Your search keyword '"live attenuated vaccine"' showing total 62 results

1. Efficacy of the NS1-truncated live attenuated influenza virus vaccine for swine against infection with viruses of major North American and European H3N2 lineages

Author

Vandoorn, Elien, Parys, Anna, Chepkwony, Sharon, Chiers, Koen, and Van Reeth, Kristien

Subjects

ANTIBODY-RESPONSES, TRANSMISSION, Swine, Vaccine efficacy, UNITED-STATES, IMMUNITY, Swine influenza A virus, Antibodies, Viral, Vaccines, Attenuated, Orthomyxoviridae Infections, A VIRUS, Animals, PIGS, Veterinary Sciences, PROTECTION, PIGLETS, Swine Diseases, General Veterinary, General Immunology and Microbiology, INDUCTION, Influenza A Virus, H3N2 Subtype, Public Health, Environmental and Occupational Health, NS1 truncation, H3N2, Texas, Infectious Diseases, Influenza A virus, Influenza Vaccines, CROSS-REACTIVITY, Live attenuated vaccine, Molecular Medicine, Cross-protection

Abstract

Control of swine influenza A virus (swIAV) in North America and Europe is complicated because multiple antigenically distinct swIAV strains co-circulate in the field, and no vaccine is available that can provide broad cross-protection against all these swIAVs. In 2017, the first live attenuated influenza vaccine (LAIV) for swine was licensed in the US. The non-structural protein 1 (NS1)-truncated cluster I H3N2 strain A/swine/Texas/4199-2/98 NS1del126 (TX98 LAIV) in this vaccine provides partial cross-protection against heterologous North American cluster II and IV H3N2 swIAV strains. Its efficacy against European or more recent North American H3N2 lineages remains to be investigated. In this study, we evaluated the level of cross-protection against heterologous IAVs representative of the major H3N2 swIAV lineages in Europe and North America. TX98 LAIV prevented both nasal shedding and replication in the lungs of a North American cluster IV H3N2 swIAV for 2/4 pigs, prevented considerable nasal shedding of a North American novel human-like H3N2 swIAV for 2/4 pigs, and reduced replication of a European H3N2 swIAV in the lower respiratory tract to minimal titers for 1/3 pigs. Although TX98 LAIV elicited neutralizing antibodies against the homologous virus in serum and to a lesser extent in nose and lungs, no significant cross-reactive antibody titers against the heterologous swIAVs were detected. Partial cross-protection therefore likely relies on cellular and mucosal immune responses against conserved parts of the swIAV proteins. Since TX98 LAIV can offer partial protection against a broad range of H3N2 swIAVs, it might be a suitable priming vaccine for use in a heterologous prime-boost vaccination strategy.

Published

2022

2. Immunogenicity of the drug 'Live intranasal vaccine for the prevention of pertussis' (GamLPV) with a single use in healthy volunteers

Author

A. Yu. Medkova, A. A. Lidzhiyeva, E. G. Semin, L. N. Sinyashina, R. A. Syundyukova, N. A. Snegireva, I. N. Chernyshova, M. V. Gavrilova, K. K. Bushkova, L. V. Kolobukhina, I. S. Kruzhkova, L. N. Merkulova, M. G. Rusanova, I. N. Dyakov, and G. I. Karatayev

Subjects

live attenuated vaccine, mucosal response, pertussis, Medicine (miscellaneous), General Medicine, bordetella pertussis, immunogenicity, intranasal vaccination, cellular response, Microbiology, humoral response, QR1-502

Abstract

Introduction. A significant increase in the incidence of pertussis in the world, including among adolescents and adults, the prevalence of mild forms of the disease and asymptomatic carrier of bacteria B. pertussis, and the resulting need for mass revaccination of different age groups determine the demand for new vaccines against B. pertussis. In N.F. Gamaleya Federal Research Center for Epidemiology and Microbiology, a live intranasal pertussis vaccine for the prevention of pertussis (GamLPV) has been developed. The GamLPV vaccine underwent preclinical studies that proved its safety and effectiveness in experiments on small laboratory animals and nonhuman monkeys. Safety of vaccine is shown in clinical studies on healthy volunteers.The aim of the study is to assess the immunogenicity of different doses of the drug GamLPV when first used in healthy volunteers.Materials and methods. The study was conducted as randomized placebo-controlled, blind trial with consistent volunteer inclusion and dose escalation. Study ID in clinicaltrials.gov database: NCT03137927 (A Phase I Clinical Study of a GamLPV, a Live Intranasal Bordetella Pertussis Vaccine). The following parameters of humoral and cellular immune responses were assessed in dynamics: levels of specific IgM, IgG and IgA antibodies in blood serum of volunteers and the number of cytokines interleukin-17, tumor necrosis factor-α, interferon-γ produced after specific induction in vitro of blood mononuclears of vaccinated volunteers. Dynamics of attenuated bacteria persistence in nasopharynx of vaccinated volunteers was evaluated.Results. Intranasal vaccination of volunteers with the drug Gam LPV resulted in the formation of a specific humoral (IgG and IgA) and cellular immune response. The dose-dependent nature of immunoglobulin and cytokine production was shown. Attenuated bacteria persisted for a long time in the nose/oropharynx of vaccinated volunteers.Discussion. Good tolerability of all tested doses of the drug justifies the choice for further investigation of a vaccine dose equal to 4 × 109 CFU. At the next stage, the safety and immunogenicity of two-time vaccination of volunteers will be studied.

Published

2022

3. Could live attenuated vaccines better control COVID-19?

Author

Hirotaka Ebina and Shinya Okamura

Subjects

COVID-19 Vaccines, Review, Disease, Vaccines, Attenuated, Viral vector, Immunity, Pandemic, Humans, Medicine, Pandemics, Attenuated vaccine, General Veterinary, General Immunology and Microbiology, SARS-CoV-2, business.industry, Public Health, Environmental and Occupational Health, COVID-19, Review article, Vaccination, Infectious Diseases, Live attenuated vaccine, Immunology, Humoral immunity, Molecular Medicine, business, Vaccine

Abstract

In an effort to control the COVID-19 pandemic, large-scale vaccination is being implemented in various countries using anti-SARS-CoV-2 vaccines based on mRNAs, adenovirus vectors, and inactivated viruses. However, there are concerns regarding adverse effects, such as the induction of fever attributed to mRNA vaccines and pre-existing immunity against adenovirus vectored vaccines or their possible involvement in the development of thrombosis. The induction of antibodies against the adenovirus vector itself constitutes another hindrance, rendering boosting vaccinations ineffective. Additionally, it has been questioned whether inactivated vaccines that predominantly induce humoral immunity are effective against newly arising variants, as some isolated strains were found to be resistant to the serum from COVID-19-recovered patients. Although the number of vaccinated people is steadily increasing on a global scale, it is still necessary to develop vaccines to address the difficulties and concerns mentioned above. Among the various vaccine modalities, live attenuated vaccines have been considered the most effective, since they closely replicate a natural infection without the burden of the disease. In our attempt to provide an additional option to the repertoire of COVID-19 vaccines, we succeeded in isolating temperature-sensitive strains with unique phenotypes that could serve as seeds for a live attenuated vaccine. In this review article, we summarize the characteristics of the currently approved SARS-CoV-2 vaccines and discuss their advantages and disadvantages. In particular, we focus on the novel temperature-sensitive variants of SARS-CoV-2 that we have recently isolated, and their potential application as live-attenuated vaccines. Based on a thorough evaluation of the different vaccine modalities, we argue that it is important to optimize usage not only based on efficacy, but also on the phases of the pandemic. Our findings can be used to inform vaccination practices and improve global recovery from the COVID-19 pandemic.

Published

2021

4. Oronasal or Intramuscular Immunization with a Thermo-Attenuated ASFV Strain Provides Full Clinical Protection against Georgia 2007/1 Challenge

Author

Olivier Bourry, Evelyne Hutet, Mireille Le Dimna, Pierrick Lucas, Yannick Blanchard, Amélie Chastagner, Frédéric Paboeuf, and Marie-Frédérique Le Potier

Subjects

Vaccines, ASF, live attenuated vaccine, oronasal, intramuscular, Infectious Diseases, Swine, Virology, Sus scrofa, Animals, Immunization, Viral Vaccines, African Swine Fever, African Swine Fever Virus

Abstract

African swine fever (ASF) is a contagious viral disease of suids that induces high mortality in domestic pigs and wild boars. Given the current spread of ASF, the development of a vaccine is a priority. During an attempt to inactivate the Georgia 2007/1 strain via heat treatment, we fortuitously generated an attenuated strain called ASFV-989. Compared to Georgia, the ASFV-989 strain genome has a deletion of 7458 nucleotides located in the 5′-end encoding region of MGF 505/360, which allowed for developing a DIVA PCR system. In vitro, in porcine alveolar macrophages, the replication kinetics of the ASFV-989 and Georgia strains were identical. In vivo, specific-pathogen-free (SPF) pigs inoculated with the ASFV-989 strain, either intramuscularly or oronasally, exhibited transient hyperthermia and slightly decreased growth performance. Animals immunized with the ASFV-989 strain showed viremia 100 to 1000 times lower than those inoculated with the Georgia strain and developed a rapid antibody and cell-mediated response. In ASFV-989-immunized pigs challenged 2 or 4 weeks later with the Georgia strain, no symptoms were recorded and no viremia for the challenge strain was detected. These results show that the ASFV-989 strain is a promising non-GMO vaccine candidate that is usable either intramuscularly or oronasally.

Published

2022

5. Evaluation of the Delivery of a Live Attenuated Porcine Reproductive and Respiratory Syndrome Virus as a Unit Solid Dose Injectable Vaccine

Author

Ellie Hayhurst, Emily Rose, Miriam Pedrera, Jane C. Edwards, Natalia Kotynska, Daisy Grainger, Yashar Sadigh, John Flannery, Ludo Bonnet, Ritwik Ritwik, Pawan Dulal, M. Keith Howard, Simon P. Graham, Flannery, John, and Graham, Simon P.

Subjects

Pharmacology, Pig, Infectious Diseases, Live attenuated vaccine, Drug Discovery, Immunology, Porcine reproductive and respiratory syndrome virus, Pharmacology (medical), Solid dose vaccine formulation, porcine reproductive and respiratory syndrome virus, live attenuated vaccine, solid dose vaccine formulation, immunogenicity, pig, Immunogenicity

Abstract

Solid dose vaccine formulation and delivery systems offer potential advantages over traditional liquid vaccine formulations. In addition to enhanced thermostability, needle-free delivery of unit solid dose injectable (USDI) vaccines offers safe, rapid, and error-free administration, with applicability to both human and animal health. Solid dose formulation technologies can be adapted for delivery of different vaccine formats including live attenuated vaccines, which remain the 'gold standard' for many disease targets. Porcine reproductive and respiratory syndrome viruses (PRRSV) cause one of the most economically important diseases affecting the global pig industry. Despite several shortcomings, live attenuated vaccines are widely used to control PRRSV. We optimised a freeze-dried USDI formulation of live attenuated PRRSV-1, which fully retained infectious titre, and evaluated its immunogenicity in comparison to virus delivered in liquid suspension via intramuscular and subcutaneous needle inoculation. Pigs vaccinated with the USDI formulation displayed vaccine viraemia, and PRRSV-specific antibody and T cell responses comparable to animals immunised with the liquid vaccine. The USDI vaccine formulation was stable for at least 6 months when stored refrigerated. These data demonstrate the potential for a solid dose vaccine delivery system as an alternative to conventional needle-syringe delivery of live attenuated PRRSV vaccines.

Published

2022

6. Inmunizaciones en niños, adolescentes y adultos inmunosuprimidos

Author

Luisa Durán and Rodolfo Villena

Subjects

030203 arthritis & rheumatology, live attenuated vaccine, 03 medical and health sciences, immunosuppression, vaccine-preventable diseases, 0302 clinical medicine, immunecompromised host, 030225 pediatrics, Medicine, General Medicine, Immunizations, inactived vaccine

Abstract

Resumen: Los pacientes inmunosuprimidos presentan un riesgo mayor de infecciones, debido a sus disfunciones inmunes, producto de la actividad de su enfermedad y la terapia inmunosupresora. El uso de vacunas disminuye este riesgo, otorgando protección directa e indirecta, a través de la vacunación del paciente y sus contactos. Las vacunas inactivadas han demostrado un perfil de seguridad adecuado en estos pacientes, por lo que no están contraindicadas, aunque su respuesta inmune puede ser inadecuada. Las vacunas vivas atenuadas, formalmente contraindicadas, poseen una información creciente que permite evaluar su riesgo/beneficio de manera individual. Por este motivo es necesario procurar mantener el calendario de vacunas actualizado y complementado, evitando el retraso en esquemas de vacunación y poniéndolo al día lo antes posible, con estrategias basadas en el individuo. Para llevar a cabo esto, se debe conocer y considerar los intervalos entre las vacunas, los esquemas acelerados, la solicitud de vacunas especiales, las aprobaciones vigentes y, finalmente, sus contraindicaciones. Summary: Immunecompromised patients are at higher risk of infections due to their immune dysfunction caused by ongoing disease processes and immunosuppressive therapy.Patient vaccination or vaccination of the people in contact with patients diminishes their risk of infection. Although the immune response of immunocompromised patients might be impaired, the use of inactivated vaccines is safe and it is not contraindicated in these patients. Formerly, live attenuated vaccines were contraindicated in immunecompromised patients, but recently more data supports their use when evaluating case by case the risks and benefits of their application. Thus, it is important to keep and up-to-date, taylor-based and enhanced vaccination schedule in these cases. For this, specialists need to be informed about the availability of regular and special vaccines, their current approvals, vaccine administration protocols under specific situations and vaccine contraindications.

