on iPSCs generation method. [ABSTRACT FROM AUTHOR]

Published

2024

10. Immunogenicity and Protective Efficacy of a Single Intranasal Dose Vectored Vaccine Based on Sendai Virus (Moscow Strain) against SARS-CoV-2 Variant of Concern.

Author

Kochneva, Galina V., Kudrov, Gleb A., Zainutdinov, Sergei S., Shulgina, Irina S., Shipovalov, Andrei V., Zaykovskaya, Anna V., Borgoyakova, Mariya B., Starostina, Ekaterina V., Bodnev, Sergei A., Sivolobova, Galina F., Grazhdantseva, Antonina A., Ivkina, Daria I., Zadorozhny, Alexey M., Karpenko, Larisa I., and P'yankov, Oleg V.

Subjects

SARS-CoV-2 Delta variant, SENDAI virus, INTRANASAL administration, GOLDEN hamster, SARS-CoV-2

Abstract

The mouse paramyxovirus Sendai, which is capable of limited replication in human bronchial epithelial cells without causing disease, is well suited for the development of vector-based intranasal vaccines against respiratory infections, including SARS-CoV-2. Using the Moscow strain of the Sendai virus, we developed a vaccine construct, Sen-Sdelta(M), which expresses the full-length spike (S) protein of the SARS-CoV-2 delta variant. A single intranasal delivery of Sen-Sdelta(M) to Syrian hamsters and BALB/c mice induced high titers of virus-neutralizing antibodies specific to the SARS-CoV-2 delta variant. A significant T-cell response, as determined by IFN-γ ELISpot and ICS methods, was also demonstrated in the mouse model. Mice and hamsters vaccinated with Sen-Sdelta(M) were well protected against SARS-CoV-2 challenge. The viral load in the lungs and nasal turbinates, measured by RT-qPCR and TCID50 assay, decreased dramatically in vaccinated groups. The most prominent effect was revealed in a highly sensitive hamster model, where no tissue samples contained detectable levels of infectious SARS-CoV-2. These results indicate that Sen-Sdelta(M) is a promising candidate as a single-dose intranasal vaccine against SARS-CoV-2, including variants of concern. [ABSTRACT FROM AUTHOR]

Published

2024

11. Characterization of immortalized ovarian epithelial cells with BRCA1/2 mutation.

Author

Komatsu, Hiroaki, Okawa, Masayo, Kazuki, Yasuhiro, Kazuki, Kanako, Hichiwa, Genki, Shimoya, Kazuto, Sato, Shinya, Taniguchi, Fuminori, Oshimura, Mitsuo, and Harada, Tasuku

Subjects

EPITHELIAL cells, CHROMOSOME abnormalities, SENDAI virus, CHROMOSOMES, POLYMERASE chain reaction, HUMAN carcinogenesis

Abstract

We aimed to elucidate the mechanism underlying carcinogenesis by comparing normal and BRCA1/2-mutated ovarian epithelial cells established via Sendai virus-based immortalization. Ovarian epithelial cells (normal epithelium: Ovn; with germline BRCA1 mutation: OvBRCA1; with germline BRCA2 mutation: OvBRCA2) were infected with Sendai virus vectors carrying three immortalization genes (Bmi-1, hTERT, and SV40T). The immunoreactivity to anti-epithelial cellular adhesion molecule (EpCAM) antibodies in each cell line and cells after 25 passages was confirmed using flow cytometry. Chromosomes were identified and karyotyped to detect numerical and structural abnormalities. Total RNA extracted from the cells was subjected to human transcriptome sequencing. Highly expressed genes in each cell line were confirmed using real-time polymerase chain reaction. Immortalization techniques allowed 25 or more passages of Ovn, OvBRCA1, and OvBRCA2 cells. No anti-EpCAM antibody reactions were observed in primary cultures or after long-term passages of each cell line. Structural abnormalities in the chromosomes were observed in each cell line; however, the abnormal chromosomes were successfully separated from the normal structures via cloning. Only normal cells from each cell line were cloned. MMP1, CCL2, and PAPPA were more predominantly expressed in OvBRCA1 and OvBRCA2 cells than in Ovn cells. Immortalized ovarian cells derived from patients with germline BRCA1 or BRCA2 mutations showed substantially higher MMP1 expression than normal ovarian cells. However, the findings need to be validated in the future. [ABSTRACT FROM AUTHOR]

Published

2024

12. Local treatment of HVJ-E with T cell costimulatory molecule stimulation elicits systemic anti-tumor effects

Author

Airi Ishibashi, Yue Li, Yuuta Hisatomi, Noriko Ohta, Yuko Uegaki, Atsushi Tanemura, Riuko Ohashi, Koji Kitamura, Kotaro Saga, Yasuhide Yoshimura, Satoko Inubushi, Kyoso Ishida, Sadahiro Iwabuchi, Shinichi Hashimoto, Eiji Kiyohara, Hideo Yagita, Yasufumi Kaneda, and Keisuke Nimura

Subjects

Sendai virus, HVJ, HVJ-E, OX40, Nkg2d, Nkg2d ligand, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

The tumor-infiltrating lymphocyte (TIL) is a crucial factor in controlling tumor growth. A therapeutic method activating TIL is desired for treating patients with metastatic tumors. Here, we show that treating a local tumor with a combination therapy of UV-irradiated hemagglutinating virus of Japan envelope (HVJ-E) plus agonist antibodies, including OX40, against T cell costimulatory molecules induces systemic anti-tumor effects in a T cell-dependent manner in multiple cancer cell lines. Transcriptome and T cell receptor repertoire analyses revealed that HVJ-E + anti-OX40 antibody treatment activates CD4 and CD8 T cells and promotes T cell trafficking between tumors. These systemic anti-tumor effects required an association between Nkg2d and Nkg2d ligands. Our findings provide insights into how systemic anti-tumor effects are induced and may help the development of therapeutic strategies for eliciting such effects.

Published

2024

13. A multistage Sendai virus vaccine incorporating latency-associated antigens induces protection against acute and latent tuberculosis

Author

Zhidong Hu, Jingxian Xia, Juan Wu, Huimin Zhao, Ping Ji, Ling Gu, Wenfei Gu, Zhenyan Chen, Jinchuan Xu, Xuejiao Huang, Jian Ma, Anke Chen, Jixi Li, Tsugumine Shu, and Xiao-Yong Fan

Subjects

Suberculosis, latent infection, Sendai virus, BCG, vaccine, multistage, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

One-quarter of the world’s population is infected with Mycobacterium tuberculosis (Mtb). After initial exposure, more immune-competent persons develop asymptomatic latent tuberculosis infection (LTBI) but not active diseases, creates an extensive reservoir at risk of developing active tuberculosis. Previously, we constructed a novel recombinant Sendai virus (SeV)-vectored vaccine encoding two dominant antigens of Mtb, which elicited immune protection against acute Mtb infection. In this study, nine Mtb latency-associated antigens were screened as potential supplementary vaccine candidate antigens, and three antigens (Rv2029c, Rv2028c, and Rv3126c) were selected based on their immune-therapeutic effect in mice, and their elevated immune responses in LTBI human populations. Then, a recombinant SeV-vectored vaccine, termed SeV986A, that expresses three latency-associated antigens and Ag85A was constructed. In murine models, the doses, titers, and inoculation sites of SeV986A were optimized, and its immunogenicity in BCG-primed and BCG-naive mice were determined. Enhanced immune protection against the Mtb challenge was shown in both acute-infection and latent-infection murine models. The expression levels of several T-cell exhaustion markers were significantly lower in the SeV986A-vaccinated group, suggesting that the expression of latency-associated antigens inhibited the T-cell exhaustion process in LTBI infection. Hence, the multistage quarter-antigenic SeV986A vaccine holds considerable promise as a novel post-exposure prophylaxis vaccine against tuberculosis.

Published

2024

14. Editorial: Antiviral options for emerging and reemerging viral diseases: current therapeutics, novel drug candidates and new approaches.

Author

Meseko, Clement, Sanicas, Melvin, Gupta, Yash, and Kumar, Binod

Subjects

SENDAI virus, VIRUS diseases, POST-acute COVID-19 syndrome, INFLUENZA vaccines, COVID-19 pandemic, AVIAN influenza

Published

2024

15. Generation of two induced pluripotent stem cell lines (CHOCi002-A and CHOCi003-A) from Pompe disease patients with compound heterozygous mutations in the GAA gene.

Author

Christensen, Chloe, Heckman, Perla, Rha, Allisandra, Kan, Shih-Hsin, Harb, Jerry, and Wang, Raymond

Subjects

Humans, Glycogen Storage Disease Type II, alpha-Glucosidases, Genotype, Mutation, Induced Pluripotent Stem Cells, Induced pluripotent stem cells, Lysosomal storage disorder, Pompe disease, Sendai virus, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Chronic Liver Disease and Cirrhosis, Liver Disease, Genetics, Digestive Diseases, Rare Diseases, Stem Cell Research, Stem Cell Research - Induced Pluripotent Stem Cell, 2.1 Biological and endogenous factors, Aetiology, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

Pompe disease is an autosomal recessive lysosomal storage disease caused by pathogenic variants in GAA, which encodes an enzyme integral to glycogen catabolism, acid α-glucosidase. Disease-relevant cell lines are necessary to evaluate the efficacy of genotype-specific therapies. Dermal fibroblasts from two patients presenting clinically with Pompe disease were reprogrammed to induced pluripotent stem cells using the Sendai viral method. One patient is compound heterozygous for the c.258dupC (p.N87QfsX9) frameshift mutation and the c.2227C>T (p.Q743X) nonsense mutation. The other patient harbors the c.-32-13T>G splice variant and the c.1826dupA (p.Y609X) frameshift mutation in compound heterozygosity.