Published

2020

7. Vaccine Safety and Efficacy in Preventing Rotavirus Infection

Author

V. A. Shevtsov, E. E. Evreinova, I. N. Indikova, L. M. Khantimirova, D. V. Gorenkov, and A. V. Rukavishnikov

Subjects

rotavirus infection, 0301 basic medicine, Pediatrics, medicine.medical_specialty, 030106 microbiology, efficacy and safety of vaccines, medicine.disease_cause, Herd immunity, 03 medical and health sciences, 0302 clinical medicine, Rotavirus, Pharmacovigilance, medicine, herd immunity, media_common.cataloged_instance, 030212 general & internal medicine, European union, non-replicating vaccines, media_common, intussusception, live attenuated vaccine, Attenuated vaccine, business.industry, Infant mortality, Clinical trial, Vaccination, Automotive Engineering, Medicine, business, TP248.13-248.65, Biotechnology

Abstract

The rotavirus infection causes acute gastroenteritis and is a major cause of lethal severe dehydrating diarrhoea in children under 5 years of age worldwide. Live attenuated rotavirus vaccines are the only means of preventing severe forms of the disease. The aim of the study was to analyse the twenty-year international experience of prophylactic immunisation against rotavirus infection. The paper summarises safety and efficacy data on the long-term use of Rotarix® (Belgium) and RotaTeq® (USA) for the prevention of rotavirus infection in the WHO European Region, the European Union and other countries. It addresses the development of correlates of immune protection for vaccines as well as evaluation of efficacy and safety of the new vaccines Rotavac® and Rotasiil® (India) in clinical trials. The authors analysed international experience of using the vaccines in countries that do not keep records of infant mortality from diarrhoea. The study summarises the results of clinical studies on the use of new vaccines prequalified by WHO in 2018 in regions with high rates of infant mortality from diarrhoea. It was demonstrated that vaccination not only reduces the rates of hospital admission of immunised children, but also contributes to the development of herd immunity. Rotarix® and RotaTeq® vaccines are authorised or included in the national immunisation schedules of many countries, but this type of vaccination is not mandatory in most of these countries. Vaccination coverage in the EU countries is about 24 %. Alternative vaccination schemes using live attenuated vaccines based on strains derived from newborn children, and parenteral rotavirus vaccines which do not replicate in the intestine may help reduce existing risks. It was concluded that the introduction of live rotavirus vaccines in immunisation schedules should be accompanied by the analysis of incidence of intussusception of the small intestine before and after the introduction of mass immunisation, and by active pharmacovigilance.

Published

2019

8. Developments in Vaccination for Herpes Simplex Virus

Author

Krishnan, Rohini and Stuart, Patrick M.

Subjects

DNA vaccine, Microbiology (medical), live attenuated vaccine, mRNA vaccine, viruses, herpes simplex virus type 2, herpes simplex virus type 1, Review, subunit vaccine, vaccines, Microbiology, QR1-502

Abstract

Herpes simplex virus (HSV) is an alpha herpes virus, with two subtypes: HSV-1 and HSV-2. HSV is one of the most prevalent sexually transmitted infections. It is the cause of severe neonatal infections and a leading cause of infectious blindness in the Western world. As of 2016, 13.2% of the global population ages 15–49 were existing with HSV-2 infection and 66.6% with HSV-1. This high prevalence of disease and the fact that resistance to current therapies is on the rise makes it imperative to develop and discover new methods of HSV prevention and management. Among the arsenal of therapies/treatments for this virus has been the development of a prophylactic or therapeutic vaccine to prevent the complications of HSV reactivation. Our current understanding of the immune responses involved in latency and reactivation provides a unique challenge to the development of vaccines. There are no approved vaccines currently available for either prophylaxis or therapy. However, there are various promising candidates in the pre-clinical and clinical phases of study. Vaccines are being developed with two broad focuses: preventative and therapeutic, some with a dual use as both immunotherapeutic and prophylactic. Within this article, we will review the current guidelines for the treatment of herpes simplex infections, our understanding of the immunological pathways involved, and novel vaccine candidates in development.

Published

2021

9. Development Real-Time PCR Assays to Genetically Differentiate Vaccinated Pigs From Infected Pigs With the Eurasian Strain of African Swine Fever Virus

Author

Elizabeth Ramirez-Medina, Manuel V. Borca, Elizabeth A Vuono, Douglas P. Gladue, Lauro Velazquez-Salinas, Nallely Espinoza, Sarah Pruitt, and Ayushi Rai

Subjects

live attenuated vaccine, Attenuated vaccine, General Veterinary, biology, genetic DIVA test, Veterinary medicine, Virulence, biology.organism_classification, African swine fever virus, Virology, Virus, law.invention, phylogenetics, Diva, Vaccination, Real-time polymerase chain reaction, ASF real time PCR, law, SF600-1100, Veterinary Science, ASFV, Polymerase chain reaction, Original Research

Abstract

Currently, African swine fever virus (ASFV) represents one of the most important economic threats for the global pork industry. Recently, significant advances have been made in the development of potential vaccine candidates to protect pigs against this virus. We have previously developed attenuated vaccine candidates by deleting critical viral genes associated with virulence. Here, we present the development of the accompanying genetic tests to discriminate between infected and vaccinated animals (DIVA), a necessity during an ASFV vaccination campaign. We describe here the development of three independent real-time polymerase chain reaction (qPCR) assays that detect the presence of MGF-360-12L, UK, and I177L genes, which were previously deleted from the highly virulent Georgia strain of ASFV to produce the three recombinant live attenuated vaccine candidates. When compared with the diagnostic reference qPCR that detects the p72 gene, all assays demonstrated comparable levels of sensitivity, specificity, and efficiency of amplification to detect presence/absence of the ASFV Georgia 2007/1 strain (prototype virus of the Eurasian lineage) from a panel of blood samples from naïve, vaccinated, and infected pigs. Collectively, the results of this study demonstrate the potential of these real-time PCR assays to be used as genetic DIVA tests, supporting vaccination campaigns associated with the use of ASFV-ΔMGF, ASFV-G-Δ9GL/ΔUK, and ASFV-ΔI177L or cell culture adapted ASFV-ΔI177LΔLVR live attenuated vaccines in the field.

Published

2021

10. The Feasibility of Using Coxiella burnetii Avirulent Nine Mile Phase II Viable Bacteria as a Live Attenuated Vaccine Against Q fever

Author

Guoquan Zhang, Shawkat Alam, Yan Zhang, and Venkatesh Kumaresan

Subjects

live attenuated vaccine, Attenuated vaccine, biology, Immunology, Virulence, Q fever, RC581-607, Coxiella burnetii, biology.organism_classification, medicine.disease, Microbiology, Nine Mile-Phase I/Phase II LPS, Immune system, Immunization, humoral and cellular immunity, BALB/c mice, Splenocyte, medicine, bacteria, Immunology and Allergy, Immunologic diseases. Allergy, viable avirulent bacteria, CD8

Abstract

This study aimed to explore if viable C. burnetii avirulent Nine Mile phase II (NMII) can elicit protective immunity against virulent NM phase I (NMI) infection. Interestingly, mice immunized with viable NMII elicited significant protection against NMI infection at different time points post-immunization. Viable NMII induced a dose-dependent NMI-specific IgG response in mice, but all doses of NMII-immunized mice conferred a similar level of protection. Comparing different routes of immunization indicated that intranasally immunized mice showed significantly higher levels of protection than other immunization routes. The observation that viable NMII induced a similar level of long-term protection against NMI challenge as the formalin-inactivated NMI vaccine (PIV) suggests that viable NMII bacteria can induce a similar level of long-term protection against virulent NMI challenge as the PIV. Viable NMII also induced significant protection against challenge with virulent Priscilla and Scurry strains, suggesting that viable NMII can elicit broad protection. Immune sera and splenocytes from viable NMII-immunized mice are protective against NMI infection, but immune serum-receiving mice did not control NMI replication. Additionally, viable NMII conferred a comparable level of protection in wild-type, CD4+ T cell-deficient, and CD8+ T cell-deficient mice, and partial protection in B cell-deficient mice. However, NMII-immunized T cell-deficient mice were unable to prevent C. burnetii replication. Thus, both B cells and T cells are required for viable NMII-induced protective immunity but T cells may play a critical role. Collectively, this study demonstrates the feasibility of using avirulent NMII as a live attenuated vaccine against human Q fever.

Published

2021

11. Simultaneous Infection With Porcine Reproductive and Respiratory Syndrome and Influenza Viruses Abrogates Clinical Protection Induced by Live Attenuated Porcine Reproductive and Respiratory Syndrome Vaccination

Author

Tiphany Chrun, Elma Tchilian, Nanchaya Wanasen, Eleni Vatzia, Francisco J. Salguero, Surapong Koonpaew, Emmanuel Atangana Maze, Basudev Paudyal, Matthew Edmans, Veronica Martini, Adam McNee, Simon P. Graham, and Tanuja Manjegowda

Subjects

pig, Swine, animal diseases, viruses, Datasets as Topic, Antibodies, Viral, Madin Darby Canine Kidney Cells, Immunology and Allergy, Original Research, Attenuated vaccine, biology, Coinfection, Respiratory disease, Vaccination, virus diseases, respiratory system, Viral Load, porcine reproductive and respiratory syndrome virus, medicine.anatomical_structure, Cytokines, Female, Viral load, Immunology, Porcine Reproductive and Respiratory Syndrome, Vaccine Efficacy, Viremia, Vaccines, Attenuated, Virus, swine influenza A virus, Dogs, co-infection, Orthomyxoviridae Infections, medicine, Animals, Porcine respiratory and reproductive syndrome virus, live attenuated vaccine, business.industry, Influenza A Virus, H3N2 Subtype, Viral Vaccines, RC581-607, Vaccine efficacy, medicine.disease, Porcine reproductive and respiratory syndrome virus, biology.organism_classification, Virology, Immunologic diseases. Allergy, business, Respiratory tract

Abstract

The porcine respiratory disease complex (PRDC) is responsible for significant economic losses in the pig industry worldwide. Porcine reproductive and respiratory syndrome virus (PRRSV) and swine influenza virus are major viral contributors to PRDC. Vaccines are cost-effective measures for controlling PRRS, however, their efficacy in the context of co-infections has been poorly investigated. In this study, we aimed to determine the effect of PRRSV-2 and swine influenza H3N2 virus co-infection on the efficacy of PRRSV modified live virus (MLV) vaccination, which is widely used in the field. Following simultaneous challenge with contemporary PRRSV-2 and H3N2 field isolates, we found that the protective effect of PRRS MLV vaccination on clinical disease and pathology was abrogated, although viral load was unaffected and antibody responses were enhanced. In contrast, co-infection in non-immunized animals reduced PRRSV-2 viremia and H3N2 virus load in the upper respiratory tract and potentiated T cell responses against both PRRSV-2 and H3N2 in the lung. Further analysis suggested that an upregulation of inhibitory cytokines gene expression in the lungs of vaccinated pigs may have influenced responses to H3N2 and PRRSV-2. These findings provide important insights into the effect of viral co-infections on PRRS vaccine efficacy that may help identity more effective vaccination strategies against PRDC in the field.

Published

2021

12. The Feasibility of Using

Author

Venkatesh, Kumaresan, Shawkat, Alam, Yan, Zhang, and Guoquan, Zhang

Subjects

B-Lymphocytes, live attenuated vaccine, cross-protection, T-Lymphocytes, Immunology, Vaccines, Attenuated, Mice, Nine Mile-Phase I/Phase II LPS, Coxiella burnetii, humoral and cellular immunity, Bacterial Vaccines, BALB/c mice, bacteria, Animals, Feasibility Studies, Q Fever, viable avirulent bacteria, Original Research

Abstract

This study aimed to explore if viable C. burnetii avirulent Nine Mile phase II (NMII) can elicit protective immunity against virulent NM phase I (NMI) infection. Interestingly, mice immunized with viable NMII elicited significant protection against NMI infection at different time points post-immunization. Viable NMII induced a dose-dependent NMI-specific IgG response in mice, but all doses of NMII-immunized mice conferred a similar level of protection. Comparing different routes of immunization indicated that intranasally immunized mice showed significantly higher levels of protection than other immunization routes. The observation that viable NMII induced a similar level of long-term protection against NMI challenge as the formalin-inactivated NMI vaccine (PIV) suggests that viable NMII bacteria can induce a similar level of long-term protection against virulent NMI challenge as the PIV. Viable NMII also induced significant protection against challenge with virulent Priscilla and Scurry strains, suggesting that viable NMII can elicit broad protection. Immune sera and splenocytes from viable NMII-immunized mice are protective against NMI infection, but immune serum-receiving mice did not control NMI replication. Additionally, viable NMII conferred a comparable level of protection in wild-type, CD4+ T cell-deficient, and CD8+ T cell-deficient mice, and partial protection in B cell-deficient mice. However, NMII-immunized T cell-deficient mice were unable to prevent C. burnetii replication. Thus, both B cells and T cells are required for viable NMII-induced protective immunity but T cells may play a critical role. Collectively, this study demonstrates the feasibility of using avirulent NMII as a live attenuated vaccine against human Q fever.

Published

2021

13. Replication/Assembly Defective Avian Flavivirus With Internal Deletions in the Capsid Can Be Used as an Approach for Living Attenuated Vaccine

Author

Yu He, Xiaoli Wang, Jiaqi Guo, Li Mao, Senzhao Zhang, Tao Hu, Mingshu Wang, Renyong Jia, Dekang Zhu, Mafeng Liu, Xinxin Zhao, Qiao Yang, Ying Wu, Shaqiu Zhang, Juan Huang, Sai Mao, Xumin Ou, Qun Gao, Di Sun, Yunya Liu, Ling Zhang, Yanling Yu, Anchun Cheng, and Shun Chen

Subjects

0301 basic medicine, Vaccines, Live, Unattenuated, replication deficient, viruses, assembly deficient, 030106 microbiology, Immunology, Virulence, Virus Replication, immune response, Virus, Cell Line, Flavivirus Infections, protective immunity, 03 medical and health sciences, Immunogenicity, Vaccine, Cricetinae, Animals, Immunology and Allergy, Replicon, Poultry Diseases, Original Research, Sequence Deletion, live attenuated vaccine, Attenuated vaccine, biology, Flavivirus, Virus Assembly, avian Tembusu virus, capsid protein deletion, Vaccination, Viral Vaccines, RC581-607, biology.organism_classification, Virology, Reverse genetics, Ducks, 030104 developmental biology, Viral replication, Capsid, Capsid Proteins, Immunologic diseases. Allergy

Abstract

Avian Tembusu virus (TMUV) is a novel flavivirus causing severe egg drop and fatal encephalitis in avian in Asia. In the present study, we screened the structural and functional requirements of TMUV capsid protein (CP) for viral morphogenesis using reverse genetics methods in combination with replicon packaging assays. TMUV-CP showed dramatic functional and structural flexibility, and even though 44 residues were removed from the N-terminus, it was still capable of packaging replicon RNA; in addition, 33 residues were deleted from the C-terminus (containing nearly the entire α4-helix), and infectious particles were still produced, although α4-α4’ is supposedly vital for CP dimerization and nucleocapsid formation. We further analyzed two mutants (ΔC20-43 and ΔC64-96 viruses) with relatively large deletions that still replicated well in BHK-21 cells. Our data indicate that internal deletions within CP impaired viral replication or assembly, resulting in attenuated virus proliferation in cells and attenuated virulence in duck embryos, and these deletion mutations are quite stable in cell culture. An in vivo assay indicated that both ΔC20-43 virus and ΔC64-96 virus were highly attenuated in ducklings but still immunogenic. Single-dose immunization with ΔC20-43 virus or ΔC64-96 virus could protect ducklings from a lethal challenge with good antigen clearance. Together, our data shed light on replication/assembly defective TMUV with internal deletions in CP and provide an effective approach to attenuate viral virulence in live vaccines without changing the antigen composition.