Published

2023

16. Expandable Sendai-Virus-Reprogrammed Human iPSC-Neuronal Precursors: In Vivo Post-Grafting Safety Characterization in Rats and Adult Pig

Author

Kobayashi, Yoshiomi, Shigyo, Michiko, Platoshyn, Oleksandr, Marsala, Silvia, Kato, Tomohisa, Takamura, Naoki, Yoshida, Kenji, Kishino, Akiyoshi, Bravo-Hernandez, Mariana, Juhas, Stefan, Juhasova, Jana, Studenovska, Hana, Proks, Vladimir, Driscoll, Shawn P, Glenn, Thomas D, Pfaff, Samuel L, Ciacci, Joseph D, and Marsala, Martin

Subjects

Biological Sciences, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research - Induced Pluripotent Stem Cell, Neurosciences, Neurodegenerative, Transplantation, Stem Cell Research - Nonembryonic - Human, Stem Cell Research, Regenerative Medicine, Spinal Cord Injury, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Adult, Animals, Humans, Rats, Cell Differentiation, Cellular Reprogramming, Genetic Vectors, Graft Survival, Induced Pluripotent Stem Cells, Injections, Spinal, Neural Stem Cells, Sendai virus, Specimen Handling, Stem Cell Transplantation, Swine, Tissue and Organ Harvesting, Treatment Outcome, Brain, Spinal Cord, human induced pluripotent stem cells, neural precursor cells, cryopreservation, spinal cord, human injection device, immunosuppressed adult pig, Technology, Medical and Health Sciences, Neurology & Neurosurgery, Biological sciences

Abstract

One of the challenges in clinical translation of cell-replacement therapies is the definition of optimal cell generation and storage/recovery protocols which would permit a rapid preparation of cell-treatment products for patient administration. Besides, the availability of injection devices that are simple to use is critical for potential future dissemination of any spinally targeted cell-replacement therapy into general medical practice. Here, we compared the engraftment properties of established human-induced pluripotent stem cells (hiPSCs)-derived neural precursor cell (NPCs) line once cells were harvested fresh from the cell culture or previously frozen and then grafted into striata or spinal cord of the immunodeficient rat. A newly developed human spinal injection device equipped with a spinal cord pulsation-cancelation magnetic needle was also tested for its safety in an adult immunosuppressed pig. Previously frozen NPCs showed similar post-grafting survival and differentiation profile as was seen for freshly harvested cells. Testing of human injection device showed acceptable safety with no detectable surgical procedure or spinal NPCs injection-related side effects.

Published

2023

17. Derivation of Sendai-Virus-Reprogrammed Human iPSCs-Neuronal Precursors: In Vitro and In Vivo Post-grafting Safety Characterization.

Author

Shigyo, Michiko, Kobayashi, Yoshiomi, Platoshyn, Oleksandr, Marsala, Silvia, Kato, Tomohisa, Takamura, Naoki, Yoshida, Kenji, Kishino, Akiyoshi, Bravo-Hernandez, Mariana, Juhas, Stefan, Juhasova, Jana, Studenovska, Hana, Proks, Vladimir, Ciacci, Joseph D, and Marsala, Martin

Subjects

Neurons, Leukocytes, Mononuclear, Animals, Humans, Rats, Sendai virus, Cell Differentiation, Induced Pluripotent Stem Cells, Neural Stem Cells, brain grafting, human-induced pluripotent stem cells, immunodeficient rat, manual selection, neural precursor cells, spinal cord grafting, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research - Induced Pluripotent Stem Cell, Genetics, Neurosciences, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Regenerative Medicine, Clinical Research, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Neurological, Biological Sciences, Technology, Medical and Health Sciences, Neurology & Neurosurgery

Abstract

The critical requirements in developing clinical-grade human-induced pluripotent stem cells-derived neural precursors (hiPSCs-NPCs) are defined by expandability, genetic stability, predictable in vivo post-grafting differentiation, and acceptable safety profile. Here, we report on the use of manual-selection protocol for generating expandable and stable human NPCs from induced pluripotent stem cells. The hiPSCs were generated by the reprogramming of peripheral blood mononuclear cells with Sendai-virus (SeV) vector encoding Yamanaka factors. After induction of neural rosettes, morphologically defined NPC colonies were manually harvested, re-plated, and expanded for up to 20 passages. Established NPCs showed normal karyotype, expression of typical NPCs markers at the proliferative stage, and ability to generate functional, calcium oscillating GABAergic or glutamatergic neurons after in vitro differentiation. Grafted NPCs into the striatum or spinal cord of immunodeficient rats showed progressive maturation and expression of early and late human-specific neuronal and glial markers at 2 or 6 months post-grafting. No tumor formation was seen in NPCs-grafted brain or spinal cord samples. These data demonstrate the effective use of in vitro manual-selection protocol to generate safe and expandable NPCs from hiPSCs cells. This protocol has the potential to be used to generate GMP (Good Manufacturing Practice)-grade NPCs from hiPSCs for future clinical use.

Published

2023

18. The Dual-Pseudotyped Lentiviral Vector with VSV-G and Sendai Virus HN Enhances Infection Efficiency through the Synergistic Effect of the Envelope Proteins.

Author

Jargalsaikhan, Bat-Erdene, Muto, Masanaga, Been, Youngeun, Matsumoto, Shoma, Okamura, Eiichi, Takahashi, Tadanobu, Narimichi, Yutaka, Kurebayashi, Yuuki, Takeuchi, Hideyuki, Shinohara, Takashi, Yamamoto, Ryo, and Ema, Masatsugu

Subjects

*SENDAI virus, *NEURAMINIDASE, *HEMATOPOIETIC stem cells, *VIRAL tropism, *SIALIC acids, *VESICULAR stomatitis, *KRA

Abstract

A gene delivery system utilizing lentiviral vectors (LVs) requires high transduction efficiency for successful application in human gene therapy. Pseudotyping allows viral tropism to be expanded, widening the usage of LVs. While vesicular stomatitis virus G (VSV-G) single-pseudotyped LVs are commonly used, dual-pseudotyping is less frequently employed because of its increased complexity. In this study, we examined the potential of phenotypically mixed heterologous dual-pseudotyped LVs with VSV-G and Sendai virus hemagglutinin-neuraminidase (SeV-HN) glycoproteins, termed V/HN-LV. Our findings demonstrated the significantly improved transduction efficiency of V/HN-LV in various cell lines of mice, cynomolgus monkeys, and humans compared with LV pseudotyped with VSV-G alone. Notably, V/HN-LV showed higher transduction efficiency in human cells, including hematopoietic stem cells. The efficient incorporation of wild-type SeV-HN into V/HN-LV depended on VSV-G. SeV-HN removed sialic acid from VSV-G, and the desialylation of VSV-G increased V/HN-LV infectivity. Furthermore, V/HN-LV acquired the ability to recognize sialic acid, particularly N-acetylneuraminic acid on the host cell, enhancing LV infectivity. Overall, VSV-G and SeV-HN synergistically improve LV transduction efficiency and broaden its tropism, indicating their potential use in gene delivery. [ABSTRACT FROM AUTHOR]

Published

2024

19. Utilizing Immunoinformatics for mRNA Vaccine Design against Influenza D Virus.

Author

Oladipo, Elijah Kolawole, Adeyemo, Stephen Feranmi, Akinboade, Modinat Wuraola, Akinleye, Temitope Michael, Siyanbola, Kehinde Favour, Adeogun, Precious Ayomide, Ogunfidodo, Victor Michael, Adekunle, Christiana Adewumi, Elutade, Olubunmi Ayobami, Omoathebu, Esther Eghogho, Taiwo, Blessing Oluwatunmise, Akindiya, Elizabeth Olawumi, Ochola, Lucy, and Onyeaka, Helen

Subjects

*MESSENGER RNA, *SENDAI virus, *IMMUNOINFORMATICS, *LYMPHOCYTES, *ANIMAL health

Abstract

Background: Influenza D Virus (IDV) presents a possible threat to animal and human health, necessitating the development of effective vaccines. Although no human illness linked to IDV has been reported, the possibility of human susceptibility to infection remains uncertain. Hence, there is a need for an animal vaccine to be designed. Such a vaccine will contribute to preventing and controlling IDV outbreaks and developing effective countermeasures against this emerging pathogen. This study, therefore, aimed to design an mRNA vaccine construct against IDV using immunoinformatic methods and evaluate its potential efficacy. Methods: A comprehensive methodology involving epitope prediction, vaccine construction, and structural analysis was employed. Viral sequences from six continents were collected and analyzed. A total of 88 Hemagglutinin Esterase Fusion (HEF) sequences from IDV isolates were obtained, of which 76 were identified as antigenic. Different bioinformatics tools were used to identify preferred CTL, HTL, and B-cell epitopes. The epitopes underwent thorough analysis, and those that can induce a lasting immunological response were selected for the construction. Results: The vaccine prototype comprised nine epitopes, an adjuvant, MHC I-targeting domain (MITD), Kozaq, 3′ UTR, 5′ UTR, and specific linkers. The mRNA vaccine construct exhibited antigenicity, non-toxicity, and non-allergenicity, with favourable physicochemical properties. The secondary and tertiary structure analyses revealed a stable and accurate vaccine construct. Molecular docking simulations also demonstrated strong binding affinity with toll-like receptors. Conclusions: The study provides a promising framework for developing an effective mRNA vaccine against IDV, highlighting its potential for mitigating the global impact of this viral infection. Further experimental studies are needed to confirm the vaccine's efficacy and safety. [ABSTRACT FROM AUTHOR]