Published

2021

14. Characteristics of Classical Swine Fever Virus Variants Derived from Live Attenuated GPE

Author

Taksoo, Kim, Loc Tan, Huynh, Shizuka, Hirose, Manabu, Igarashi, Takahiro, Hiono, Norikazu, Isoda, and Yoshihiro, Sakoda

Subjects

live attenuated vaccine, Swine, Genetic Variation, Viral Vaccines, Antibodies, Viral, Vaccines, Attenuated, GPE−, classical swine fever virus, NS5B, Article, Classical Swine Fever, vaccine seed, Viral Proteins, variant, Animals, type I interferon, Amino Acid Sequence, Sequence Alignment

Abstract

The GPE− strain is a live attenuated vaccine for classical swine fever (CSF) developed in Japan. In the context of increasing attention for the differentiating infected from vaccinated animals (DIVA) concept, the achievement of CSF eradication with the GPE− proposes it as a preferable backbone for a recombinant CSF marker vaccine. While its infectious cDNA clone, vGPE−, is well characterized, 10 amino acid substitutions were recognized in the genome, compared to the original GPE− vaccine seed. To clarify the GPE− seed availability, this study aimed to generate and characterize a clone possessing the identical amino acid sequence to the GPE− seed. The attempt resulted in the loss of the infectious GPE− seed clone production due to the impaired replication by an amino acid substitution in the viral polymerase NS5B. Accordingly, replication-competent GPE− seed variant clones were produced. Although they were mostly restricted to propagate in the tonsils of pigs, similarly to vGPE−, their type I interferon-inducing capacity was significantly lower than that of vGPE−. Taken together, vGPE− mainly retains ideal properties for the CSF vaccine, compared with the seed variants, and is probably useful in the development of a CSF marker vaccine.

Published

2021

15. Modern Development and Production of a New Live Attenuated Bacterial Vaccine, SCHU S4

Author

J Wayne, Conlan, Anders, Sjöstedt, H Carl, Gelhaus, Perry, Fleming, Kevan, McRae, Ronald R, Cobb, Roberto, De Pascalis, and Karen L, Elkins

Subjects

live attenuated vaccine, Francisella tularensis, product development, Article, tularemia

Abstract

Inhalation of small numbers of Francisella tularensis subspecies tularensis (Ftt) in the form of small particle aerosols causes severe morbidity and mortality in people and many animal species. For this reason, Ftt was developed into a bona fide biological weapon by the USA, by the former USSR, and their respective allies during the previous century. Although such weapons were never deployed, the 9/11 attack quickly followed by the Amerithrax attack led the U.S. government to seek novel countermeasures against a select group of pathogens, including Ftt. Between 2005–2009, we pursued a novel live vaccine against Ftt by deleting putative virulence genes from a fully virulent strain of the pathogen, SCHU S4. These mutants were screened in a mouse model, in which the vaccine candidates were first administered intradermally (ID) to determine their degree of attenuation. Subsequently, mice that survived a high dose ID inoculation were challenged by aerosol or intranasally (IN) with virulent strains of Ftt. We used the current unlicensed live vaccine strain (LVS), first discovered over 70 years ago, as a comparator in the same model. After screening 60 mutants, we found only one, SCHU S4 ΔclpB, that outperformed LVS in the mouse ID vaccination-respiratory-challenge model. Currently, SCHU S4 ΔclpB has been manufactured under current good manufacturing practice conditions, and tested for safety and efficacy in mice, rats, and macaques. The steps necessary for advancing SCHU S4 ΔclpB to this late stage of development are detailed herein. These include developing a body of data supporting the attenuation of SCHU S4 ΔclpB to a degree sufficient for removal from the U.S. Select Agent list and for human use; optimizing SCHU S4 ΔclpB vaccine production, scale up, and long-term storage; and developing appropriate quality control testing approaches.

Published

2021

16. Deletion Mutants of

Author

Brandi E, Hobbs, Courtney A, Matson, Vasileios I, Theofilou, Tonya J, Webb, Rania H, Younis, and Eileen M, Barry

Subjects

live attenuated vaccine, MFS transporter, organ burdens, Live Vaccine Strain (LVS), flow cytometry, C57BL/6J mice, histopathology, bacterial infections and mycoses, Francisella tularensis, complex mixtures, Article, attenuation, cytokines

Abstract

Francisella tularensis (Ft) is a Gram-negative, facultative intracellular bacterium that is a Tier 1 Select Agent of concern for biodefense for which there is no licensed vaccine. A subfamily of 9 Francisella phagosomal transporter (fpt) genes belonging to the Major Facilitator Superfamily of transporters was identified as critical to pathogenesis and potential targets for attenuation and vaccine development. We evaluated the attenuation and protective capacity of LVS derivatives with deletions of the fptA and fptF genes in the C57BL/6J mouse model of respiratory tularemia. LVSΔfptA and LVSΔfptF were highly attenuated with LD50 values of >20 times that of LVS when administered intranasally and conferred 100% protection against lethal challenge. Immune responses to the fpt mutant strains in mouse lungs on day 6 post-infection were substantially modified compared to LVS and were associated with reduced organ burdens and reduced pathology. The immune responses to LVSΔfptA and LVSΔfptF were characterized by decreased levels of IL-10 and IL-1β in the BALF versus LVS, and increased numbers of B cells, αβ and γδ T cells, NK cells, and DCs versus LVS. These results support a fundamental requirement for FptA and FptF in the pathogenesis of Ft and the modulation of the host immune response.

Published

2021

17. The Conserved Molecular Determinants of Virulence in Dengue Virus

Author

Zuleeza Ahmad and Chit Laa Poh

Subjects

Serotype, Virulence Factors, Dengue Vaccines, Review, Genome, Viral, Dengue virus, Vaccines, Attenuated, medicine.disease_cause, Virus, Dengue fever, Dengue, 03 medical and health sciences, Flaviviridae, Capsid, 0302 clinical medicine, Viral Envelope Proteins, vaccine, medicine, Humans, 3' Untranslated Regions, Dengue vaccine, live attenuated vaccine, Vaccines, Synthetic, Attenuated vaccine, dengue virus, Virulence, biology, Yellow fever, General Medicine, mutations, biology.organism_classification, medicine.disease, Virology, Clinical Trials, Phase III as Topic, Mutation, 030211 gastroenterology & hepatology, 5' Untranslated Regions

Abstract

Dengue virus belongs to the Flaviviridae family which also includes viruses such as the Zika, West Nile and yellow fever virus. Dengue virus generally causes mild disease, however, more severe forms of the dengue virus infection, dengue haemorrhagic fever (DHF) and dengue haemorrhagic fever with shock syndrome (DSS) can also occur, resulting in multiple organ failure and even death, especially in children. The only dengue vaccine available in the market, CYD-TDV offers limited coverage for vaccinees from 9-45 years of age and is only recommended for individuals with prior dengue exposure. A number of mutations that were shown to attenuate virulence of dengue virus in vitro and/or in vivo have been identified in the literature. The mutations which fall within the conserved regions of all four dengue serotypes are discussed. This review hopes to provide information leading to the construction of a live attenuated dengue vaccine that is suitable for all ages, irrespective of the infecting dengue serotype and prior dengue exposure.

Published

2019

18. Commercial Vaccines Do Not Confer Protection against Two Genogroups of Piscirickettsia salmonis, LF-89 and EM-90, in Atlantic Salmon

Author

Carolina Figueroa, Débora Torrealba, Byron Morales-Lange, Luis Mercado, Brian Dixon, Pablo Conejeros, Gabriela Silva, Carlos Soto, and José A. Gallardo

Subjects

General Immunology and Microbiology, General Agricultural and Biological Sciences, pentavalent vaccine, bacterin vaccine, live attenuated vaccine, monovalent vaccine, Piscirickettsiosis, Salmo salar, cohabitation, sea lice, vaccine efficacy, General Biochemistry, Genetics and Molecular Biology

Abstract

In Atlantic salmon, vaccines have failed to control and prevent Piscirickettsiosis, for reasons that remain elusive. In this study, we report the efficacy of two commercial vaccines developed with the Piscirickettsia salmonis isolates AL100005 and AL 20542 against another two genogroups which are considered highly and ubiquitously prevalent in Chile: LF-89 and EM-90. Two cohabitation trials were performed to mimic field conditions and vaccine performance: (1) post-smolt fish were challenged with a single infection of LF-89, (2) adults were coinfected with EM-90, and a low level coinfection of sea lice. In the first trial, the vaccine delayed smolt mortalities by two days; however, unvaccinated and vaccinated fish did not show significant differences in survival (unvaccinated: 60.3%, vaccinated: 56.7%; p = 0.28). In the second trial, mortality started three days later for vaccinated fish than unvaccinated fish. However, unvaccinated and vaccinated fish did not show significant differences in survival (unvaccinated: 64.6%, vaccinated: 60.2%, p = 0.58). Thus, we found no evidence that the evaluated vaccines confer effective protection against the genogroups LF-89 and EM-90 of P. salmonis with estimated relative survival proportions (RPSs) of −9% and −12%, respectively. More studies are necessary to evaluate whether pathogen heterogeneity is a key determinant of the lack of vaccine efficacy against P. salmonis.

Published

2022

19. Recombinant LSDV Strains in Asia: Vaccine Spillover or Natural Emergence?

Author

Frank Vandenbussche, Elisabeth Mathijs, Wannes Philips, Meruyert Saduakassova, Ilse De Leeuw, Akhmetzhan Sultanov, Andy Haegeman, and Kris De Clercq

Subjects

lumpy skin disease virus, homologous vaccine, live attenuated vaccine, spillover, recombination, Asia, Lumpy skin disease virus, Infectious Diseases, Lumpy Skin Disease, Virology, Animals, Cattle, Viral Vaccines, Vaccines, Attenuated

Abstract

From 2017 to 2019, several vaccine-like recombinant strains of lumpy skin disease virus (LSDV) were discovered in Kazakhstan and neighbouring regions of Russia and China. Shortly before their emergence, the authorities in Kazakhstan launched a mass vaccination campaign with the Neethling-based Lumpivax vaccine. Since none of the other countries in the affected region had used a homologous LSDV vaccine, it was soon suspected that the Lumpivax vaccine was the cause of these unusual LSDV strains. In this study, we performed a genome-wide molecular analysis to investigate the composition of two Lumpivax vaccine batches and to establish a possible link between the vaccine and the recent outbreaks. Although labelled as a pure Neethling-based LSDV vaccine, the Lumpivax vaccine appears to be a complex mixture of multiple CaPVs. Using an iterative enrichment/assembly strategy, we obtained the complete genomes of a Neethling-like LSDV vaccine strain, a KSGP-like LSDV vaccine strain and a Sudan-like GTPV strain. The same analysis also revealed the presence of several recombinant LSDV strains that were (almost) identical to the recently described vaccine-like LSDV strains. Based on their InDel/SNP signatures, the vaccine-like recombinant strains can be divided into four groups. Each group has a distinct breakpoint pattern resulting from multiple recombination events, with the number of genetic exchanges ranging from 126 to 146. The enormous divergence of the recombinant strains suggests that they arose during seed production. The recent emergence of vaccine-like LSDV strains in large parts of Asia is, therefore, most likely the result of a spillover from animals vaccinated with the Lumpivax vaccine.

Published

2022

20. Immunization with

Author

Pallab, Chaudhuri, Mani, Saminathan, Syed Atif, Ali, Gurpreet, Kaur, Shiv Varan, Singh, Jonathan, Lalsiamthara, Tapas K, Goswami, Ashwini K, Singh, Sandeep K, Singh, Praveen, Malik, and Raj K, Singh

Subjects

buffalo, live attenuated vaccine, S19Δper, animal diseases, brucellosis, DIVA, complex mixtures, protective efficacy, Article

Abstract

Vaccination of cattle and buffaloes with Brucella abortus strain 19 has been the mainstay for control of bovine brucellosis. However, vaccination with S19 suffers major drawbacks in terms of its safety and interference with serodiagnosis of clinical infection. Brucella abortus S19∆per, a perosamine synthetase wbkB gene deletion mutant, overcomes the drawbacks of the S19 vaccine strain. The present study aimed to evaluate the potential of Brucella abortus S19Δper vaccine candidate in the natural host, buffaloes. Safety of S19∆per, for animals use, was assessed in guinea pigs. Protective efficacy of vaccine was assessed in buffaloes by immunizing with normal dose (4 × 1010 colony forming units (CFU)/animal) and reduced dose (2 × 109 CFU/animal) of S19Δper and challenged with virulent strain of B. abortus S544 on 300 days post immunization. Bacterial persistency of S19∆per was assessed in buffalo calves after 42 days of inoculation. Different serological, biochemical and pathological studies were performed to evaluate the S19∆per vaccine. The S19Δper immunized animals showed significantly low levels of anti-lipopolysaccharides (LPS) antibodies. All the immunized animals were protected against challenge infection with B. abortus S544. Sera from the majority of S19Δper immunized buffalo calves showed moderate to weak agglutination to RBPT antigen and thereby, could apparently be differentiated from S19 vaccinated and clinically-infected animals. The S19Δper was more sensitive to buffalo serum complement mediated lysis than its parent strain, S19. Animals culled at 6-weeks-post vaccination showed no gross lesions in organs and there was comparatively lower burden of infection in the lymph nodes of S19Δper immunized animals. With attributes of higher safety, strong protective efficacy and potential of differentiating infected from vaccinated animals (DIVA), S19Δper would be a prospective alternate to conventional S19 vaccines for control of bovine brucellosis as proven in buffaloes.