Published

2024

20. Monitoring Influenza C and D Viruses in Patients With Respiratory Diseases in Japan, January 2018 to March 2023.

Author

Shimizu, Kohei, Kawakami, Chiharu, Matsuzaki, Yoko, Fujisaki, Seiichiro, Nagata, Shiho, Morita, Hiroko, Watanabe, Kayo, Miura, Hideka, Momoki, Tomoko, Saikusa, Miwako, Ozawa, Hiroki, Kumazaki, Makoto, Usuku, Shuzo, Tanaka, Nobuko, Senda, Ryuichi, Okubo, Ichiro, Watanabe, Shinji, Hasegawa, Hideki, Kawaoka, Yoshihiro, and Takashita, Emi

Subjects

*SENDAI virus, *RESPIRATORY diseases, *INFLUENZA B virus, *INFLUENZA viruses, *HEMAGGLUTINATION tests, *VIRUS diseases

Abstract

Background: Influenza viruses can cause zoonotic infections that pose public health risks. Surveillance of influenza A and B viruses is conducted globally; however, information on influenza C and D viruses is limited. Longitudinal monitoring of influenza C virus in humans has been conducted in several countries, but there has been no long‐term monitoring of influenza D virus in humans. The public health risks associated with the influenza D virus therefore remain unknown. Methods: We established a duplex real‐time RT‐PCR to detect influenza C and D viruses and analyzed respiratory specimens collected from 2144 patients in Japan with respiratory diseases between January 2018 and March 2023. We isolated viruses and conducted hemagglutination inhibition tests to examine antigenicity and focus reduction assays to determine susceptibility to the cap‐dependent endonuclease inhibitor baloxavir marboxil. Results: We detected three influenza C viruses belonging to the C/Kanagawa‐ or C/Sao Paulo‐lineages, which recently circulated globally. None of the specimens was positive for the influenza D virus. The C/Yokohama/1/2022 strain, isolated from the specimen with the highest viral RNA load and belonging to the C/Kanagawa‐lineage, showed similar antigenicity to the reference C/Kanagawa‐lineage strain and was susceptible to baloxavir. Conclusions: Our duplex real‐time RT‐PCR is useful for the simultaneous detection of influenza C and D viruses from the same specimen. Adding the influenza D virus to the monitoring of the influenza C virus would help in assessing the public health risks posed by this virus. [ABSTRACT FROM AUTHOR]

Published

2024

21. LTN1 promotes RLR degradation to inhibit immune response to RNA virus through the ESCRT pathway.

Author

Qin, Fei, Cai, Baoshan, Wang, Peng, Cao, Runyu, Zhang, Yuling, Wen, Hongling, Zheng, Yi, Zhao, Wei, Gao, Chengjiang, and Liu, Bingyu

Subjects

IMMUNE response, RNA virus infections, DNA helicases, DOUBLE-stranded RNA, INTERFERON receptors, RNA viruses, VESICULAR stomatitis, SENDAI virus

Abstract

The excessive activation of immune responses will trigger autoimmune diseases or inflammatory injury. The endosomal sorting complexes required for transport (ESCRT) system can capture and mediate ubiquitinated protein degradation, which timely terminates signaling pathway hyperactivation. However, whether the ESCRT system participates in regulating RIGI-like receptor (RLR)-mediated antiviral responses remains unknown. In this study, we show that LTN1/listerin, a major component of RQC, can recruit E3 ubiquitin ligase TRIM27 to trigger K63-linked polyubiquitination of RIGI and IFIH1/MDA5. This K63-linked polyubiquitination facilitates the sorting and degradation of RIGI and IFIH1 proteins through the ESCRT-dependent pathway. Concordantly, LTN1 deficiency enhances the innate antiviral response to infection with RNA viruses. Thus, our work uncovers a new mechanism for RIGI and IFIH1 degradation and identifies the role of LTN1 in negatively regulating RLR-mediated antiviral innate immunity, which may provide new targets for the intervention of viral infection. Abbreviation: 5'-pppRNA: 5' triphosphate double stranded RNA; ATG5: autophagy related 5; ATG7: autophagy related 7; BafA1: bafilomycin A1; ESCRT: endosomal sorting complexes required for transport; CHX: cycloheximide; IFIH1/MDA5: interferon induced with helicase C domain 1; IFN: interferon; PIK3C3/VPS34: phosphatidylinositol 3-kinase catalytic subunit type 3; RIGI: RNA sensor RIG-I; RLR: RIGI-like receptors; RQC: ribosome-associated protein quality control; SeV: Sendai virus; TRIM27: tripartite motif-containing 27; VSV: vesicular stomatitis virus; VPS4: vacuolar protein sorting 4. [ABSTRACT FROM AUTHOR]

Published

2024

22. Comparing Occurrence of Bovine Respiratory Pathogens Detected by High-Throughput Real-Time PCR in Nasal Swabs and Non-Endoscopic Bronchoalveolar Lavage Samples from Dairy and Veal Calves.

Author

Otten, Nina Dam, Goecke, Nicole Bakkegård, Michelsen, Anne Marie, Nielsen, Liza Rosenbaum, Capion, Nynne, Martin, Henrik Læssøe, Nielsen, Bodil Højlund, Larsen, Lars Erik, and Petersen, Mette Bisgaard

Subjects

SENDAI virus, CALVES, BRONCHOALVEOLAR lavage, MYCOPLASMA bovis, ANIMAL herds, RESPIRATORY syncytial virus, MANNHEIMIA haemolytica, CATTLE herding

Abstract

This study aimed to enhance our understanding of the agreement between two sampling methods for the detection of bovine respiratory disease (BRD) pathogens in calves using high-throughput real-time qPCR (ht-RT-qPCR). In total, 233 paired nasal swab (NS) and non-endoscopic bronchoalveolar lavage (nBAL) samples were collected from 152 calves from 12 Danish cattle herds. In 202 of the observations, the calves were examined using a standardized clinical protocol. Samples were tested for three viruses (bovine respiratory syncytial virus, bovine corona virus, and influenza D virus) and six bacteria (Histophilus somni, Mannheimia haemolytica, Mycoplasma bovis, Mycoplasma species, Pasteurella multocida, and Truepurella pyogenes). The results showed age-related differences in disease and pathogen occurrence, with the highest detection rates in calves aged 35 days or older. Poor to moderate agreement was found between the NS and nBAL results. The presence of Mannheimia haemolytica in both NS and nBAL in younger calves and in nBAL in older calves was associated with clinical BRD. There was a potential link between BRD and influenza D virus in older calves, although it was only found in one herd in a small sample size. Overall, NS was a relatively poor predictor of pathogens in the lower respiratory tract. The present study confirms the complexity of pathogen detection in BRD, with marked influences of age and the sampling method on pathogen detection and disease associations. [ABSTRACT FROM AUTHOR]

Published

2024

23. Nonstructural Protein A238L of the African Swine Fever Virus (ASFV) Enhances Antiviral Immune Responses by Activating the TBK1-IRF3 Pathway.

Author

Liu, Wei, Yang, Lanlan, Di, Chuanyuan, Sun, Jing, Liu, Penggang, and Liu, Huisheng

Subjects

AFRICAN swine fever virus, HUMAN herpesvirus 1, IMMUNE response, TYPE I interferons, DNA viruses, SENDAI virus

Abstract

Simple Summary: A238L, a non-structural protein of the African swine fever virus (ASFV), inhibits the activation of NF-κB by suppressing the HAT activity of p300. Whether A238L also affects the transcriptional activity of IRF3 remains unexplored. Here we first confirmed the ability of A238L to suppress NF-κB-activity in L929 cells. In contrast, A238L did not inhibit but rather increased TBK1 and IRF3 phosphorylation and enhanced innate antiviral immunity in the absence or presence of poly d (A:T) or poly (I:C) stimulation, or herpes simplex virus type 1 (HSV-1) or Sendai virus (SeV) infection. This study reveals an unrecognized role for A238L in promoting antiviral immune responses by activating the TBK1-IRF3 pathway. African swine fever virus (ASFV) is a double-stranded DNA virus with an envelope. ASFV has almost the largest genome among all DNA viruses, and its mechanisms of immune evasion are complex. Better understanding of the molecular mechanisms of ASFV genes will improve vaccine design. A238L, a nonstructural protein of ASFV, inhibits NF-κB activation by suppressing the HAT activity of p300. Whether A238L also affects the transcriptional activity of IRF3 remains unexplored. Here we first confirmed the ability of A238L to suppress NF-κB-activity in L929 cells. A238L inhibits the expression of proinflammatory cytokine genes. In contrast, A238L increased the phosphorylation levels of TBK1 and IRF3 in three different cell lines. A238L increases the IRF3-driven promoter activity and induces IRF3 nuclear translocation. Furthermore, A238L enhanced innate antiviral immunity in the absence or presence of poly d (A:T) or poly (I:C) stimulation, or herpes simplex virus type 1 (HSV-1) or Sendai virus (SeV) infection. This study reveals a previously unrecognized role of A238L in promoting antiviral immune responses by TBK1-IRF3 pathway activation. [ABSTRACT FROM AUTHOR]

Published

2024

24. Pathogenesis, Transmission, and Within-Host Evolution of Bovine-Origin Influenza D Virus in Pigs.

Author

Gorin, Stéphane, Richard, Gautier, Quéguiner, Stéphane, Chastagner, Amélie, Barbier, Nicolas, Deblanc, Céline, Hervé, Séverine, Blanchard, Yannick, Paboeuf, Frédéric, and Simon, Gaëlle

Subjects

*SENDAI virus, *SWINE, *VIRAL shedding, *INFECTIOUS disease transmission, *VIRAL replication