Published

2021

21. A live attenuated-vaccine model confers cross-protective immunity against different species of the Leptospira genus

Author

Li Liang, Haritha Adhikarla, Jarlath E. Nally, Albert I. Ko, Katharine A Owers Bonner, Philip L. Felgner, David P. Alt, Mitermayer G. Reis, Peter J. Diggle, Camila Hamond, Vimla Bisht, Elsio A. Wunder, and Camila B. Rodrigues

Subjects

Male, 0301 basic medicine, Serotype, QH301-705.5, Science, Cross Protection, 030106 microbiology, cross-protective immunity, Biology, Vaccines, Attenuated, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, leptospira, Immune system, Immunity, Leptospira, leptospirosis, Animals, Biology (General), Microbiology and Infectious Disease, live attenuated vaccine, Attenuated vaccine, Mesocricetus, General Immunology and Microbiology, General Neuroscience, General Medicine, biology.organism_classification, Virology, Mice, Inbred C57BL, 030104 developmental biology, Immunization, Infectious disease (medical specialty), Bacterial Vaccines, biology.protein, Medicine, Female, Other, Leptospira interrogans, Antibody, Research Article

Abstract

Leptospirosis is the leading zoonotic disease in terms of morbidity and mortality worldwide. Effective prevention is urgently needed as the drivers of disease transmission continue to intensify. The key challenge has been developing a widely applicable vaccine that protects against the >300 serovars that can cause leptospirosis. Live attenuated mutants are enticing vaccine candidates and poorly explored in the field. We evaluated a recently characterized motility-deficient mutant lacking the expression of a flagellar protein, FcpA. Although the fcpA- mutant has lost its ability to cause disease, transient bacteremia was observed. In two animal models, immunization with a single dose of the fcpA- mutant was sufficient to induce a robust anti-protein antibodies response that promoted protection against infection with different pathogenic Leptospira species. Furthermore, characterization of the immune response identified a small repertoire of biologically relevant proteins that are highly conserved among pathogenic Leptospira species and potential correlates of cross-protective immunity., eLife digest Leptospirosis is a life-threatening disease with flu-like symptoms that is caused by bacteria known as Leptospira. It is more common in warmer regions with high rainfall, especially in impoverished areas. The disease is spread in the urine of animals such as rodents, farm animals or dogs. Humans and other animals can get leptospirosis when they come in contact with urine-contaminated water and soil. Current measures to control leptospirosis are largely ineffective. Although a vaccine is available for animals, it only protects against a few types of the 300 disease-causing Leptospira bacteria. It also fails to stop the bacteria from colonizing the kidneys of the infected animals, which means that vaccinated animals can still spread disease. Previous research has shown that inactivating a protein called FcpA, which is necessary for Leptospira bacteria to move, can stop them from infecting hamsters. Moreover, when these animals were exposed to the mutant bacteria, they did not get sick nor developed the disease. Here, Wunder et al. tested whether bacteria lacking the FcpA protein could be used as an attenuated vaccine. This form of vaccine contains live bacteria that have been modified to become harmless but are able to train the immune system to produce a long-lasting immune response against the invaders. The results showed that a single dose of the vaccine was enough to prevent hamsters and mice from dying of leptospirosis. It also worked against several types of Leptospira and could stop them from colonizing mice kidneys. Moreover, Wunder et al. found that the immune system targeted specific proteins that were common to various types of Leptospira, which may explain the broad spectrum of protection the vaccine offered. Rapid urbanization and climate change are among the main drivers of leptospirosis. An effective vaccine for this disease would reduce the public health burden by providing protection against leptospirosis and by reducing the spread of the disease. A next step will be to ensure the mutant Leptospira are safe to use in animals and potentially humans.

Published

2021

22. Development of safe and highly protective live-attenuated SARS-CoV-2 vaccine candidates by genome recoding

Author

Volker Thiel, Tran Thi Nhu Thao, Julia Adler, Theresa C. Firsching, Jakob Trimpert, Nikolaus Osterrieder, Joerg Jores, Fabien Labroussaa, Susanne Kaufer, Dusan Kunec, Thomas Höfler, Achim D. Gruber, Azza Abdelgawad, Kristina Dietert, Nadine Ebert, Daria Vladimirova, Luca D. Bertzbach, and Andelé M. Conradie

Subjects

synthetic attenuated virus engineering, COVID-19 Vaccines, Syrian hamster, viruses, Respiratory System, coronavirus, 610 Medicine & health, Genome, Viral, Disease, Roborovski dwarf hamster, Vaccines, Attenuated, Virus Replication, medicine.disease_cause, Article, General Biochemistry, Genetics and Molecular Biology, Virus, Immunity, Chlorocebus aethiops, Pandemic, medicine, Animals, Humans, codon pair deoptimization, Pandemics, Vero Cells, Coronavirus, Gene Editing, live attenuated vaccine, Attenuated vaccine, 630 Agriculture, Mesocricetus, biology, business.industry, SARS-CoV-2, COVID-19, 500 Naturwissenschaften und Mathematik::570 Biowissenschaften, Biologie::570 Biowissenschaften, Biologie, biology.organism_classification, Virology, Viral replication, genome recoding, Mutation, 570 Life sciences, 590 Animals (Zoology), business

Abstract

Safe and effective vaccines are urgently needed to stop the pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). We construct a series of live attenuated vaccine candidates by large-scale recoding of the SARS-CoV-2 genome and assess their safety and efficacy in Syrian hamsters. Animals were vaccinated with a single dose of the respective recoded virus and challenged 21 days later. Two of the tested viruses do not cause clinical symptoms but are highly immunogenic and induce strong protective immunity. Attenuated viruses replicate efficiently in the upper but not in the lower airways, causing only mild pulmonary histopathology. After challenge, hamsters develop no signs of disease and rapidly clear challenge virus: at no time could infectious virus be recovered from the lungs of infected animals. The ease with which attenuated virus candidates can be produced and administered favors their further development as vaccines to combat the ongoing pandemic., Graphical abstract, Trimpert et al. construct safe and efficacious live attenuated SARS-CoV-2 vaccine candidates by recoding the SARS-CoV-2 genome. The lead vaccine candidate, sCPD9, is apathogenic in Syrian and Roborovski dwarf hamsters. A single intranasal droplet vaccination with sCPD9 induces strong neutralizing antibody responses and protects hamsters from disease caused by SARS-CoV-2.

Published

2021

23. Antibody-Dependent Enhancement: A Challenge for Developing a Safe Dengue Vaccine

Author

Rajgokul K. Shanmugam, Rahul Shukla, Richa Ahuja, Navin Khanna, and Viswanathan Ramasamy

Subjects

0301 basic medicine, Microbiology (medical), dengue virus (DENV), viruses, 030106 microbiology, Immunology, lcsh:QR1-502, Dengue Vaccines, Review, Dengue virus, Antibodies, Viral, medicine.disease_cause, Microbiology, lcsh:Microbiology, Epitope, Virus, virus-like particle, Dengue fever, 03 medical and health sciences, Cellular and Infection Microbiology, Viral Envelope Proteins, dengue vaccine, Dengvaxia, medicine, Animals, Antibody-dependent enhancement, antibody-dependent enhancement (ADE), Dengue vaccine, live attenuated vaccine, Attenuated vaccine, business.industry, Dengue Virus, Entry into host, medicine.disease, Antibodies, Neutralizing, Antibody-Dependent Enhancement, dengue, Virology, 030104 developmental biology, Infectious Diseases, business

Abstract

In 2019, the United States Food and Drug Administration accorded restricted approval to Sanofi Pasteur's Dengvaxia, a live attenuated vaccine (LAV) for dengue fever, a mosquito-borne viral disease, caused by four antigenically distinct dengue virus serotypes (DENV 1-4). The reason for this limited approval is the concern that this vaccine sensitized some of the dengue-naïve recipients to severe dengue fever. Recent knowledge about the nature of the immune response elicited by DENV viruses suggests that all LAVs have inherent capacity to predominantly elicit antibodies (Abs) against the pre-membrane (prM) and fusion loop epitope (FLE) of DENV. These antibodies are generally cross-reactive among DENV serotypes carrying a higher risk of promoting Antibody-Dependent Enhancement (ADE). ADE is a phenomenon in which suboptimal neutralizing or non-neutralizing cross-reactive antibodies bind to virus and facilitate Fcγ receptor mediated enhanced entry into host cells, followed by its replication, and thus increasing the cellular viral load. On the other hand, antibody responses directed against the host-cell receptor binding domain of DENV envelope domain-III (EDIII), exhibit a higher degree of type-specificity with lower potential of ADE. The challenges associated with whole DENV-based vaccine strategies necessitate re-focusing our attention toward the designed dengue vaccine candidates, capable of inducing predominantly type-specific immune responses. If the designed vaccines elicited predominantly EDIII-directed serotype specific antibodies in the absence of prM and FLE antibodies, this could avoid the ADE phenomenon largely associated with the prM and FLE antibodies. The generation of type-specific antibodies to each of the four DENV serotypes by the designed vaccines could avoid the immune evasion mechanisms of DENVs. For the enhanced vaccine safety, all dengue vaccine candidates should be assessed for the extent of type-specific (minimal ADE) vs. cross-reactive (ADE promoting) neutralizing antibodies. The type-specific EDIII antibodies may be more directly related to protection from disease in the absence of ADE promoted by the cross-reactive antibodies.

Published

2020

24. Salmonella Typhimurium Lacking YjeK as a Candidate Live Attenuated Vaccine Against Invasive Salmonella Infection

Author

Seong-Tshool Hong, Tae-Wook Hahn, Bogyo Jung, Soyeon Park, Eunsuk Kim, and Hyunjin Yoon

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Salmonella, elongation factor P, Immunology, Mutant, Virulence, Spleen, Salmonella infection, Biology, medicine.disease_cause, non-typhoidal Salmonella, Microbiology, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Immunology and Allergy, Original Research, live attenuated vaccine, immune protection, Attenuated vaccine, medicine.disease, virulence, Vaccination, 030104 developmental biology, medicine.anatomical_structure, Salmonella Typhimurium, YjeK, lcsh:RC581-607, 030215 immunology

Abstract

Non-typhoidal Salmonella (NTS) causes gastrointestinal infection, which is commonly self-limiting in healthy humans but may lead to invasive infection at extraintestinal sites, leading to bacteremia and focal systemic infections in the immunocompromised. However, a prophylactic vaccine against invasive NTS has not yet been developed. In this work, we explored the potential of a ΔyjeK mutant strain as a live attenuated vaccine against invasive NTS infection. YjeK in combination with YjeA is required for the post-translational modification of elongation factor P (EF-P), which is critical for bacterial protein synthesis. Therefore, malfunction of YjeK and YjeA-mediated EF-P activation might extensively influence protein expression during Salmonella infection. Salmonella lacking YjeK showed substantial alterations in bacterial motility, antibiotics resistance, and virulence. Interestingly, deletion of the yjeK gene increased the expression levels of Salmonella pathogenicity island (SPI)-1 genes but decreased the transcription levels of SPI-2 genes, thereby influencing bacterial invasion and survival abilities in contact with host cells. In a mouse model, the ΔyjeK mutant strain alleviated the levels of splenomegaly and bacterial burdens in the spleen and liver in comparison with the wild-type strain. However, mice immunized with the ΔyjeK mutant displayed increased Th1- and Th2-mediated immune responses at 28 days post-infection, promoting cytokines and antibodies production. Notably, the Th2-associated antibody response was highly induced by administration of the ΔyjeK mutant strain. Consequently, vaccination with the ΔyjeK mutant strain protected 100% of the mice against challenge with lethal invasive Salmonella and significantly relieved bacterial burdens in the organs. Collectively, these results suggest that the ΔyjeK mutant strain can be exploited as a promising live attenuated NTS vaccine.

Published

2020

25. A T3SS Regulator Mutant of

Author

Shihui, Zhou, Xueting, Tu, Huanying, Pang, Rowena, Hoare, Sean J, Monaghan, Jiajun, Luo, and Jichan, Jian

Subjects

live attenuated vaccine, tyeA, type III secretory system, Vaccines, Attenuated, Anti-Bacterial Agents, Fish Diseases, Cellular and Infection Microbiology, regulator, Vibrio Infections, Bacterial Vaccines, Animals, Vibrio alginolyticus, Zebrafish, Original Research

Abstract

Vibrio alginolyticus is a major cause of Vibriosis in farmed marine aquatic animals and has caused large economic losses to the Asian aquaculture industry in recent years. Therefore, it is necessary to control V. alginolyticus effectively. The virulence mechanism of V. alginolyticus, the Type III secretion system (T3SS), is closely related to its pathogenicity. In this study, the T3SS gene tyeA was cloned from V. alginolyticus wild-type strain HY9901 and the results showed that the deduced amino acid sequence of V. alginolyticus tyeA shared 75–83% homology with other Vibrio spp. The mutant strain HY9901ΔtyeA was constructed by Overlap-PCR and homologous recombination techniques. The HY9901ΔtyeA mutant exhibited an attenuated swarming phenotype and an ~40-fold reduction in virulence to zebrafish. However, the HY9901ΔtyeA mutant showed no difference in growth, biofilm formation and ECPase activity. Antibiotic susceptibility test was observed that wild and mutant strains were extremely susceptible to Amikacin, Minocycline, Gentamicin, Cefperazone; and resistant to oxacillin, clindamycin, ceftazidime. In contrast wild strains are sensitive to tetracycline, chloramphenicol, kanamycin, doxycycline, while mutant strains are resistant to them. qRT-PCR was employed to analyze the transcription levels of T3SS-related genes, the results showed that compared with HY9901 wild type, ΔtyeA had increased expression of vscL, vscK, vscO, vopS, vopN, vscN, and hop. Following vaccination with the mutant strain, zebrafish had significantly higher survival than controls following infection with the wild-type HY9901 (71.2% relative percent survival; RPS). Analysis of immune gene expression by qPCR showed that vaccination with HY9901ΔtyeA increased the expression of IgM, IL-1β, IL-6, and TNF-α in zebrafish. This study provides evidence of protective efficacy of a live attenuated vaccine targeting the T3SS of V. alginolyticus which may be facilitated by up-regulated pro-inflammatory and immunoglobulin-related genes.

Published

2020

26. Evaluation of glycoprotein E subunit and live attenuated varicella-zoster virus vaccines formulated with a single-strand RNA-based adjuvant

Author

Hae Li Ko, Jung Eun Lee, Hun Kim, Hyo Jung Park, Lee Su Jeen, Hyun Joo Lee, and Jae-Hwan Nam

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Herpesvirus 3, Human, medicine.medical_treatment, viruses, RNA adjuvant, gE subunit vaccine, medicine.disease_cause, Antibodies, Viral, Mice, 0302 clinical medicine, Viral Envelope Proteins, Cricetinae, Immunology and Allergy, Herpes Zoster Vaccine, Neutralizing antibody, shingles, Original Research, chickenpox, Immunity, Cellular, Attenuated vaccine, virus diseases, Vaccines, Subunit, Antibody, Adjuvant, lcsh:Immunologic diseases. Allergy, Immunology, Guinea Pigs, CHO Cells, Biology, Vaccines, Attenuated, varicella‐zoster virus, Herpes Zoster, Virus, varicella-zoster virus, live attenuated vaccine, 03 medical and health sciences, Cricetulus, Antigen, Adjuvants, Immunologic, medicine, Animals, Humans, RNA, Messenger, Varicella zoster virus, Virology, Mice, Inbred C57BL, 030104 developmental biology, A549 Cells, Humoral immunity, biology.protein, lcsh:RC581-607, 030215 immunology

Abstract

Introduction Varicella‐zoster virus (VZV), a human alphaherpesvirus 3, elicits both chickenpox and shingles and/or postherpetic neuralgia. A live attenuated vaccine (LAV) and glycoprotein E (gE) subunit vaccine were developed to prevent VZV‐induced diseases. We recently reported that single‐strand RNA (ssRNA) based on the intergenic region of the internal ribosome entry site of cricket paralysis virus (CrPV) is an effective adjuvant for protein‐based and virus‐like particle‐based vaccines. Here, Chinese hamster ovary expression system and an LAV from Oka/SK strains. Methods We appraised the adjuvant effect of the same CrPV ssRNA encoding the gE gene formulated in the two vaccines using VZV‐primed C57BL/6 mice and guinea pigs. Humoral immunity and cell‐mediated immunity were assessed by enzyme‐linked immunosorbent assay (ELISA) and ELISPOT in gE subunit vaccine and by ELISA and fluorescent antibody to membrane antigen in LAV. Results The gE subunit vaccine‐induced gE‐specific antibodies and CD4+ T‐cell responses (indicated by interferon‐γ [IFN‐γ] and interleukin‐2 secretion) in the ssRNA‐based adjuvant containing the VZV gE gene. Therefore, an ssRNA adjuvant combined with gE antigen can trigger the innate immune response and induce an adaptive immune response to ultimately activate humoral and cell‐mediated responses. VZV LAV could also induce VZV‐specific antibodies and IFN‐γ stimulated by LAV, whereas the effect of ssRNA as a vaccine adjuvant could not be confirmed. However, the ssRNA adjuvant increased VZV‐specific neutralizing antibody response. Conclusions Taken together, these results highlight that the gE subunit vaccine and LAV developed in this study can be functional VZV vaccines, and ssRNAs appear to function better as adjuvants in a subunit vaccine than in an LAV., We evaluated two new varicella‐zoster virus (VSV) vaccines, a glycoprotein E (gE) subunit‐based vaccine and live attenuated vaccine, that were formulating with single‐strand RNA (ssRNA) as a potential adjuvant. The gE subunit vaccine and LAV developed in this study can be functional VZV vaccines, and ssRNAs appear to function better as adjuvants in a subunit vaccine than in an LAV.

Published

2019

27. Development of Next Generation

Author

Malihe, Masomian, Zuleeza, Ahmad, Lai Ti, Gew, and Chit Laa, Poh

Subjects

live attenuated vaccine, pneumococcal surface-exposed protein, Streptococcus pneumoniae, nanoparticle, Review, vaccines, bacterium-like particle

Abstract

Streptococcus pneumoniae is a major pathogen causing pneumonia with over 2 million deaths annually, especially in young children and the elderly. To date, at least 98 different pneumococcal capsular serotypes have been identified. Currently, the vaccines for prevention of S. pneumoniae infections are the 23-valent pneumococcal polysaccharide-based vaccine (PPV23) and the pneumococcal conjugate vaccines (PCV10 and PCV13). These vaccines only cover some pneumococcal serotypes and are unable to protect against non-vaccine serotypes and unencapsulated S. pneumoniae. This has led to a rapid increase in antibiotic-resistant non-vaccine serotypes. Hence, there is an urgent need to develop new, effective, and affordable pneumococcal vaccines, which could cover a wide range of serotypes. This review discusses the new approaches to develop effective vaccines with broad serotype coverage as well as recent development of promising pneumococcal vaccines in clinical trials. New vaccine candidates are the inactivated whole-cell vaccine strain (Δpep27ΔcomD mutant) constructed by mutations of specific genes and several protein-based S. pneumoniae vaccines using conserved pneumococcal antigens, such as lipoprotein and surface-exposed protein (PspA). Among the vaccines in Phase 3 clinical trials are the pneumococcal conjugate vaccines, PCV-15 (V114) and 20vPnC. The inactivated whole-cell and several protein-based vaccines are either in Phase 1 or 2 trials. Furthermore, the recent progress of nanoparticles that play important roles as delivery systems and adjuvants to improve the performance, as well as the immunogenicity of the nanovaccines, are reviewed.

Published

2019

28. Cross-genotype protection of live-attenuated vaccine candidate for severe fever with thrombocytopenia syndrome virus in a ferret model

Author

Min-Ah Yu, Young Ki Choi, Benjamin Brennan, Kwang-Min Yu, Su-Jin Park, Young-Il Kim, Younho Choi, and Jae U. Jung

Subjects

viruses, bunyavirus, Microbiology, Virus, 03 medical and health sciences, Immune system, medicine, emerging banyangvirus, 030304 developmental biology, 0303 health sciences, Tick-borne disease, live attenuated vaccine, Multidisciplinary, Attenuated vaccine, SFTS, 030306 microbiology, business.industry, Biological Sciences, medicine.disease, Virology, 3. Good health, Severe fever with thrombocytopenia syndrome, Humoral immunity, ferret model, business, Viral load, Severe fever with thrombocytopenia syndrome virus

Abstract

Significance Severe fever with thrombocytopenia syndrome virus (SFTSV) is an emerging viral pathogen discovered in 2009. The virus is present in countries of East Asia and is transmitted through the bite of an infected Haemaphysalis longicornis tick. SFTSV disease is associated with high morbidity and is often fatal. Despite the incidence of disease, no antiviral therapy or vaccine has been approved for use. Here, we report and assess 2 live attenuated viruses as vaccine candidates in our recently described ferret model of infection. We show that the viruses caused no clinical disease or mortality in healthy animals. Immunized animals mounted a robust humoral immune response to a single dose of virus, and this response protected the animals from a lethal challenge., Severe fever with thrombocytopenia syndrome (SFTS) virus (SFTSV) is an emerging tick-borne virus classified within the Banyangvirus genus. SFTS disease has been reported throughout East Asia since 2009 and is characterized by high fever, thrombocytopenia, and leukopenia and has a 12 to 30% case fatality rate. Due to the recent emergence of SFTSV, there has been little time to conduct research into preventative measures aimed at combatting the virus. SFTSV is listed as one of the World Health Organization’s Prioritized Pathogens for research into antiviral therapeutics and vaccine development. Here, we report 2 attenuated recombinant SFTS viruses that induce a humoral immune response in immunized ferrets and confer complete cross-genotype protection to lethal challenge. Animals infected with rHB29NSsP102A or rHB2912aaNSs (both genotype D) had a reduced viral load in both serum and tissues and presented without high fever, thrombocytopenia, or mortality associated with infection. rHB29NSsP102A- or rHB2912aaNSs-immunized animals developed a robust anti-SFTSV immune response against cross-genotype isolates of SFTSV. This immune response was capable of neutralizing live virus in a focus-reduction neutralization test (FRNT) and was 100% protective against a cross-genotype lethal challenge with the CB1/2014 strain of SFTSV (genotype B). Thus, using our midsized, aged ferret infection model, we demonstrate 2 live attenuated vaccine candidates against the emerging pathogen SFTSV.

Published

2019

29. A Novel Live Attenuated Vaccine Candidate Protects Against Heterologous Senecavirus A Challenge

Author

Bishwas Sharma, Maureen H. V. Fernandes, Marcelo de Lima, Lok R. Joshi, Steve Lawson, and Diego G. Diel

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Cellular immunity, Swine, T-Lymphocytes, Immunology, Picornaviridae, Biology, Antibodies, Viral, Vaccines, Attenuated, Recombinant virus, Virus, 03 medical and health sciences, 0302 clinical medicine, Animals, Immunology and Allergy, Viral shedding, Neutralizing antibody, Original Research, Swine Diseases, live attenuated vaccine, Vaccines, Synthetic, Picornaviridae Infections, Attenuated vaccine, Immunogenicity, Viral Vaccines, inactivated vaccine, Antibodies, Neutralizing, Virology, Senecavirus A, Seneca Valley virus, 030104 developmental biology, Inactivated vaccine, biology.protein, Immunization, recombinant virus, lcsh:RC581-607, 030215 immunology

Abstract

Senecavirus A (SVA) is an emerging picornavirus causing vesicular disease (VD) clinically indistinguishable from foot-and-mouth disease (FMD) in pigs. Currently there are no vaccines currently available for SVA. Here we developed a recombinant SVA strain (rSVAm SacII) using reverse genetics and assessed its immunogenicity and protective efficacy in pigs. In vivo characterization of the rSVAm SacII strain demonstrated that the virus is attenuated, as evidenced by absence of lesions, decreased viremia and virus shedding in inoculated animals. Notably, while attenuated, rSVA mSacII virus retained its immunogenicity as high neutralizing antibody (NA) responses were detected in inoculated animals. To assess the immunogenicity and protective efficacy of rSVA mSacII, 4-week-old piglets were sham-immunized or immunized with inactivated or live rSVA mSacII virus-based formulations. A single immunization with live rSVA mSacII virus via the intramuscular (IM) and intranasal (IN) routes resulted in robust NA responses with antibodies being detected between days 3–7 pi. Neutralizing antibody responses in animals immunized with the inactivated virus via the IM route were delayed and only detected after a booster on day 21 pi. Immunization with live virus resulted in recall T cell proliferation (CD4+, CD8+, and CD4+/CD8+ T cells), demonstrating efficient stimulation of cellular immunity. Notably, a single dose of the live attenuated vaccine candidate resulted in protection against heterologous SVA challenge, as demonstrated by absence of overt disease and reduced viremia, virus shedding and viral load in tissues. The live attenuated vaccine candidate developed here represents a promising alternative to prevent and control SVA in swine.

Published

2019

30. Emerging Highly Virulent Porcine Epidemic Diarrhea Virus: Molecular Mechanisms of Attenuation and Rational Design of Live Attenuated Vaccines

Author

Yixuan J. Hou and Qiuhong Wang

Subjects

0301 basic medicine, Swine, 030106 microbiology, coronavirus, Virulence, Review, Vaccines, Attenuated, medicine.disease_cause, Catalysis, lcsh:Chemistry, Inorganic Chemistry, 03 medical and health sciences, Immunity, medicine, Animals, Physical and Theoretical Chemistry, lcsh:QH301-705.5, Molecular Biology, porcine epidemic diarrhea virus, attenuation, Spectroscopy, Coronavirus, Swine Diseases, live attenuated vaccine, Attenuated vaccine, biology, Organic Chemistry, Alphacoronavirus, Viral Vaccines, General Medicine, biology.organism_classification, Virology, Computer Science Applications, virulence, Vaccination, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, Vero cell, Colostrum, Coronavirus Infections, Porcine epidemic diarrhea virus

Abstract

The highly virulent porcine epidemic diarrhea virus (PEDV) emerged in China in 2010. It infects pigs of all ages, and causes severe diarrhea and high mortality rates in newborn pigs, leading to devastating economic losses in the pork industry worldwide. Effective and safe vaccines against highly virulent PEDV strains are still unavailable, hampering the further prevention, control and eradication of the disease in herds. Vaccination of pregnant sows with live attenuated vaccines (LAVs) is the most effective strategy to induce lactogenic immunity in the sows, which provides A passive protection of suckling piglets against PEDV via the colostrum (beestings, or first milk) and milk. Several LAV candidates have been developed via serially passaging the highly virulent PEDV isolates in non-porcine Vero cells. However, their efficacies in the induction of sufficient protection against virulent PEDV challenge vary in vivo. In this review, we summarize the current knowledge of the virulence-related mutations of PEDV and their potential roles in PEDV attenuation in vivo. With the successful development of reverse genetics systems for PEDV, we also discuss how to use them to generate promising LAV candidates that are safe, effective and genetically stable. This article provides timely insight into the rational design of effective and safe PEDV LAV candidates.

Published

2019

31. Herpes Zoster and Diabetes Mellitus: A Review

Author

Marianthi Papagianni, Symeon Metallidis, and Konstantinos Tziomalos

Subjects

medicine.medical_specialty, viruses, Endocrinology, Diabetes and Metabolism, Herpes zoster, Population, Post-herpetic neuralgia, Review, 030204 cardiovascular system & hematology, Virus, 03 medical and health sciences, Diabetes mellitus, 0302 clinical medicine, Internal Medicine, medicine, 030212 general & internal medicine, Risk factor, education, education.field_of_study, Attenuated vaccine, integumentary system, business.industry, Incidence (epidemiology), Vaccination, virus diseases, medicine.disease, Dermatology, Live attenuated vaccine, Neuralgia, Adjuvanted vaccine, business

Abstract

Accumulating evidence suggests that diabetes mellitus (DM) represents an important risk factor for both herpes zoster and post-herpetic neuralgia. Moreover, post-herpetic neuralgia appears to be more severe and persistent in diabetic patients. On the other hand, a novel vaccine against varicella-zoster virus (VZV) was recently introduced in clinical practice. Given the increased risk and severity of herpes zoster infection in patients with DM, this vaccine might be useful in this population. However, there are limited data regarding the efficacy and safety of vaccination against herpes zoster in the diabetic population. The aim of the present review is to discuss the incidence and consequences of herpes zoster infection in DM and to comment on the role of vaccination against VZV in these patients.

Published

2018

32. Immunization with Brucella abortus S19Δper Conferred Protection in Water Buffaloes against Virulent Challenge with B. abortus Strain S544

Author

Praveen Malik, Shiv Varan Singh, Syed A. Ali, Sandeep Singh, Pallab Chaudhuri, A.K. Singh, Gurpreet Kaur, Raj Kumar Singh, Mani Saminathan, Jonathan Lalsiamthara, and Tapas Kumar Goswami

Subjects

S19Δper, animal diseases, Immunology, Virulence, DIVA, Biology, complex mixtures, Serology, Microbiology, Antigen, Drug Discovery, medicine, Pharmacology (medical), protective efficacy, buffalo, Pharmacology, live attenuated vaccine, Attenuated vaccine, Brucellosis, medicine.disease, Vaccination, Infectious Diseases, Immunization, brucellosis, biology.protein, Medicine, Antibody

Abstract

Vaccination of cattle and buffaloes with Brucella abortus strain 19 has been the mainstay for control of bovine brucellosis. However, vaccination with S19 suffers major drawbacks in terms of its safety and interference with serodiagnosis of clinical infection. Brucella abortus S19∆per, a perosamine synthetase wbkB gene deletion mutant, overcomes the drawbacks of the S19 vaccine strain. The present study aimed to evaluate the potential of Brucella abortus S19Δper vaccine candidate in the natural host, buffaloes. Safety of S19∆per, for animals use, was assessed in guinea pigs. Protective efficacy of vaccine was assessed in buffaloes by immunizing with normal dose (4 × 1010 colony forming units (CFU)/animal) and reduced dose (2 × 109 CFU/animal) of S19Δper and challenged with virulent strain of B. abortus S544 on 300 days post immunization. Bacterial persistency of S19∆per was assessed in buffalo calves after 42 days of inoculation. Different serological, biochemical and pathological studies were performed to evaluate the S19∆per vaccine. The S19Δper immunized animals showed significantly low levels of anti-lipopolysaccharides (LPS) antibodies. All the immunized animals were protected against challenge infection with B. abortus S544. Sera from the majority of S19Δper immunized buffalo calves showed moderate to weak agglutination to RBPT antigen and thereby, could apparently be differentiated from S19 vaccinated and clinically-infected animals. The S19Δper was more sensitive to buffalo serum complement mediated lysis than its parent strain, S19. Animals culled at 6-weeks-post vaccination showed no gross lesions in organs and there was comparatively lower burden of infection in the lymph nodes of S19Δper immunized animals. With attributes of higher safety, strong protective efficacy and potential of differentiating infected from vaccinated animals (DIVA), S19Δper would be a prospective alternate to conventional S19 vaccines for control of bovine brucellosis as proven in buffaloes.