Abstract

Whereas bovine has been demonstrated as the main reservoir of influenza D virus (IDV), this virus was first isolated in a pig and is regularly detected in some swine populations. However, the role of swine in IDV ecology, as well as the outcomes of IDV infection in pigs, is still unclear. This study aimed to provide additional information on pathogenesis, transmission, and adaptation of a bovine-origin IDV in swine. An infection and transmission study, using an IDV strain isolated following a first passage on pig of a bovine IDV, was conducted on specific pathogen-free pigs, including inoculated and direct contact pigs. Two routes of inoculation were tested, i.e., nasal and tracheal. None of the inoculated or their contact pigs showed clinical signs, but all of them shed the virus in nasal secretions and seroconverted. Virus shedding started earlier in pigs inoculated intranasally as well as in their contact pigs, compared to pigs inoculated intratracheally and associated contacts, suggesting that the viral replication occurred preferentially in the upper respiratory tract. Sequencing data brought to light a mutation on hemagglutinin-esterase-fusion protein (L118F) in the bovine IDV-derived isolate obtained after the first passage on pig. This mutation was fixed in all viral strains obtained in this study, either from inoculated or contact pigs, and was maintained over the second and third passages on swine. The L118F mutation could be linked to the adaptation of the parental bovine IDV to the swine host and might have contributed to an efficient viral multiplication and subsequent pig-to-pig transmission. [ABSTRACT FROM AUTHOR]

Published

2024

25. Bovine Parainfluenza Virus 3 and Bovine Respiratory Syncytial Virus: Dominant Viral Players in Bovine Respiratory Disease Complex among Serbian Cattle.

Author

Milićević, Vesna, Šolaja, Sofija, Glišić, Dimitrije, Ninković, Milan, Milovanović, Bojan, Đorđević, Milan, Ristevski, Snežana, Spasojević, Filip, and Dačić, Miroljub

Subjects

*RESPIRATORY syncytial virus, *MANNHEIMIA haemolytica, *PARAINFLUENZA viruses, *RESPIRATORY diseases, *SENDAI virus, *FARM size, *SERUM

Abstract

Simple Summary: This study thoroughly investigated viral pathogens associated with bovine respiratory disease complex (BRDC) in Serbian cattle using serum and nasal swab samples. Conducted in 2024 across 65 randomly selected dairy farms in Serbia, excluding ones with vaccinated cattle, this study categorized the farms by their size: small, medium, and large. Serum samples from adult cattle were tested for antibodies against BVDV, BHV-1, BRSV, and BPIV3, while nasal swabs from respiratory-symptomatic animals were PCR-tested for viral genome detection. The results showed seropositivity for all four viruses on all of the farms, with BPIV3 being universally positive. Medium-sized and large farms exhibited higher levels of seropositivity for BRSV and BHV-1 compared to small farms (p < 0.05). Our true seroprevalence estimates were 84.29% for BRSV, 54.08% for BVDV, 90.61% for BHV-1, and 84.59% for BPIV3 at the animal level. A PCR analysis of the nasal swabs detected BRSV (20%), BHV-1 (1.7%), BVDV (8%), and BPIV3 (10.9%), with no Influenza D virus found. This study provides crucial insights into viral pathogen prevalence and circulation in Serbian cattle with BRDC, emphasizing the importance of surveillance and control measures to manage respiratory diseases in cattle populations. Bovine respiratory disease complex, a complex respiratory ailment in cattle, results from a combination of viral and bacterial factors, compounded by environmental stressors such as overcrowding, transportation, and adverse weather conditions. Its impact extends beyond mere health concerns, posing significant economic threats to the cattle industry. This study presents an extensive investigation into viral pathogens associated with BRDC in Serbian cattle, utilizing serum samples and nasal swabs. A cross-sectional study was conducted in 2024 across 65 randomly selected dairy farms in Serbia, excluding farms with vaccinated cattle. The farms were categorized by their livestock count: small (≤50 animals), medium (51–200 animals), and large (>200 animals). Serum samples from adult cattle older than 24 months were tested for antibodies against BVDV, BHV-1, BRSV, and BPIV3. Nasal swab samples from the animals with respiratory signs were tested using PCR for viral genome detection. The results showed seropositivity for all four viruses across all of the farms, with BPIV3 exhibiting universal seropositivity. Medium-sized and large farms demonstrated higher levels of seropositivity for BRSV and BHV-1 compared to small farms (p < 0.05). Our true seroprevalence estimates at the animal level were 84.29% for BRSV, 54.08% for BVDV, 90.61% for BHV-1, and 84.59% for BPIV3. A PCR analysis of the nasal swabs revealed positive detections for BRSV (20%), BHV-1 (1.7%), BVDV (8%), and BPIV3 (10.9%). Influenza D virus was not found in any of the samples. This study provides critical insights into the prevalence and circulation of viral pathogens associated with BRDC in Serbian cattle, emphasizing the importance of surveillance and control measures to mitigate the impact of respiratory diseases in cattle populations. [ABSTRACT FROM AUTHOR]

Published

2024

26. CEBPA restricts alveolar type 2 cell plasticity during development and injury-repair.

Author

Hassan, Dalia and Chen, Jichao

Subjects

SENDAI virus, VIRUS diseases, TRANSCRIPTION factors, SOX transcription factors, LUNGS

Abstract

Cell plasticity theoretically extends to all possible cell types, but naturally decreases as cells differentiate, whereas injury-repair re-engages the developmental plasticity. Here we show that the lung alveolar type 2 (AT2)-specific transcription factor (TF), CEBPA, restricts AT2 cell plasticity in the mouse lung. AT2 cells undergo transcriptional and epigenetic maturation postnatally. Without CEBPA, both neonatal and mature AT2 cells reduce the AT2 program, but only the former reactivate the SOX9 progenitor program. Sendai virus infection bestows mature AT2 cells with neonatal plasticity where Cebpa mutant, but not wild type, AT2 cells express SOX9, as well as more readily proliferate and form KRT8/CLDN4+ transitional cells. CEBPA promotes the AT2 program by recruiting the lung lineage TF NKX2-1. The temporal change in CEBPA-dependent plasticity reflects AT2 cell developmental history. The ontogeny of AT2 cell plasticity and its transcriptional and epigenetic mechanisms have implications in lung regeneration and cancer. Cell plasticity underlies development and regeneration. Here, the authors show that mouse lung alveolar type 2 cells undergo maturation postnatally and their plasticity is restricted by CEBPA and increases upon viral infection. [ABSTRACT FROM AUTHOR]

Published

2024

27. Evolutionary engineering and characterization of Sendai virus mutants capable of persistent infection and autonomous production.

Author

Moe Iwata, Ryoko Kawabata, Nao Morimoto, Takeuchi, Ryosuke F., Takemasa Sakaguchi, Takashi Irie, and Fumitaka Osakada

Subjects

SENDAI virus, CHICKEN breeds, EGGS, VIRUS diseases, CO-cultures, BODY temperature, INFECTION

Abstract

Persistent virus infection involves modifying the host immune response and maintaining viral infection. Acute infection with Mononegavirales, such as Sendai viruses (SeVs), can give rise to viruses capable of persistent infection. SeVs establish persistent infection through generating copyback-type defective interfering (cbDI) genomes or acquiring temperature-sensitive mutations. Herein, we identify novel mutations associated with persistent infection and recombinant SeV mutants capable of persistent infection and autonomous production at physiological body temperature, independent of cbDI genomes or temperature-sensitive mutations. Diverse SeV populations were generated by passing the cDNA-recovered SeV Z strain 19 times through embryonated chicken eggs and subsequently infecting LLC-MK2 cells with the SeV populations to finally obtain SeV mutants capable of persistent infection and autonomous production in several types of cultured cells. Sequence analysis identified 4 or 5 mutations in the genome of the persistently infectious SeVs, distinguishing them from other existing strains with persistent infection. Recombinant SeVs carrying 4 or 5 mutations in the Z strain genome (designated SeV-Zpi or SeV-Zpi2, respectively) exhibited persistent infection and autonomous production in LLC-MK2, BHK-21, and Neuro2a cells at 37°C. SeV-Zpi and SeV-Zpi2 consistently produced viral particles even after long-term passages without cbDI particles or temperature-sensitive phenotypes. These results highlight the ability of acute infections of SeVs to spontaneously acquire mutations during replication, thereby endowing persistent infection and autonomous production at body temperature. The vectorization of SeV-Zpi and SeV-Zpi2 will contribute to both basic research and medical applications. [ABSTRACT FROM AUTHOR]

Published

2024

28. Swine acute diarrhea syndrome coronavirus nucleocapsid protein antagonizes the IFN response through inhibiting TRIM25 oligomerization and functional activation of RIG-I/TRIM25.

Author

Zhang, Jiyu, Shi, Hongyan, Zhang, Liaoyuan, Feng, Tingshuai, Chen, Jianfei, Zhang, Xin, Ji, Zhaoyang, Jing, Zhaoyang, Zhu, Xiaoyuan, Liu, Dakai, Yang, Xiaoman, Zeng, Miaomiao, Shi, Da, and Feng, Li

Subjects

CORONAVIRUSES, SENDAI virus, SWINE, COVID-19, OLIGOMERIZATION

Abstract

Swine acute diarrhea syndrome coronavirus (SADS-CoV), an emerging Alpha-coronavirus, brings huge economic loss in swine industry. Interferons (IFNs) participate in a frontline antiviral defense mechanism triggering the activation of numerous downstream antiviral genes. Here, we demonstrated that TRIM25 overexpression significantly inhibited SADS-CoV replication, whereas TRIM25 deficiency markedly increased viral yield. We found that SADS-CoV N protein suppressed interferon-beta (IFN-β) production induced by Sendai virus (SeV) or poly(I:C). Moreover, we determined that SADS-CoV N protein interacted with RIG-I N-terminal two caspase activation and recruitment domains (2CARDs) and TRIM25 coiled-coil dimerization (CCD) domain. The interaction of SADS-CoV N protein with RIG-I and TRIM25 caused TRIM25 multimerization inhibition, the RIG-I-TRIM25 interaction disruption, and consequent the IRF3 and TBK1 phosphorylation impediment. Overexpression of SADS-CoV N protein facilitated the replication of VSV-GFP by suppressing IFN-β production. Our results demonstrate that SADS-CoV N suppresses the host IFN response, thus highlighting the significant involvement of TRIM25 in regulating antiviral immune defenses. [ABSTRACT FROM AUTHOR]

Published

2024

29. Molecular and Serological Detection of Bovine Coronaviruses in Marmots (Marmota marmota) in the Alpine Region.

Author

Moreno, Ana, Canziani, Sabrina, Lelli, Davide, Castelli, Anna, Bianchi, Alessandro, Bertoletti, Irene, Maccarinelli, Federica, Carlomagno, Marco, Paini, Matteo, Rossato, Marzia, Delledonne, Massimo, Giacomelli, Stefano, Cordedda, Antonella, Nicoloso, Sandro, Bellinello, Enrica, Campagnoli, Anna, and Trogu, Tiziana

Subjects

*ALPINE regions, *CORONAVIRUSES, *SENDAI virus, *CANINE distemper virus, *WHOLE genome sequencing, *ROE deer, *FORAGE

Abstract

In this study, virological surveillance focused on coronaviruses in marmots in the Alpine region in 2022, captured as part of a population control reduction program in the Livigno area. Seventy-six faecal samples were randomly collected from marmots at the time of capture and release and tested for genome detection of pan-coronavirus, pan-pestivirus, canine distemper virus, and influenza A and D virus. Nine faecal samples were positive in the Pan-CoV RT-PCR, while all were negative for the other viruses. Pan-coronavirus positives were further identified using Illumina's complete genome sequencing, which showed the highest homology with Bovine Coronavirus previously detected in roe deer in the Alps. Blood samples (n.35) were collected randomly from animals at release and tested for bovine coronavirus (BCoV) antibodies using competitive ELISA and VNT. Serological analyses revealed that 8/35 sera were positive for BCoV antibodies in both serological tests. This study provides molecular and serological evidence of the presence of BCoV in an alpine marmot population due to a likely spillover event. Marmots share areas and pastures with roe deer and other wild ruminants, and environmental transmission is a concrete possibility. [ABSTRACT FROM AUTHOR]

Published

2024

30. Non-transcriptional IRF7 interacts with NF-?B to inhibit viral inflammation.

Author

Shumin Fan, Popli, Sonam, Chakravarty, Sukanya, Chakravarti, Ritu, and Chattopadhyay, Saurabh

Subjects

*VIRUS diseases, *SENDAI virus, *VIRAL hepatitis, *HEPATITIS A virus, *TRANSCRIPTION factors, *TOLL-like receptors, *INTERFERON receptors

Abstract

Interferon (IFN) regulatory factors (IRF) are key transcription factors in cellular antiviral responses. IRF7, a virusinducible IRF, expressed primarily in myeloid cells, is required for transcriptional induction of interferon α and antiviral genes. IRF7 is activated by virus-induced phosphorylation in the cytoplasm, leading to its translocation to the nucleus for transcriptional activity. Here, we revealed a nontranscriptional activity of IRF7 contributing to its antiviral functions. IRF7 interacted with the pro-inflammatory transcription factor NF-κB-p65 and inhibited the induction of in- flammatory target genes. Using knockdown, knockout, and overexpression strategies, we demonstrated that IRF7 inhibited NF-κB--dependent inflammatory target genes, induced by virus infection or toll-like receptor stimulation. A mutant IRF7, defective in transcriptional activity, interacted with NF-κB-p65 and suppressed NF-κB--induced gene expression. A singleaction IRF7 mutant, active in anti-inflammatory function, but defective in transcriptional activity, efficiently suppressed Sendai virus and murine hepatitis virus replication. We, therefore, uncovered an anti-inflammatory function for IRF7, independent of transcriptional activity, contributing to the antiviral response of IRF7. [ABSTRACT FROM AUTHOR]

Published

2024

31. An engineered ligand-responsive Csy4 endoribonuclease controls transgene expression from Sendai virus vectors

Author

Takumi Kishimoto, Ken Nishimura, Kana Morishita, Aya Fukuda, Yusaku Miyamae, Yutaro Kumagai, Kimio Sumaru, Mahito Nakanishi, Koji Hisatake, and Masayuki Sano

Subjects

Sendai virus, Csy4, Ligand, Gene regulation, ES cells, Neural differentiation, Biology (General), QH301-705.5

Abstract

Abstract Background Viral vectors are attractive gene delivery vehicles because of their broad tropism, high transduction efficiency, and durable expression. With no risk of integration into the host genome, the vectors developed from RNA viruses such as Sendai virus (SeV) are especially promising. However, RNA-based vectors have limited applicability because they lack a convenient method to control transgene expression by an external inducer. Results We engineered a Csy4 switch in Sendai virus-based vectors by combining Csy4 endoribonuclease with mutant FKBP12 (DD: destabilizing domain) that becomes stabilized when a small chemical Shield1 is supplied. In this Shield1-responsive Csy4 (SrC) switch, Shield1 increases Csy4 fused with DD (DD-Csy4), which then cleaves and downregulates the transgene mRNA containing the Csy4 recognition sequence (Csy4RS). Moreover, when Csy4RS is inserted in the viral L gene, the SrC switch suppresses replication and transcription of the SeV vector in infected cells in a Shield1-dependent manner, thus enabling complete elimination of the vector from the cells. By temporally controlling BRN4 expression, a BRN4-expressing SeV vector equipped with the SrC switch achieves efficient, stepwise differentiation of embryonic stem cells into neural stem cells, and then into astrocytes. Conclusion SeV-based vectors with the SrC switch should find wide applications in stem cell research, regenerative medicine, and gene therapy, especially when precise control of reprogramming factor expression is desirable.

Published

2024

32. An engineered ligand-responsive Csy4 endoribonuclease controls transgene expression from Sendai virus vectors

Author

Kishimoto, Takumi, Nishimura, Ken, Morishita, Kana, Fukuda, Aya, Miyamae, Yusaku, Kumagai, Yutaro, Sumaru, Kimio, Nakanishi, Mahito, Hisatake, Koji, and Sano, Masayuki

Published

2024

33. IDV Typer: An Automated Tool for Lineage Typing of Influenza D Viruses Based on Return Time Distribution.

Author

Limaye, Sanket, Shelke, Anant, Kale, Mohan M., Kulkarni-Kale, Urmila, and Kuchipudi, Suresh V.

Subjects

*SENDAI virus, *INFLUENZA viruses, *VIRAL tropism, *MOLECULAR phylogeny, *LINEAGE

Abstract

Influenza D virus (IDV) is the most recent addition to the Orthomyxoviridae family and cattle serve as the primary reservoir. IDV has been implicated in Bovine Respiratory Disease Complex (BRDC), and there is serological evidence of human infection of IDV. Evolutionary changes in the IDV genome have resulted in the expansion of genetic diversity and the emergence of multiple lineages that might expand the host tropism and potentially increase the pathogenicity to animals and humans. Therefore, there is an urgent need for automated, accurate and rapid typing tools for IDV lineage typing. Currently, IDV lineage typing is carried out using BLAST-based searches and alignment-based molecular phylogeny of the hemagglutinin-esterase fusion (HEF) gene sequences, and lineage is assigned to query sequences based on sequence similarity (BLAST search) and proximity to the reference lineages in the tree topology, respectively. To minimize human intervention and lineage typing time, we developed IDV Typer server, implementing alignment-free method based on return time distribution (RTD) of k-mers. Lineages are assigned using HEF gene sequences. The server performs with 100% sensitivity and specificity. The IDV Typer server is the first application of an RTD-based alignment-free method for typing animal viruses. [ABSTRACT FROM AUTHOR]

Published

2024

34. Proteomic and Lipidomic Profiling of Calves Experimentally Co-Infected with Influenza D Virus and Mycoplasma bovis : Insights into the Host–Pathogen Interactions.

Author

Alvarez, Ignacio, Ducatez, Mariette, Guo, Yongzhi, Lion, Adrien, Widgren, Anna, Dubourdeau, Marc, Baillif, Vincent, Saias, Laure, Zohari, Siamak, Bergquist, Jonas, Meyer, Gilles, Valarcher, Jean-Francois, and Hägglund, Sara

Subjects

*MYCOPLASMA bovis, *SENDAI virus, *CALVES, *LIQUID chromatography-mass spectrometry, *PROTEOMICS, *ARACHIDONIC acid

Abstract

The role of Influenza D virus (IDV) in bovine respiratory disease remains unclear. An in vivo experiment resulted in increased clinical signs, lesions, and pathogen replication in calves co-infected with IDV and Mycoplasma bovis (M. bovis), compared to single-infected calves. The present study aimed to elucidate the host–pathogen interactions and profile the kinetics of lipid mediators in the airways of these calves. Bronchoalveolar lavage (BAL) samples collected at 2 days post-infection (dpi) were used for proteomic analyses by liquid chromatography-tandem mass spectrometry (LC-MS/MS). Additionally, lipidomic analyses were performed by LC-MS/MS on BAL samples collected at 2, 7 and 14 dpi. Whereas M. bovis induced the expression of proteins involved in fibrin formation, IDV co-infection counteracted this coagulation mechanism and downregulated other acute-phase response proteins, such as complement component 4 (C4) and plasminogen (PLG). The reduced inflammatory response against M. bovis likely resulted in increased M. bovis replication and delayed M. bovis clearance, which led to a significantly increased abundance of oxylipids in co-infected calves. The identified induced oxylipids mainly derived from arachidonic acid; were likely oxidized by COX-1, COX-2, and LOX-5; and peaked at 7 dpi. This paper presents the first characterization of BAL proteome and lipid mediator kinetics in response to IDV and M. bovis infection in cattle and raises hypotheses regarding how IDV acts as a co-pathogen in bovine respiratory disease. [ABSTRACT FROM AUTHOR]

Published

2024

35. Influenza D virus utilizes both 9-O-acetylated N-acetylneuraminic and 9-O-acetylated N-glycolylneuraminic acids as functional entry receptors.