Published

2021

33. Response to Measles, Mumps and Rubella (MMR) Vaccine in Transfusion-Dependent Patients

Author

Silverio Perrotta, Saverio Misso, Nicoletta Di Maio, Rita Tomeo, Valentina Verde, Domenico Roberti, Saverio Scianguetta, Maddalena Casale, Maria Grazia Di Girolamo, Casale, M., Di Maio, N., Verde, V., Scianguetta, S., Di Girolamo, M. G., Tomeo, R., Roberti, D., Misso, S., and Perrotta, S.

Subjects

0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Pediatrics, medicine.medical_specialty, Mump, Immunology, MMR vaccine, Measles, Rubella, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Measle, Drug Discovery, medicine, measles, Pharmacology (medical), 030212 general & internal medicine, transfusion, Pharmacology, live attenuated vaccine, Attenuated vaccine, business.industry, Immunogenicity, rubella, medicine.disease, Vaccination, Red blood cell, 030104 developmental biology, Infectious Diseases, Medicine, mumps, business, red blood cells

Abstract

Measles, mumps and rubella (MMR) still determine significant morbidity and mortality, although a highly effective vaccine is available. Postponing the MMR vaccination until 6 months after the last red blood cell (RBC) transfusion is recommended, but this delay is incompatible with chronic transfusions. The present study aimed at investigating the impact of blood transfusions on the immunogenicity of the MMR vaccine. In this observational study, a group of 45 transfusion- dependent (TD) patients was compared to 24 non-transfusion-dependent (NTD) patients. Immunity to measles was achieved in 35 (78%) TD and 21 (88%) NTD subjects (p = 0.7), to mumps in 36 (80%) TD and 21 (88%) NTD subjects (p = 0.99), and to rubella in 40 (89%) TD and 23 (96%) NTD subjects (p = 0.99). No significant difference was observed in the number of non-immune individuals or those with doubtful protection between the two groups (p &gt, 0.05). The mean IgG value, assayed in 50 pre-storage leukoreduced RBC units, was 0.075 ± 0.064 mg/mL, ten times lower than the level assumed in blood units and considered detrimental to the immune response in TD patients. This work shows a favorable response to MMR vaccination in TD and NTDT patients and paves the way for further larger studies assessing the impact of chronic transfusions on vaccine response.

Published

2021

34. African Horse Sickness Caused by Genome Reassortment and Reversion to Virulence of Live, Attenuated Vaccine Viruses, South Africa, 2004–2014

Author

Darren P. Martin, Phillippa Burger, Carina W. Lourens, John Duncan Grewar, Alan John Guthrie, Esthea Rossouw, N. James MacLachlan, Christopher Joone, Camilla Theresa Weyer, Peter Coetzee, Estelle Hildegard Venter, and Misha le Grange

Subjects

0301 basic medicine, Serotype, Epidemiology, viruses, Reassortment, African Horse Sickness Virus, genome reassortment, lcsh:Medicine, Disease Outbreaks, South Africa, African Horse Sickness, Phylogeny, Attenuated vaccine, biology, Viral Vaccine, African Horse Sickness Caused by Genome Reassortment and Reversion to Virulence of Live, Attenuated Vaccine Viruses, South Africa, 2004–2014, asymptomatic viral infections, Infectious Diseases, African horse sickness, Reassortant Viruses, Microbiology (medical), Genotype, Genome, Viral, Vaccines, Attenuated, vaccine progenitor availability, History, 21st Century, Polymorphism, Single Nucleotide, environmental vaccine identification, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Animals, lcsh:RC109-216, Horses, Serotyping, live attenuated vaccine, Whole Genome Sequencing, reversion, Research, lcsh:R, veterinary epidemiology, Outbreak, Viral Vaccines, vaccine transmission, biology.organism_classification, Virology, virulence, 030104 developmental biology

Abstract

Epidemiologic and phylogenetic analyses show repeated outbreaks derived from vaccine viruses., African horse sickness (AHS) is a hemorrhagic viral fever of horses. It is the only equine disease for which the World Organization for Animal Health has introduced specific guidelines for member countries seeking official recognition of disease-free status. Since 1997, South Africa has maintained an AHS controlled area; however, sporadic outbreaks of AHS have occurred in this area. We compared the whole genome sequences of 39 AHS viruses (AHSVs) from field AHS cases to determine the source of 3 such outbreaks. Our analysis confirmed that individual outbreaks were caused by virulent revertants of AHSV type 1 live, attenuated vaccine (LAV) and reassortants with genome segments derived from AHSV types 1, 3, and 4 from a LAV used in South Africa. These findings show that despite effective protection of vaccinated horses, polyvalent LAV may, paradoxically, place susceptible horses at risk for AHS.

Published

2016

35. Evaluation of the Safety and Protection Efficacy of

Author

Qiuchun, Li, Yue, Zhu, Jingwei, Ren, Zhuang, Qiao, Chao, Yin, Honghong, Xian, Yu, Yuan, Shizhong, Geng, and Xinan, Jiao

Subjects

live attenuated vaccine, spiC, Salmonella enterica serovar Enteritidis (S. Enteritidis), Article, nmpC, rfaL

Abstract

Salmonella enterica serovar Enteritidis (S. Enteritidis) is a host-ranged pathogen that can infect both animals and humans. Poultry and poultry products are the main carriers of S. Enteritidis, which can be transmitted to humans through the food chain. To eradicate the prevalence of S. Enteritidis in poultry farms, it is necessary to develop novel vaccines against the pathogen. In this study, we constructed two vaccine candidates, CZ14-1∆spiC∆nmpC and CZ14-1∆spiC∆rfaL, and evaluated their protective efficacy. Both mutant strains were much less virulent than the parental strain, as determined by the 50% lethal dose (LD50) for three-day-old specific-pathogen free (SPF) White Leghorns and Hyline White chickens. Immunization with the mutant candidates induced highly specific humoral immune responses and expression of cytokines IFN-γ, IL-1β, and IL-6. In addition, the mutant strains were found to be persistent for almost three weeks post-infection. The survival percentages of chickens immunized with CZ14-1∆spiC∆nmpC and CZ14-1∆spiC∆rfaL reached 80% and 75%, respectively, after challenge with the parental strain. Overall, these results demonstrate that the two mutant strains can be developed as live attenuated vaccines.

Published

2019

36. Serotype-Independent Protection Against Invasive Pneumococcal Infections Conferred by Live Vaccine With lgt Deletion

Author

A-Yeung Jang, Ki Bum Ahn, Yong Zhi, Hyun-Jung Ji, Jing Zhang, Seung Hyun Han, Huichen Guo, Sangyong Lim, Joon Yong Song, Jae Hyang Lim, and Ho Seong Seo

Subjects

lcsh:Immunologic diseases. Allergy, 0301 basic medicine, Serotype, Immunology, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Streptococcus pneumoniae, Immunology and Allergy, Medicine, Pathogen, live attenuated vaccine, Attenuated vaccine, business.industry, Immunogenicity, lipoprotein, medicine.disease, Virology, Pneumococcal infections, 030104 developmental biology, Pneumococcal vaccine, Immunization, Lgt, mucosal immunity, lcsh:RC581-607, business, 030215 immunology

Abstract

Streptococcus pneumoniae is the most common respiratory bacterial pathogen among cases of community-acquired infection in young children, older adults, and individuals with underlying medical conditions. Although capsular polysaccharide-based pneumococcal vaccines have contributed to significant decrease in invasive pneumococcal infections, these vaccines have some limitations, including limited serotype coverage, lack of effective mucosal antibody responses, and high costs. In this study, we investigated the safety and immunogenicity of a live, whole-cell pneumococcal vaccine constructed by deleting the gene for prolipoprotein diacylglyceryl transferase (lgt) from the encapsulated pneumococcal strain TIGR4 (TIGR4Δlgt) for protection against heterologous pneumococcal strains. Pneumococcal strain TIGR4 was successfully attenuated by deletion of lgt, resulting in the loss of inflammatory activity and virulence. TIGR4Δlgt colonized the nasopharynx long enough to induce strong mucosal IgA and IgG2b-dominant systemic antibody responses that were cross-reactive to heterologous pneumococcal serotypes. Finally, intranasal immunization with TIGR4Δlgt provided serotype-independent protection against pneumococcal challenge in mice. Taken together, our results suggest that TIGR4Δlgt is an avirulent and attractive broad-spectrum pneumococcal vaccine candidate. More broadly, we assert that modulation of such “master” metabolic genes represents an emerging strategy for developing more effective vaccines against numerous infectious agents.

Published

2019

37. Burkholderia pseudomallei Δ tonB Δ hcp1 Live Attenuated Vaccine Strain Elicits Full Protective Immunity against Aerosolized Melioidosis Infection

Author

Daniel Tapia, Janice J. Endsley, Preeti Bharaj, Alfredo G. Torres, David H. Walker, Brittany N. Ross, Paul B. Kilgore, Nittaya Khakhum, and Julia N. Myers

Subjects

0301 basic medicine, Burkholderia pseudomallei, Melioidosis, 030106 microbiology, hcp1, lcsh:QR1-502, Microbiology, lcsh:Microbiology, tonB, Th1, 03 medical and health sciences, Burkholderia mallei, Immune system, humoral immunity, medicine, Molecular Biology, live attenuated vaccine, Attenuated vaccine, biology, business.industry, Immunogenicity, Glanders, medicine.disease, biology.organism_classification, Vaccination, 030104 developmental biology, melioidosis, Th17, business

Abstract

Burkholderia pseudomallei is a Gram-negative facultative intracellular bacterium and the causative agent of melioidosis, a severe infectious disease found throughout the tropics. This organism is closely related to Burkholderia mallei, the etiological agent of glanders disease which primarily affects equines. These two pathogenic bacteria are classified as Tier 1 select agents due to their amenability to aerosolization, limited treatment options, and lack of an effective vaccine. We have previously successfully demonstrated the immunogenicity and protective efficacy of a live attenuated vaccine strain, B. malleiΔtonB Δhcp1 (CLH001). Thus, we applied this successful approach to the development of a similar vaccine against melioidosis by constructing the B. pseudomalleiΔtonB Δhcp1 (PBK001) strain. C57BL/6 mice were vaccinated intranasally with the live attenuated PBK001 strain and then challenged with wild-type B. pseudomallei K96243 by the aerosol route. Immunization with strain PBK001 resulted in full protection (100% survival) against acute aerosolized melioidosis with very low bacterial burden as observed in the lungs, livers, and spleens of immunized mice. PBK001 vaccination induced strong production of B. pseudomallei-specific serum IgG antibodies and both Th1 and Th17 CD4+ T cell responses. Further, humoral immunity appeared to be essential for vaccine-induced protection, whereas CD4+ and CD8+ T cells played a less direct immune role. Overall, PBK001 was shown to be an effective attenuated vaccine strain that activates a robust immune response and offers full protection against aerosol infection with B. pseudomallei. IMPORTANCE In recent years, an increasing number of melioidosis cases have been reported in several regions where melioidosis is endemic and in areas where melioidosis had not commonly been diagnosed. Currently, the estimated burden of disease is around 165,000 new cases annually, including 89,000 cases that have fatal outcomes. This life-threatening infectious disease is caused by B. pseudomallei, which is classified as a Tier 1 select agent. Due to the high case fatality rate, intrinsic resistance to multiple antibiotic treatments, susceptibility to infection via the aerosol route, and potential use as a bioweapon, we have developed an effective live attenuated PBK001 vaccine capable of protecting against aerosolized melioidosis.

Published

2019

38. Serotype-Independent Protection Against Invasive Pneumococcal Infections Conferred by Live Vaccine With

Author

A-Yeung, Jang, Ki Bum, Ahn, Yong, Zhi, Hyun-Jung, Ji, Jing, Zhang, Seung Hyun, Han, Huichen, Guo, Sangyong, Lim, Joon Yong, Song, Jae Hyang, Lim, and Ho Seong, Seo

Subjects

Male, Immunology, Serogroup, Vaccines, Attenuated, Pneumococcal Infections, Pneumococcal Vaccines, Mice, Immunogenicity, Vaccine, Bacterial Proteins, Transferases, Nasopharynx, Animals, Immunity, Mucosal, Administration, Intranasal, Bacterial Capsules, Original Research, live attenuated vaccine, Virulence, lipoprotein, Antibodies, Bacterial, Immunoglobulin Isotypes, Mice, Inbred C57BL, RAW 264.7 Cells, Streptococcus pneumoniae, Vaccines, Inactivated, Genes, Bacterial, Lgt, mucosal immunity

Abstract

Streptococcus pneumoniae is the most common respiratory bacterial pathogen among cases of community-acquired infection in young children, older adults, and individuals with underlying medical conditions. Although capsular polysaccharide-based pneumococcal vaccines have contributed to significant decrease in invasive pneumococcal infections, these vaccines have some limitations, including limited serotype coverage, lack of effective mucosal antibody responses, and high costs. In this study, we investigated the safety and immunogenicity of a live, whole-cell pneumococcal vaccine constructed by deleting the gene for prolipoprotein diacylglyceryl transferase (lgt) from the encapsulated pneumococcal strain TIGR4 (TIGR4Δlgt) for protection against heterologous pneumococcal strains. Pneumococcal strain TIGR4 was successfully attenuated by deletion of lgt, resulting in the loss of inflammatory activity and virulence. TIGR4Δlgt colonized the nasopharynx long enough to induce strong mucosal IgA and IgG2b-dominant systemic antibody responses that were cross-reactive to heterologous pneumococcal serotypes. Finally, intranasal immunization with TIGR4Δlgt provided serotype-independent protection against pneumococcal challenge in mice. Taken together, our results suggest that TIGR4Δlgt is an avirulent and attractive broad-spectrum pneumococcal vaccine candidate. More broadly, we assert that modulation of such “master” metabolic genes represents an emerging strategy for developing more effective vaccines against numerous infectious agents.