Author

Uprety, Tirth, Jieshi Yu, Nogales, Aitor, Naveed, Ahsan, Hai Yu, Xi Chen, Yunpeng Liu, Bowman, Andrew S., Martinez-Sobrido, Luis, Parrish, Colin R., Melikyan, Gregory B., Dan Wang, and Feng Li

Subjects

*SENDAI virus, *ACIDS, *AGRICULTURE

Abstract

Influenza D virus (IDV) utilizes bovines as a primary reservoir with periodical spillover to other hosts. We have previously demonstrated that IDV binds both 9-O-acetylated N-acetylneuraminic acid (Neu5,9Ac2) and 9-O-acetylated N-glycolylneuraminic acid (Neu5Gc9Ac). Bovines produce both Neu5,9Ac2 and Neu5Gc9Ac, while humans are genetically unable to synthesize Neu5Gc9Ac. 9-O-Acetylation of sialic acids is catalyzed by CASD1 via a covalent acetyl-enzyme intermediate. To characterize the role of Neu5,9Ac2 and Neu5Gc9Ac in IDV infection and determine which form of 9-O-acetylated sialic acids drives IDV entry, we took advantage of a CASD1 knockout (KO) MDCK cell line and carried out feeding experiments using synthetic 9-O-acetyl sialic acids in combination with the single-round and multi-round IDV infection assays. The data from our studies show that (i) CASD1 KO cells are resistant to IDV infection and lack of IDV binding to the cell surface is responsible for the failure of IDV replication; (ii) feeding CASD1 KO cells with Neu5,9Ac2 or Neu5Gc9Ac resulted in a dose-dependent rescue of IDV infectivity; and (iii) diverse IDVs replicated robustly in CASD1 KO cells fed with either Neu5,9Ac2 or Neu5Gc9Ac at a level similar to that in wild-type cells with a functional CASD1. These data demonstrate that IDV can utilize Neu5,9Ac2- or non-human Neu5Gc9Ac-containing glycan receptor for infection. Our findings provide evidence that IDV has acquired the ability to infect and transmit among agricultural animals that are enriched in Neu5Gc9Ac, in addition to posing a zoonotic risk to humans expressing only Neu5,9Ac2. [ABSTRACT FROM AUTHOR]

Published

2024

36. Antigenic commonality and divergence of hemagglutinin-esterase-fusion protein among influenza D virus lineages revealed using epitope mapping.

Author

Misa Katayama, Shin Murakami, Hiroho Ishida, Hiromichi Matsugo, Wataru Sekine, Kosuke Ohira, Akiko Takenaka-Uema, and Taisuke Horimoto

Subjects

*SENDAI virus, *MONOCLONAL antibodies, *ANTIGENIC variation, *VIRAL proteins, *VIRAL mutation, *RECOMBINANT viruses

Abstract

Influenza D virus (IDV) is one of the causative agents of bovine respiratory disease complex, which is the most common and economically burdensome disease affecting the cattle industry, and the need for an IDV vaccine has been proposed to enhance disease control. IDVs are classified into five genetic lineages based on the coding sequences of the hemagglutinin-esterase-fusion (HEF) protein, an envelope glycoprotein, which is the main target of protective antibodies against IDV infection. Herein, we prepared a panel of monoclonal antibodies (mAbs) against the HEF protein of viruses of various lineages to investigate the antigenic characteristics of IDVs and found that the mAbs could be largely separated into three groups. The first, second, and third groups demonstrated lineage-specific reactivity, cross-reactivity to viruses of multiple but not all lineages, and cross-reactivity to viruses of all lineages, respectively. Analyzing the escape mutant viruses from virus-neutralizing mAbs revealed that the receptor-binding region of the HEF molecule harbors virus-neutralizing epitopes that are conserved across multiple lineage viruses. In contrast, the apex region of the molecule possessed epitopes unique to each lineage virus. Furthermore, reverse genetics-generated recombinant viruses with point mutations revealed that amino acids within positions 210-214 of the HEF protein determined the antigenic specificity of each lineage virus. Taken together, this study reveals considerable antigenic variation among IDV lineages, although they are presumed to form a single serotype in terms of HEF antigenicity. Characterization of the antigenic epitope structure of HEF may contribute to selecting and creating effective vaccine viruses against IDV. [ABSTRACT FROM AUTHOR]

Published

2024

37. Developing an integrated approach to assess the emergence threat associated with influenza D viruses' circulating in Europe.

Author

Alvarez, Ignacio, Carrera, Maya, Chiapponi, Chiara, Ducatez, Mariette, El Agrebi, Noëmie, Faccini, Silvia, Garcia, Karely, Cuartero, Laura Garza, Gaudino, Maria, Meyer, Gilles, Moreno, Ana, Näslund, Katarina, Quinless, Emma, Rosignoli, Carlo, Saegerman, Claude, Sausy, Aurélie, Sikht, Fatima‐Zohra, Snoeck, Chantal, Soliani, Laura, and Wielick, Constance

Subjects

*SENDAI virus, *ORTHOMYXOVIRUSES

Abstract

Recent studies have identified a new genus of the Orthomyxoviridae family, Influenza D virus (IDV). This virus was shown to infect farm animals including swine and cattle, and to efficiently replicate and transmit in ferrets (Hause et al., 2013; Liu et al., 2020), the animal model of choice for transmission of influenza A virus to humans. This partnering grant (Flu‐D project) on IDV addressed the need for capacity building at EU level to improve the EU's scientific assessment capacity and international competitiveness. We have promoted cross‐disciplinary cooperation between the partner institutes representing six Member States (BE, FR, IE, IT, LU, and SE). We have shown that the available antibody testing methods allow reliable influenza D diagnostics in partners' laboratories but that molecular diagnostic systems required some primers/protocols adjustments. Serological results in European cattle suggest that influenza D virus is enzootic and antigenic maps generated with reference antisera showed 2 main antigenic clusters, matching the genetic clustering. Virus diversity is still unfolding with new virus introductions identified, as well as the discovery of new reassortants whose differential clinical impact or cross‐protection levels are still poorly understood. A quantitative risk assessment model (QRAM) of IDV through introduction of cattle in a country or a herd was developed and refined including several mitigation measures (e.g. testing strategy, vaccination/biosecurity). Complementary, an innovative tool that estimated the biosecurity level of protection of a farm was developed and pre‐tested. The present project led to ideas and data sharing, cross‐consortium training, and to the sustainability of our influenza D network in Europe with perspectives on future collaborative projects. [ABSTRACT FROM AUTHOR]

Published

2024

38. Serological Evidence for Circulation of Influenza D Virus in the Ovine Population in Italy.

Author

Lanave, Gianvito, Camero, Michele, Coppola, Chiara, Marchi, Serena, Cascone, Giuseppe, Salina, Felice, Coltraro, Miriana, Odigie, Amienwanlen E., Montomoli, Emanuele, Chiapponi, Chiara, Cicirelli, Vincenzo, Martella, Vito, and Trombetta, Claudia M.

Subjects

SENDAI virus, ANIMAL herds, DAIRY cattle, DAIRY microbiology

Abstract

Influenza D virus (IDV) is a novel orthomyxovirus initially isolated from pigs exhibiting influenza-like disease in the USA. Since then, IDV has been detected worldwide in several host species, including livestock animals, whilst specific antibodies have been identified in humans, raising concerns about interspecies transmission and zoonotic risks. Few data regarding the seroprevalence of IDV in small ruminants have been available to date. In this study, we assessed the prevalence of antibodies against IDV in ovine serum samples in Sicily, Southern Italy. Six hundred serum samples, collected from dairy sheep herds located in Sicily in 2022, were tested by haemagglutination inhibition (HI) and virus neutralization (VN) assays using reference strains, D/660 and D/OK, representative of two distinct IDV lineages circulating in Italy. Out of 600 tested samples, 168 (28.0%) tested positive to either IDV strain D/660 or D/OK or to both by HI whilst 378 (63.0%) tested positive to either IDV strain D/660 or D/OK or to both by VN. Overall, our findings demonstrate that IDV circulates in ovine dairy herds in Sicily. Since IDV seems to have a broad host range and it has zoonotic potential, it is important to collect epidemiological information on susceptible species. [ABSTRACT FROM AUTHOR]

Published

2024

39. Ebola virus sequesters IRF3 in viral inclusion bodies to evade host antiviral immunity.

Author

Lin Zhu, Jing Jin, Tingting Wang, Yong Hu, Hainan Liu, Ting Gao, Qincai Dong, Yanwen Jin, Ping Li, Zijing Liu, Yi Huang, Xuan Liu, and Cheng Cao

Subjects

*EBOLA virus, *CELLULAR inclusions, *INTERFERON regulatory factors, *VIRAL proteins, *SENDAI virus, *TYPE I interferons

Abstract

Viral inclusion bodies (IBs) commonly form during the replication of Ebola virus (EBOV) in infected cells, but their role in viral immune evasion has rarely been explored. Here, we found that interferon regulatory factor 3 (IRF3), but not TANK-binding kinase 1 (TBK1) or IκB kinase epsilon (IKKε), was recruited and sequestered in viral IBs when the cells were infected by EBOV transcription- and replication-competent virus-like particles (trVLPs). Nucleoprotein/virion protein 35 (VP35)-induced IBs formation was critical for IRF3 recruitment and sequestration, probably through interaction with STING. Consequently, the association of TBK1 and IRF3, which plays a vital role in type I interferon (IFN-I) induction, was blocked by EBOV trVLPs infection. Additionally, IRF3 phosphorylation and nuclear translocation induced by Sendai virus or poly(I:C) stimulation were suppressed by EBOV trVLPs. Furthermore, downregulation of STING significantly attenuated VP35-induced IRF3 accumulation in IBs. Coexpression of the viral proteins by which IB-like structures formed was much more potent in antagonizing IFN-I than expression of the IFN-I antagonist VP35 alone. These results suggested a novel immune evasion mechanism by which EBOV evades host innate immunity. [ABSTRACT FROM AUTHOR]

Published

2024

40. Detecting Respiratory Viruses Using a Portable NIR Spectrometer—A Preliminary Exploration with a Data Driven Approach.