Published

2019

39. Pathogenicity and immunogenicity of attenuated porcine epidemic diarrhea virus PC22A strain in conventional weaned pigs

Author

Shristi Ghimire, Chun-Ming Lin, Anastasia N. Vlasova, Linda J. Saif, Patricia A. Boley, Qiuhong Wang, Stephanie N. Langel, and Yixuan J. Hou

Subjects

Diarrhea, Swine, 040301 veterinary sciences, Weaning, Biology, Vaccines, Attenuated, Virus, 0403 veterinary science, Random Allocation, 03 medical and health sciences, Immunogenicity, Vaccine, Blood serum, Mucosal immunity, Immunity, Porcine epidemic diarrhea virus (PEDV), medicine, Animals, 030304 developmental biology, 0303 health sciences, lcsh:Veterinary medicine, Attenuated vaccine, General Veterinary, Porcine epidemic diarrhea virus, Immunogenicity, Viral Vaccines, 04 agricultural and veterinary sciences, General Medicine, Weaned pigs, biology.organism_classification, Virology, Vaccination, Live attenuated vaccine, lcsh:SF600-1100, medicine.symptom, Coronavirus Infections, Research Article

Abstract

Background Porcine epidemic diarrhea virus (PEDV) causes diarrhea in all ages of pigs with 50–100% mortality rates in neonatal piglets. In the United States, inactivated and subunit PEDV vaccines for pregnant sows are available, but fail to induce sufficient protection in neonatal piglets farrowed from PEDV naïve sows. A safe and efficacious live attenuated vaccine that can prime mucosal immune responses is urgently needed. In this study, we evaluated the safety and efficacy of two attenuated PEDV vaccine candidates, the emerging non-S INDEL PEDV strain PC22A at the 100th cell culture passage level - Clone no. 4 (P100C4) and at the 120th passage level (P120), in weaned pigs. Results Four groups of 40-day-old weaned pigs were inoculated orally with PEDV PC22A-P3 (virulent), -P100C4, -P120, and mock, respectively, and challenged with the P3 virus at 24 days post-inoculation (dpi). After inoculation, P3 caused diarrhea in all pigs with a high level of fecal viral RNA shedding. P100C4 and P120 did not cause diarrhea in pigs, although viral RNA was detected in feces of all pigs, except for one P100C4-inoculated pig. Compared with the P120 group, P3- and P100C4-inoculated pigs had higher serum PEDV-specific IgG and viral neutralizing (VN) antibody (Ab) titers at 14 dpi. After the challenge, no pigs in the P3 group but all pigs in the P100C4, P120, and mock groups had diarrhea. Compared with the P120 group, pigs in the P100C4 group had a more rapid decline in fecal PEDV RNA shedding titers, higher titers of serum PEDV-specific IgG, IgA, and VN Abs, and higher numbers of intestinal IgA Ab-secreting cells. Conclusions PEDV PC22A P100C4 and P120 were fully attenuated in weaned pigs but failed to elicit protection against virulent P3 challenge. P100C4 induced higher PEDV-specific antibody responses than P120 post inoculation resulting in a greater anamnestic response post challenge. Therefore, P100C4 potentially could be tested as a priming vaccine or be further modified using reverse genetics. It also can be administered in multiple doses or be combined with inactivated or subunit vaccines and adjuvants as a PEDV vaccination regimen, whose efficacy can be tested in the future. Electronic supplementary material The online version of this article (10.1186/s12917-018-1756-x) contains supplementary material, which is available to authorized users.

Published

2019

40. Genotyping of Infectious Laryngotracheitis Virus (ILTV) Isolates from Western Canadian Provinces of Alberta and British Columbia Based on Partial Open Reading Frame (ORF) a and b

Author

Kevin Fonseca, Mohamed Faizal Abdul-Careem, Frank van der Meer, Carl A. Gagnon, Victor Palomino-Tapia, Madhu Ravi, Delores Peters, Robin King, Ana Perez Contreras, Catalina Barboza-Solis, Tommy Joseph, and Université de Montréal. Faculté de médecine vétérinaire

Subjects

0301 basic medicine, Canada, Sanger sequencing, 040301 veterinary sciences, Virulence, Single-nucleotide polymorphism, Biology, Infectious laryngotracheitis, Article, infectious laryngotracheitis, 0403 veterinary science, 03 medical and health sciences, symbols.namesake, lcsh:Zoology, lcsh:QL1-991, Genotyping, live attenuated vaccine, lcsh:Veterinary medicine, Attenuated vaccine, General Veterinary, Wild type, 04 agricultural and veterinary sciences, Virology, Open reading frame, 030104 developmental biology, genotyping, symbols, lcsh:SF600-1100, Animal Science and Zoology

Abstract

Infectious laryngotracheitis virus (ILTV) causes an acute upper respiratory disease in chickens called infectious laryngotracheitis (ILT). Live attenuated vaccines are effective in disease control, however, they have residual virulence, which makes them able to replicate, cause disease and revert to the original virulent form. Information is scarce on the molecular nature of ILTV that is linked to ILT in Canada. This study aims to determine whether isolates originating from ILT cases in Western Canada are a wild type or vaccine origin. Samples submitted for the diagnosis of ILT between 2009&ndash, 2018 were obtained from Alberta (AB, n = 46) and British Columbia (BC, n = 9). For genotyping, a Sanger sequencing of open reading frame (ORF) a and b was used. A total of 27 from AB, and 5 from BC samples yielded a fragment of 1751 base pairs (bp). Three of the BC samples classified as group IV (CEO vaccine strains) and 2 as group V (CEO revertant). Of the AB samples, 22 samples clustered with group V, 3 with group VI (wild type), and 2 with group VII, VIII, and IX (wild type). Overall, 17 non-synonymous single nucleotide polymorphisms (SNPs) were detected. Further studies are underway to ascertain the virulence and transmission potential of these isolates.

Published

2020

41. Development of Next Generation Streptococcus pneumoniae Vaccines Conferring Broad Protection

Author

Lai Ti Gew, Chit Laa Poh, Malihe Masomian, and Zuleeza Ahmad

Subjects

0301 basic medicine, Serotype, Immunology, lcsh:Medicine, medicine.disease_cause, 03 medical and health sciences, 0302 clinical medicine, Vaccine strain, Antigen, Drug Discovery, Streptococcus pneumoniae, medicine, Pharmacology (medical), 030212 general & internal medicine, Pathogen, streptococcus pneumoniae, Pharmacology, live attenuated vaccine, Attenuated vaccine, business.industry, nanoparticle, Immunogenicity, lcsh:R, vaccines, bacterium-like particle, medicine.disease, Virology, pneumococcal surface-exposed protein, Pneumonia, 030104 developmental biology, Infectious Diseases, business

Abstract

Streptococcus pneumoniae is a major pathogen causing pneumonia with over 2 million deaths annually, especially in young children and the elderly. To date, at least 98 different pneumococcal capsular serotypes have been identified. Currently, the vaccines for prevention of S. pneumoniae infections are the 23-valent pneumococcal polysaccharide-based vaccine (PPV23) and the pneumococcal conjugate vaccines (PCV10 and PCV13). These vaccines only cover some pneumococcal serotypes and are unable to protect against non-vaccine serotypes and unencapsulated S. pneumoniae. This has led to a rapid increase in antibiotic-resistant non-vaccine serotypes. Hence, there is an urgent need to develop new, effective, and affordable pneumococcal vaccines, which could cover a wide range of serotypes. This review discusses the new approaches to develop effective vaccines with broad serotype coverage as well as recent development of promising pneumococcal vaccines in clinical trials. New vaccine candidates are the inactivated whole-cell vaccine strain (Δpep27ΔcomD mutant) constructed by mutations of specific genes and several protein-based S. pneumoniae vaccines using conserved pneumococcal antigens, such as lipoprotein and surface-exposed protein (PspA). Among the vaccines in Phase 3 clinical trials are the pneumococcal conjugate vaccines, PCV-15 (V114) and 20vPnC. The inactivated whole-cell and several protein-based vaccines are either in Phase 1 or 2 trials. Furthermore, the recent progress of nanoparticles that play important roles as delivery systems and adjuvants to improve the performance, as well as the immunogenicity of the nanovaccines, are reviewed.

Published

2020

42. Live Attenuated Tularemia Vaccines for Protection Against Respiratory Challenge With Virulent F. tularensis subsp. tularensis

Author

Marcus A. Horwitz and Qingmei Jia

Subjects

0301 basic medicine, bioterrorism, lcsh:QR1-502, Review, lcsh:Microbiology, Tularemia, Mice, Francisella tularensis, tularemia vaccine, Heat-Shock Proteins, Sequence Deletion, media_common, Attenuated vaccine, Virulence, biology, Type VI Secretion Systems, 3. Good health, Vaccination, Infectious Diseases, homologous vaccine, Bacterial Vaccines, Vaccines, Subunit, Microbiology (medical), Lipoproteins, 030106 microbiology, Immunology, Vaccines, Attenuated, complex mixtures, Microbiology, 03 medical and health sciences, Bacterial Proteins, medicine, Animals, Humans, media_common.cataloged_instance, heterologous vaccine, European union, Bacterial Capsules, live attenuated vaccine, Heterologous vaccine, Superoxide Dismutase, bacterial infections and mycoses, biology.organism_classification, Vaccine efficacy, medicine.disease, Listeria monocytogenes, Virology, Tularemia vaccine, Disease Models, Animal, Oxidative Stress, prime-boost vaccine

Abstract

Francisella tularensis is the causative agent of tularemia and a Tier I bioterrorism agent. In the 1900s, several vaccines were developed against tularemia including the killed "Foshay" vaccine, subunit vaccines comprising F. tularensis protein(s) or lipoproteins(s) in an adjuvant formulation, and the F. tularensis Live Vaccine Strain (LVS); none were licensed in the U.S.A. or European Union. The LVS vaccine retains toxicity in humans and animals-especially mice-but has demonstrated efficacy in humans, and thus serves as the current gold standard for vaccine efficacy studies. The U.S.A. 2001 anthrax bioterrorism attack spawned renewed interest in vaccines against potential biowarfare agents including F. tularensis. Since live attenuated-but not killed or subunit-vaccines have shown promising efficacy and since vaccine efficacy against respiratory challenge with less virulent subspecies holarctica or F. novicida, or against non-respiratory challenge with virulent subsp. tularensis (Type A) does not reliably predict vaccine efficacy against respiratory challenge with virulent subsp. tularensis, the route of transmission and species of greatest concern in a bioterrorist attack, in this review, we focus on live attenuated tularemia vaccine candidates tested against respiratory challenge with virulent Type A strains, including homologous vaccines derived from mutants of subsp. holarctica, F. novicida, and subsp. tularensis, and heterologous vaccines developed using viral or bacterial vectors to express F. tularensis immunoprotective antigens. We compare the virulence and efficacy of these vaccine candidates with that of LVS and discuss factors that can significantly impact the development and evaluation of live attenuated tularemia vaccines. Several vaccines meet what we would consider the minimum criteria for vaccines to go forward into clinical development-safety greater than LVS and efficacy at least as great as LVS, and of these, several meet the higher standard of having efficacy ≥LVS in the demanding mouse model of tularemia. These latter include LVS with deletions in purMCD, sodBFt , capB or wzy; LVS ΔcapB that also overexpresses Type VI Secretion System (T6SS) proteins; FSC200 with a deletion in clpB; the single deletional purMCD mutant of F. tularensis SCHU S4, and a heterologous prime-boost vaccine comprising LVS ΔcapB and Listeria monocytogenes expressing T6SS proteins.

Published

2018

43. Effect of a live attenuated vaccine against Lawsonia intracellularis in weaned and finishing pig settings in Finland

Author

Jouni Junnila, Birger Taneli Tirkkonen, Kati Susanna Peiponen, Mari Heinonen, Departments of Faculty of Veterinary Medicine, Faculty of Veterinary Medicine, Production Animal Medicine, Mari Heinonen / Principal Investigator, Research Centre for Animal Welfare, and Teachers' Academy

Subjects

0301 basic medicine, Swine, animal diseases, Lawsonia Bacteria, Sus scrofa, Weight Gain, 413 Veterinary science, 0403 veterinary science, Anti-Infective Agents, Medicine, Ileitis, Finland, HERDS, Swine Diseases, 2. Zero hunger, lcsh:Veterinary medicine, Attenuated vaccine, IMMUNE-RESPONSES, Vaccination, 04 agricultural and veterinary sciences, General Medicine, 3. Good health, Desulfovibrionaceae Infections, Live attenuated vaccine, Bacterial Vaccines, ILEITIS, Female, medicine.symptom, Average daily weight gain, 040301 veterinary sciences, PROLIFERATIVE ENTEROPATHY, Vaccines, Attenuated, Feed conversion ratio, Lawsonia intracellularis, 03 medical and health sciences, Animal science, Animals, Weaning, Pig, General Veterinary, business.industry, Research, EFFICACY, medicine.disease, 030104 developmental biology, Herd, lcsh:SF600-1100, Energy Metabolism, CHALLENGE, business, Weight gain

Abstract

Background: The intracellular bacterium Lawsonia intracellularis is an important pathogen in modern swine production. The aim of this study was to investigate the effect of a live attenuated L. intracellularis vaccine (Enterisol-Ileitis (R)) on the health and production parameters of weaned and finishing pigs in a commercial Finnish 850-sow farm with diagnosed L. intracellularis infection. The herd was free from enzootic pneumonia, swine dysentery, progressive atrophic rhinitis, sarcoptic mange and salmonellosis. Four weekly groups of approximately 500 piglets were included in the study for a total of approximately 2000 piglets. Half of these piglets were vaccinated at 3 weeks of age and the other half served as controls. The study piglets were ear-tagged with individual numbers and colour-coded and were individually weighed at weaning (4 weeks), delivery to the finishing farm (12-14 weeks) and at slaughter. Mortality, symptoms of diseases and medications of the study piglets were registered in the nursery and finishing unit. Feed conversion rate was calculated for the finishing period and lean meat percentage was measured at slaughter. Results: Vaccinated piglets had a higher live weight than unvaccinated piglets at delivery to the finishing unit (+ 1.18 kg, P = 0.002) and at slaughter (+ 3.57 kg, P

Published

2018

44. Time-Resolved Transposon Insertion Sequencing Reveals Genome-Wide Fitness Dynamics during Infection

Author

Ka Yin Leung, Gabriel Billings, Matthew K. Waldor, Qiyao Wang, Joseph Park, Brigid M. Davis, Guanhua Yang, Troy P. Hubbard, Qin Liu, and Yuanxing Zhang

Subjects

0301 basic medicine, Transposable element, Computational biology, Molecular Dynamics Simulation, Biology, Vaccines, Attenuated, Microbiology, Genome, transposon insertion sequencing, 03 medical and health sciences, Virology, Edwardsiella piscicida, Animals, CRISPR, fitness dynamics and profiles, Clustered Regularly Interspaced Short Palindromic Repeats, pattern analysis of conditional essentiality (PACE), Gene, Pace, Genetics, live attenuated vaccine, Cas9, Enterobacteriaceae Infections, Fishes, Palindrome, Chromosome Mapping, High-Throughput Nucleotide Sequencing, QR1-502, Mutagenesis, Insertional, 030104 developmental biology, Edwardsiella, DNA Transposable Elements, Genetic Fitness, Functional genomics, Research Article