Author

Huang, Jian-Dong, Wang, Hui, Power, Ultan, McLaughlin, James A., Nugent, Chris, Rahman, Enayetur, Barabas, Judit, and Maguire, Paul

Subjects

*RESPIRATORY syncytial virus, *SENDAI virus, *MACHINE learning, *SPECTROMETERS, *MODEL validation

Abstract

Respiratory viruses' detection is vitally important in coping with pandemics such as COVID-19. Conventional methods typically require laboratory-based, high-cost equipment. An emerging alternative method is Near-Infrared (NIR) spectroscopy, especially a portable one of the type that has the benefits of low cost, portability, rapidity, ease of use, and mass deployability in both clinical and field settings. One obstacle to its effective application lies in its common limitations, which include relatively low specificity and general quality. Characteristically, the spectra curves show an interweaving feature for the virus-present and virus-absent samples. This then provokes the idea of using machine learning methods to overcome the difficulty. While a subsequent obstacle coincides with the fact that a direct deployment of the machine learning approaches leads to inadequate accuracy of the modelling results. This paper presents a data-driven study on the detection of two common respiratory viruses, the respiratory syncytial virus (RSV) and the Sendai virus (SEV), using a portable NIR spectrometer supported by a machine learning solution enhanced by an algorithm of variable selection via the Variable Importance in Projection (VIP) scores and its Quantile value, along with variable truncation processing, to overcome the obstacles to a certain extent. We conducted extensive experiments with the aid of the specifically developed algorithm of variable selection, using a total of four datasets, achieving classification accuracy of: (1) 0.88, 0.94, and 0.93 for RSV, SEV, and RSV + SEV, respectively, averaged over multiple runs, for the neural network modelling of taking in turn 3 sessions of data for training and the remaining one session of an 'unknown' dataset for testing. (2) the average accuracy of 0.94 (RSV), 0.97 (SEV), and 0.97 (RSV + SEV) for model validation and 0.90 (RSV), 0.93 (SEV), and 0.91 (RSV + SEV) for model testing, using two of the datasets for model training, one for model validation and the other for model testing. These results demonstrate the feasibility of using portable NIR spectroscopy coupled with machine learning to detect respiratory viruses with good accuracy, and the approach could be a viable solution for population screening. [ABSTRACT FROM AUTHOR]

Published

2024

41. Respiratory syncytial virus among hospitalized patients of severe acute respiratory infection in Bhutan: Cross‐sectional study.

Author

Dorji, Kunzang, Yuden, Pema, Ghishing, Tara Devi, Ghimeray, Govinda, Klungthong, Chonticha, Wangchuk, Sonam, and Farmer, Aaron

Subjects

*PARAINFLUENZA viruses, *RESPIRATORY syncytial virus, *RESPIRATORY syncytial virus infections, *RESPIRATORY infections, *SENDAI virus, *HOSPITAL patients, *DYSPNEA

Abstract

Introduction: Respiratory syncytial virus (RSV) is a leading cause of lower respiratory tract infections worldwide, particularly in young children. In Bhutan, respiratory disease continues to be among the top 10 diseases of morbidity for several years. This study aimed to estimate the prevalence of RSV among hospitalized patients with severe acute respiratory infection (SARI) in Bhutan. Method: Respiratory specimens were collected from SARI patients of all ages in 2016 and 2018 following influenza surveillance guidelines. Specimens were tested for influenza and RSV, human metapneumovirus, adenovirus, and human parainfluenza virus types 1, 2, and 3 using real‐time reverse‐transcription polymerase chain reaction assay. Descriptive statistics were used to analyze the result in STATA 16.1. Result: Of the 1339 SARI specimens tested, 34.8% were positive for at least one viral pathogen. RSV was detected in 18.5% of SARI cases, followed by influenza in 13.4% and other respiratory viruses in 3%. The median age of SARI cases was 3 (IQR: 0.8–21 years) years. RSV detection was higher among children aged 0–6 (Adj OR: 3.03; 95% CI: 1.7–5.39) and 7–23 months (Adj OR: 3.01; 95% CI: 1.77–5.12) compared with the children aged 5–15 years. RSV was also associated with breathing difficulty (Adj OR: 1.73; 95% CI: 1.17–2.56) and pre‐existing lung disease, including asthma (Adj OR: 2.78; 95% CI: 0.99–7.8). Conclusion: Respiratory viruses were detected in a substantial proportion of SARI hospitalizations in Bhutan. [ABSTRACT FROM AUTHOR]

Published

2024

42. Wastewater Collection and Sequencing as a Proactive Approach to Utilizing Threat Agnostic Biological Defense.

Author

Goldberg, Zev, Linder, Alexander G., Miller, Lauren N., and Sorrell, Erin M.

Subjects

EMERGING infectious diseases, SEWAGE, PUBLIC health surveillance, PARAINFLUENZA viruses, MIDDLE East respiratory syndrome, PUBLIC health infrastructure, SENDAI virus

Abstract

The article discusses the importance of proactive biological surveillance in detecting and containing infectious diseases. It emphasizes the limitations of event-based surveillance, which relies on individuals seeking healthcare, and proposes the use of pathogen agnostic wastewater surveillance as a proactive approach. Wastewater testing, coupled with next-generation sequencing (NGS), can detect a wide range of viruses and provide early warning of emerging and novel pathogens. The article suggests the development of national guidelines for pathogen agnostic wastewater surveillance in high-risk areas, such as locations with animal agriculture and international ports of entry. The implementation of such a system would require standardized protocols, bioinformatics pipelines, and interagency collaboration. The article concludes that shifting from event-based surveillance to proactive surveillance will greatly benefit global health and biological defense. [Extracted from the article]

Published

2024

43. Generation of induced pluripotent stem cell line (VRISGi004-A) from a healthy female donor by reprogramming erythroid progenitor cells

Author

Thi-Hoa Luong, Tuan-Anh Pham, Thi-Hong Nhung Nguyen, and Xuan-Hung Nguyen

Subjects

Vietnamese iPSC line, Feeder-free, Sendai virus, Induced cardiomyocytes, Biology (General), QH301-705.5

Abstract

We generated a human induced pluripotent stem cell (hiPSC) line from erythroid progenitor cells (EPCs) of a 20-year-old female healthy donor using Sendai virus vector encoding Yamanaka factors OCT3/4, SOX2, c-MYC, and KLF4. The established hiPSCs showed a standard morphology and expression of typical undifferentiated stem cell markers, a normal karyotype (46, XX), and demonstrated potential for differentiation in vitro. Furthermore, they were successfully differentiated into cardiomyocytes that expressed cardiomyocyte-specific markers. The iPSC line and iPSC-derived cardiomyocytes will provide new avenues for future drug testing/development and personalized cell therapy for cardiovascular diseases (CVDs).

Published

2024

44. Detection of Influenza D Antibodies in Dogs, Apulia Region, Italy, 2016 and 2023.

Author

Maria Trombetta, Claudia, Marchi, Serena, Marotta, Maria Giovanna, Moreno, Ana, Chiapponi, Chiara, Montomoli, Emanuele, Lanave, Gianvito, Camero, Michele, and Martella, Vito

Subjects

*SENDAI virus, *DOGS, *INFLUENZA, *IMMUNOGLOBULINS, *INFLUENZA viruses

Abstract

Dogs are known to be susceptible to influenza A viruses, although information on influenza D virus (IDV) is limited. We investigated the seroprevalence of IDV in 426 dogs in the Apulia region of Italy during 2016 and 2023. A total of 14 samples were positive for IDV antibodies, suggesting exposure to IDV in dogs. [ABSTRACT FROM AUTHOR]

Published

2024

45. Coronaviruses Among Swine Workers in Northern Vietnam.

Author

Pulscher, Laura A., Dao, Duy Tung, Cody, Samantha G., DelPrincipe, Victor, and Gray, Gregory C.