Abstract

Transposon insertion sequencing (TIS) is a powerful high-throughput genetic technique that is transforming functional genomics in prokaryotes, because it enables genome-wide mapping of the determinants of fitness. However, current approaches for analyzing TIS data assume that selective pressures are constant over time and thus do not yield information regarding changes in the genetic requirements for growth in dynamic environments (e.g., during infection). Here, we describe structured analysis of TIS data collected as a time series, termed pattern analysis of conditional essentiality (PACE). From a temporal series of TIS data, PACE derives a quantitative assessment of each mutant’s fitness over the course of an experiment and identifies mutants with related fitness profiles. In so doing, PACE circumvents major limitations of existing methodologies, specifically the need for artificial effect size thresholds and enumeration of bacterial population expansion. We used PACE to analyze TIS samples of Edwardsiella piscicida (a fish pathogen) collected over a 2-week infection period from a natural host (the flatfish turbot). PACE uncovered more genes that affect E. piscicida’s fitness in vivo than were detected using a cutoff at a terminal sampling point, and it identified subpopulations of mutants with distinct fitness profiles, one of which informed the design of new live vaccine candidates. Overall, PACE enables efficient mining of time series TIS data and enhances the power and sensitivity of TIS-based analyses., IMPORTANCE Transposon insertion sequencing (TIS) enables genome-wide mapping of the genetic determinants of fitness, typically based on observations at a single sampling point. Here, we move beyond analysis of endpoint TIS data to create a framework for analysis of time series TIS data, termed pattern analysis of conditional essentiality (PACE). We applied PACE to identify genes that contribute to colonization of a natural host by the fish pathogen Edwardsiella piscicida. PACE uncovered more genes that affect E. piscicida’s fitness in vivo than were detected using a terminal sampling point, and its clustering of mutants with related fitness profiles informed design of new live vaccine candidates. PACE yields insights into patterns of fitness dynamics and circumvents major limitations of existing methodologies. Finally, the PACE method should be applicable to additional “omic” time series data, including screens based on clustered regularly interspaced short palindromic repeats with Cas9 (CRISPR/Cas9).

Published

2017

45. Long term follow-up study to evaluate immunogenicity and safety of a single dose of live attenuated hepatitis a vaccine in children

Author

Anju Aggarwal, Gaurav Vishnoi, Apurba Ghosh, Monjori Mitra, Amey Mane, Nitin Shah, Suparna Chatterjee, Mma Faridi, VS Sankaranarayanan, Nisha Bhattacharyya, and Ganesh Kadhe

Subjects

Male, Pediatrics, medicine.medical_specialty, Immunology, Hepatitis A vaccine, India, immunization, Hepatitis A Antibodies, children, antibody, medicine, Humans, Immunology and Allergy, Seroconversion, Child, Pharmacology, live attenuated vaccine, Hepatitis A Vaccines, Attenuated vaccine, business.industry, Immunogenicity, Antibody titer, Infant, Hepatitis A, medicine.disease, Surgery, Vaccination, Child, Preschool, Female, Viral hepatitis, business, Research Paper, Follow-Up Studies

Abstract

Worldwide, viral hepatitis continues to be a cause of considerable morbidity and mortality. Mass immunization with a single dose of live attenuated HAV has been shown to significantly reduce disease burden in the community. This was a phase IV, 5-year follow up study carried out at 4 centers (Kolkata, Delhi, Mumbai and Chennai) across India. The subjects with antibody titer 20 mIU/mL). The seroconversion rates considering seroprotection levels of anti-HAV antibody titer >20 mIU/mL, following vaccination starting from 6 weeks, 6 months, 12 months, 24 months, 36 months, 48 months and 60 months were 95.1%, 97.9%, 98.3%, 96.2%, 97.8%, 92.6% and 97.3%, respectively. The geometric mean concentration (GMC) over the years increased from 64.9 mIU/mL at 6 weeks to 38.1 mIU/mL and 135.2 mIU/mL at 6 months and 12 months, respectively and was maintained at 127.1 mIU/mL at 60 months. In conclusion, the result of this 5-year follow up study showed that the single dose of live attenuated vaccine is well tolerated and provides long-term immunogenicity in healthy Indian children.

Published

2015

46. Safety and immunogenicity of single dose live attenuated varicella vaccine (VR 795 Oka strain) in healthy Indian children: A randomized controlled study

Author

Raju C Shah, Manish Narang, Suparna Chaterjee, Sucheta Roy, Gandhali Bhat, Ganesh Kadhe, Mma Faridi, Amey Mane, Monjori Mitra, Nisha Bhattacharya, Harish Choudhury, Apurba Ghosh, and Nitin Shah

Subjects

Male, Drug-Related Side Effects and Adverse Reactions, Varicella vaccine, LICENSED VACCINES/Research Papers, Immunology, India, Enzyme-Linked Immunosorbent Assay, immunogenicity, Antibodies, Viral, Vaccines, Attenuated, law.invention, Chickenpox Vaccine, Randomized controlled trial, law, Humans, Immunology and Allergy, Medicine, Chicken pox, Child, Pharmacology, live attenuated vaccine, Attenuated vaccine, biology, business.industry, Immunogenicity, Infant, Oka Strain, Virology, Healthy Volunteers, Tolerability, Immunization, Child, Preschool, Immunoglobulin G, biology.protein, Female, Antibody, business

Abstract

Varicella, an acute viral systemic infection that may cause lifelong latent infection with the potential for causing clinical reactivation, may be prevented by immunization. The present study was an open label, randomized, controlled, phase III, multicentre trial, conducted to evaluate and compare the safety, tolerability and immunogenicity of a freeze dried live attenuated Oka strain Varicella Vaccine (VR 795 Oka strain) with Varilrix (Oka-RIT strain) in children. A total of 268 healthy Indian children aged 12 months to 12 y with baseline VZV IgG antibody ( 0.05). The test live attenuated vaccine was found to be highly immunogenic, safe and comparable to Varilrix used in control arm.

Published

2015

47. Immunization of horses with a polyvalent live-attenuated African horse sickness vaccine: Serological response and disease occurrence under field conditions

Author

Massimo Scacchia, Romolo Salini, Umberto Molini, Gaetano Federico Ronchi, Adrianatus Maseke, Giuseppe Marucchella, Attilio Pini, and Mauro Di Ventura

Subjects

Serotype, Veterinary medicine, Serum neutralization, Immunology, Disease, Microbiology, Serology, African horse sickness, Field conditions, Live attenuated vaccine, Infectious Diseases, Public Health, Environmental and Occupational Health, Medicine, Attenuated vaccine, biology, business.industry, lcsh:RM1-950, Environmental and Occupational Health, biology.organism_classification, Vaccination, lcsh:Therapeutics. Pharmacology, Immunization, biology.protein, Public Health, Antibody, business

Abstract

African horse sickness (AHS) is a non-contagious, insect-borne disease of equids caused by a RNA virus (AHSV), which belongs to the genus Orbivirus, family Reoviridae. The disease is endemic in sub-Saharan and western Africa, where prevention strictly depends upon vaccination. The present paper aims at evaluating the serological response and the occurrence of AHS in horses bred under field condition and regularly immunized using the commercially available live attenuated vaccine (LAV) produced by Onderstepoort Biological Products. The study was carried out in a farm located in the district of Windhoek (Namibia), where the disease is endemic. A total of 72 cross-breed horses, out of the 150 housed on the farm, were subdivided in six age groups, from 2 to 7 years-old. Each group consisted of 12 heads which were born during the same breed- ing season and had undergone from four to nine vaccination courses. AHSV specific immune response was evaluated by serum-virus neutralization test. Data about the clinical occurrence of the AHS from 2006 to 2011 were made available. The immune response, in terms of number of seropositive horses and serum neutralizing titers, was quite variable among horses and against different serotypes. Neutralizing antibodies against all serotypes were recorded in all the horses only after eight vaccination courses at 6 years of age onwards. Immune response to AHSV-5 and 9, which are not included in the LAV formulation, were also established. A severe AHS epidemic occurred in Namibia in 2011. On the farm under study, a total of 32 animals were clinically affected, 12 died, 11 of them were 2 year-old or younger. Our data confirm that vaccination with LAV is a useful tool to reduce the severity of the disease in ende- mic areas. However, clinical and sometimes fatal AHS can still affect young vaccinated horses, thus high- lighting the necessity to better understand the immune response to AHSV and to dispose of more effective vaccines. 2015 The Authors. Published by Elsevier Ltd. This is an open access article under the CC BY-NC-ND license

Published

2015

48. Plasmid DNA initiates replication of yellow fever vaccine in vitro and elicits virus-specific immune response in mice

Author

Igor S. Lukashevich, Brian Nickols, Peter Pushko, Jenny D. Jokinen, Irina Tretyakova, and Rachmat Hidajat

Subjects

DNA vaccine, Yellow fever vaccine, Antibodies, Viral, Vaccines, Attenuated, Virus Replication, Virus, Article, DNA vaccination, Mice, Virology, Chlorocebus aethiops, Yellow Fever, 17D vaccine, medicine, Vaccines, DNA, Animals, Vero Cells, Mice, Inbred BALB C, Attenuated vaccine, biology, Flavivirus, YFV, Viral Vaccine, Yellow Fever Vaccine, Viral Vaccines, biology.organism_classification, 3. Good health, Vaccination, Viral replication, Live attenuated vaccine, Yellow fever virus, medicine.drug, Plasmids

Abstract

Yellow fever (YF) causes an acute hemorrhagic fever disease in tropical Africa and Latin America. To develop a novel experimental YF vaccine, we applied iDNA infectious clone technology. The iDNA represents plasmid that encodes the full-length RNA genome of 17D vaccine downstream from a cytomegalovirus (CMV) promoter. The vaccine was designed to transcribe the full-length viral RNA and to launch 17D vaccine virus in vitro and in vivo. Transfection with 10ng of iDNA plasmid was sufficient to start replication of vaccine virus in vitro. Safety of the parental 17D and iDNA-derived 17D viruses was confirmed in AG129 mice deficient in receptors for IFN-α/β/γ. Finally, direct vaccination of BALB/c mice with a single 20μg dose of iDNA plasmid resulted in seroconversion and elicitation of virus-specific neutralizing antibodies in animals. We conclude that iDNA immunization approach combines characteristics of DNA and attenuated vaccines and represents a promising vaccination strategy for YF.

Published

2014

49. Varicella and herpes zoster vaccine development: lessons learned

Author

Judith Breuer, Charlotte Warren-Gash, and Harriet Forbes

Subjects

0301 basic medicine, Herpes Zoster Vaccine, viruses, Immunology, Postmarketing surveillance, herpes zoster, Review, medicine.disease_cause, Vaccines, Attenuated, Varicella, Chickenpox Vaccine, 03 medical and health sciences, 0302 clinical medicine, Chickenpox, Drug Discovery, post-marketing surveillance, medicine, Product Surveillance, Postmarketing, Humans, vaccine safety, 030212 general & internal medicine, Latency (engineering), Drug Approval, Pharmacology, Neurotropic virus, Clinical Trials as Topic, live attenuated vaccine, Attenuated vaccine, integumentary system, vaccine effectiveness, business.industry, Varicella zoster virus, virus diseases, vaccine efficacy, Vaccine efficacy, Virology, 3. Good health, Vaccination, 030104 developmental biology, Treatment Outcome, Vaccines, Subunit, Molecular Medicine, subunit vaccine, business

Abstract

Introduction: Before vaccination, varicella zoster virus (VZV), which is endemic worldwide, led to almost universal infection. This neurotropic virus persists lifelong by establishing latency in sensory ganglia, where its reactivation is controlled by VZV-specific T-cell immunity. Lifetime risk of VZV reactivation (zoster) is around 30%. Vaccine development was galvanised by the economic and societal burden of VZV, including debilitating zoster complications that largely affect older individuals. Areas covered: We describe the story of development, licensing and implementation of live attenuated vaccines against varicella and zoster. We consider the complex backdrop of VZV virology, pathogenesis and immune responses in the absence of suitable animal models and examine the changing epidemiology of VZV disease. We review the vaccines’ efficacy, safety, effectiveness and coverage using evidence from trials, observational studies from large routine health datasets and clinical post-marketing surveillance studies and outline newer developments in subunit and inactivated vaccines. Expert commentary: Safe and effective, varicella and zoster vaccines have already made major inroads into reducing the burden of VZV disease globally. As these live vaccines have the potential to reactivate and cause clinical disease, developing alternatives that do not establish latency is an attractive prospect but will require better understanding of latency mechanisms.

Published

2017

50. Attenuated Actinobacillus pleuropneumoniae double-deletion mutant S-8∆clpP/apxIIC confers protection against homologous or heterologous strain challenge

Author

Gang Li, Long Zhou, Fang Xie, Chunlai Wang, Ning Cui, Siguo Liu, and Yanhe Zhang

Subjects

0301 basic medicine, Swine, animal diseases, 030106 microbiology, Mutant, Heterologous, Virulence, Microbiology, 03 medical and health sciences, Mice, Immune system, Actinobacillus Infections, Animals, Actinobacillus pleuropneumoniae, Porcine pleuropneumonia, Interleukin 4, Swine Diseases, Mice, Inbred BALB C, Attenuated vaccine, General Veterinary, biology, General Medicine, biology.organism_classification, veterinary(all), Virology, 030104 developmental biology, Live attenuated vaccine, Bacterial Vaccines, Interleukin 12, Gene Deletion, Research Article

Abstract

Background Actinobacillus pleuropneumoniae is the etiological agent of porcine pleuropneumonia, which leads to large economic losses to the swine industry worldwide. In this study, S-8△clpP△apxIIC, a double-deletion mutant of A. pleuropneumoniae was constructed, and its safety and protective efficacy were evaluated in pigs. Results The S-8△clpP△apxIIC mutant exhibited attenuated virulence in a murine (BALB/c) model, and caused no detrimental effects on pigs even at a dose of up to 1.0 × 109 CFU. Furthermore, the S-8△clpP△apxIIC mutant was able to induce a strong immune response in pigs, which included high levels of IgG1 and IgG2, stimulated gamma interferon (IFN-γ), interleukin 12 (IL-12), and interleukin 4 (IL-4) production, and conferred effective protection against the lethal challenge with A. pleuropneumoniae serovars 7 or 5a. The pigs in the S-8△clpP△apxIIC immunized groups have no lesions and reduced bacterial loads in the lung tissue after challenge. Conclusions The data obtained in this study suggest that the S-8△clpP△apxIIC mutant can serve as a highly immunogenic and potential live attenuated vaccine candidate against A. pleuropneumoniae infection.

Published

2016