Subjects

*SWINE, *CORONAVIRUSES, *SENDAI virus, *RNA replicase, *MEDICAL virology, *POULTRY farms

Abstract

A study was conducted in northern Vietnam to investigate the prevalence and potential spillover of coronaviruses (CoVs) among swine workers. Nasal wash samples were collected from 401 swine workers on five swine farms and screened for coronaviruses. Three workers (0.75%) tested positive for CoVs, specifically the human coronavirus 229E strain. No spillover of swine coronaviruses (SCoVs) was detected. The study suggests that there may be a low prevalence of CoVs among swine workers and their swine, potentially due to increased biosecurity protocols on the farms. Further research with a larger cohort is recommended to better understand the threat of novel CoVs spilling over into humans. [Extracted from the article]

Published

2024

46. Immunogenicity and Protective Efficacy of a Single Intranasal Dose Vectored Vaccine Based on Sendai Virus (Moscow Strain) against SARS-CoV-2 Variant of Concern

Author

Galina V. Kochneva, Gleb A. Kudrov, Sergei S. Zainutdinov, Irina S. Shulgina, Andrei V. Shipovalov, Anna V. Zaykovskaya, Mariya B. Borgoyakova, Ekaterina V. Starostina, Sergei A. Bodnev, Galina F. Sivolobova, Antonina A. Grazhdantseva, Daria I. Ivkina, Alexey M. Zadorozhny, Larisa I. Karpenko, and Oleg V. P’yankov

Subjects

Sendai virus, Moscow strain, recombinant variant, vectored vaccine, SARS-CoV-2 variant of concern, S protein, Medicine

Abstract

The mouse paramyxovirus Sendai, which is capable of limited replication in human bronchial epithelial cells without causing disease, is well suited for the development of vector-based intranasal vaccines against respiratory infections, including SARS-CoV-2. Using the Moscow strain of the Sendai virus, we developed a vaccine construct, Sen-Sdelta(M), which expresses the full-length spike (S) protein of the SARS-CoV-2 delta variant. A single intranasal delivery of Sen-Sdelta(M) to Syrian hamsters and BALB/c mice induced high titers of virus-neutralizing antibodies specific to the SARS-CoV-2 delta variant. A significant T-cell response, as determined by IFN-γ ELISpot and ICS methods, was also demonstrated in the mouse model. Mice and hamsters vaccinated with Sen-Sdelta(M) were well protected against SARS-CoV-2 challenge. The viral load in the lungs and nasal turbinates, measured by RT-qPCR and TCID50 assay, decreased dramatically in vaccinated groups. The most prominent effect was revealed in a highly sensitive hamster model, where no tissue samples contained detectable levels of infectious SARS-CoV-2. These results indicate that Sen-Sdelta(M) is a promising candidate as a single-dose intranasal vaccine against SARS-CoV-2, including variants of concern.

Published

2024

47. Intranasal vaccine against COVID-19 based on a recombinant variant of the Sendai virus (Paramyxoviridae: Respirovirus) strain Moscow

Author

Gleb A. Kudrov, Sergei S. Zainutdinov, Antonina A. Grazhdantseva, Andrey V. Shipovalov, Galina F. Sivolobova, Anastasiya V. Semenova, Iuliia A. Merkuleva, Dmitry N. Shcherbakov, Oleg S. Taranov, Anna V. Zaykovskaya, Irina S. Shulgina, Oleg V. Pyankov, and Galina V. Kochneva

Subjects

sendai virus, recombinant variant of the virus, sars-cov-2, rbd, immunogenicity, protectiveness, Microbiology, QR1-502

Abstract

Introduction. Intranasal vaccination using live vector vaccines based on non-pathogenic or slightly pathogenic viruses is the one of the most convenient, safe and effective ways to prevent respiratory infections, including COVID-19. Sendai virus is the best suited for this purpose, since it is respiratory virus and is capable of limited replication in human bronchial epithelial cells without causing disease. The aim of the work is to design and study the vaccine properties of recombinant Sendai virus, Moscow strain, expressing secreted receptor-binding domain of SARS-CoV-2 Delta strain S protein (RBDdelta) during a single intranasal immunization. Materials and methods. Recombinant Sendai virus carrying insertion of RBDdelta transgene between P and M genes was constructed using reverse genetics and synthetic biology methods. Expression of RBDdelta was analyzed by Western blot. Vaccine properties were studied in two models: Syrian hamsters and BALB/c mice. Immunogenicity was evaluated by ELISA and virus-neutralization assays. Protectiveness was assessed by quantitation of SARS-CoV-2 RNA in RT-PCR and histological analysis of the lungs. Results. Based on Sendai virus Moscow strain, a recombinant Sen-RBDdelta(M) was constructed that expressed a secreted RBDdelta immunologically identical to natural SARS-CoV-2 protein. A single intranasal administration of Sen-RBDdelta(M) to hamsters and mice significantly, by 15 and 107 times, respectively, reduced replicative activity of SARS-CoV-2 in lungs of animals, preventing the development of pneumonia. An effective induction of virus-neutralizing antibodies has also been demonstrated in mice. Conclusion. Sen-RBDdelta(M) is a promising vaccine construct against SARS-CoV-2 infection and has a protective properties even after a single intranasal introduction.

Published

2023

48. Influenza D in Domestic and Wild Animals.

Author

Kwasnik, Malgorzata, Rola, Jerzy, and Rozek, Wojciech

Subjects

*DOMESTIC animals, *CAPTIVE wild animals, *SENDAI virus, *KANGAROOS, *INFLUENZA, *FERAL swine, *WILD boar, *HORSE breeding

Abstract

Influenza D virus (IDV) infections have been observed in animals worldwide, confirmed through both serological and molecular tests, as well as virus isolation. IDV possesses unique properties that distinguish it from other influenza viruses, primarily attributed to the hemagglutinin-esterase fusion (HEF) surface glycoprotein, which determines the virus' tropism and wide host range. Cattle are postulated to be the reservoir of IDV, and the virus is identified as one of the causative agents of bovine respiratory disease (BRD) syndrome. Animals associated with humans and susceptible to IDV infection include camels, pigs, small ruminants, and horses. Notably, high seroprevalence towards IDV, apart from cattle, is also observed in camels, potentially constituting a reservoir of the virus. Among wild and captive animals, IDV infections have been confirmed in feral pigs, wild boars, deer, hedgehogs, giraffes, wildebeests, kangaroos, wallabies, and llamas. The transmission potential and host range of IDV may contribute to future viral differentiation. It has been confirmed that influenza D may pose a threat to humans as a zoonosis, with seroprevalence noted in people with professional contact with cattle. [ABSTRACT FROM AUTHOR]

Published

2023

49. Generation and Characterization of an Influenza D Reporter Virus.

Author

Probst, Lukas, Laloli, Laura, Licheri, Manon Flore, Licheri, Matthias, Gultom, Mitra, Holwerda, Melle, V'kovski, Philip, and Dijkman, Ronald

Subjects

*SENDAI virus, *VIRUS diseases, *DRUG discovery, *CHIMERIC proteins, *VIRAL tropism, *RECOMBINANT viruses

Abstract

Influenza D virus (IDV) can infect various livestock animals, such as cattle, swine, and small ruminants, and was shown to have zoonotic potential. Therefore, it is important to identify viral factors involved in the broad host tropism and identify potential antiviral compounds that can inhibit IDV infection. Recombinant reporter viruses provide powerful tools for studying viral infections and antiviral drug discovery. Here we present the generation of a fluorescent reporter IDV using our previously established reverse genetic system for IDV. The mNeonGreen (mNG) fluorescent reporter gene was incorporated into the IDV non-structural gene segment as a fusion protein with the viral NS1 or NS2 proteins, or as a separate protein flanked by two autoproteolytic cleavage sites. We demonstrate that only recombinant reporter viruses expressing mNG as an additional separate protein or as an N-terminal fusion protein with NS1 could be rescued, albeit attenuated, compared to the parental reverse genetic clone. Serial passaging experiments demonstrated that the mNG gene is stably integrated for up to three passages, after which internal deletions accumulate. We conducted a proof-of-principle antiviral screening with the established fluorescent reporter viruses and identified two compounds influencing IDV infection. These results demonstrate that the newly established recombinant IDV reporter virus can be applied for antiviral drug discovery and monitoring viral replication, adding a new molecular tool for investigating IDV. [ABSTRACT FROM AUTHOR]

Published

2023

50. Immune Responses to Influenza D Virus in Calves Previously Infected with Bovine Viral Diarrhea Virus 2.

Author

Vicosa Bauermann, Fernando, Falkenberg, Shollie, Rudd, Jennifer M., Peter, Cristina Mendes, Merchioratto, Ingryd, Ritchey, Jerry W., Gilliam, John, Taylor, Jared, Ma, Hao, and Maggioli, Mayara Fernanda

Subjects

*BOVINE viral diarrhea virus, *SENDAI virus, *CALVES, *IMMUNE response

Abstract

Bovine viral diarrhea virus (BVDV) induces immunosuppression and thymus depletion in calves. This study explores the impact of prior BVDV-2 exposure on the subsequent immune response to influenza D virus (IDV). Twenty 3-week-old calves were divided into four groups. Calves in G1 and G3 were mock-treated on day 0, while calves in G2 and G4 received BVDV. Calves in G1 (mock) and G2 (BVDV) were necropsied on day 13 post-infection. IDV was inoculated on day 21 in G3 calves (mock + IDV) and G4 (BVDV + IDV) and necropsy was conducted on day 42. Pre-exposed BVDV calves exhibited prolonged and increased IDV shedding in nasal secretions. An approximate 50% reduction in the thymus was observed in acutely infected BVDV calves (G2) compared to controls (G1). On day 42, thymus depletion was observed in two calves in G4, while three had normal weight. BVDV-2-exposed calves had impaired CD8 T cell proliferation after IDV recall stimulation, and the α/β T cell impairment was particularly evident in those with persistent thymic atrophy. Conversely, no difference in antibody levels against IDV was noted. BVDV-induced thymus depletion varied from transient to persistent. Persistent thymus atrophy was correlated with weaker T cell proliferation, suggesting correlation between persistent thymus atrophy and impaired T cell immune response to subsequent infections. [ABSTRACT FROM AUTHOR]

Published

2023