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21 results on '"Masavuli, Makutiro G."'

1. Long-term perturbation of the peripheral immune system months after SARS-CoV-2 infection

Author

Ryan, Feargal J, Hope, Christopher M, Masavuli, Makutiro G, Lynn, Miriam A, Mekonnen, Zelalem A, Yeow, Arthur Eng Lip, Garcia-Valtanen, Pablo, Al-Delfi, Zahraa, Gummow, Jason, Ferguson, Catherine, O’Connor, Stephanie, Reddi, Benjamin AJ, Hissaria, Pravin, Shaw, David, Kok-Lim, Chuan, Gleadle, Jonathan M, Beard, Michael R, Barry, Simon C, Grubor-Bauk, Branka, and Lynn, David J

Subjects
Emerging Infectious Diseases, Vaccine Related, Pneumonia & Influenza, Lung, Pneumonia, Prevention, Infectious Diseases, Genetics, Biodefense, 2.1 Biological and endogenous factors, Aetiology, Infection, Good Health and Well Being, Antibodies, Viral, COVID-19, Humans, Immune System, SARS-CoV-2, Post-Acute COVID-19 Syndrome, Immunity, RNA-Seq, T cell, Antibody responses, Convalescent patients, Immunophenotyping, Long COVID, Post-acute sequelae of COVID-19, Post COVID-19 condition, Medical and Health Sciences, General & Internal Medicine
Abstract

BackgroundSevere acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is a highly infectious respiratory virus which is responsible for the coronavirus disease 2019 (COVID-19) pandemic. It is increasingly clear that recovered individuals, even those who had mild COVID-19, can suffer from persistent symptoms for many months after infection, a condition referred to as "long COVID", post-acute sequelae of COVID-19 (PASC), post-acute COVID-19 syndrome, or post COVID-19 condition. However, despite the plethora of research on COVID-19, relatively little is known about the molecular underpinnings of these long-term effects.MethodsWe have undertaken an integrated analysis of immune responses in blood at a transcriptional, cellular, and serological level at 12, 16, and 24 weeks post-infection (wpi) in 69 patients recovering from mild, moderate, severe, or critical COVID-19 in comparison to healthy uninfected controls. Twenty-one of these patients were referred to a long COVID clinic and > 50% reported ongoing symptoms more than 6 months post-infection.ResultsAnti-Spike and anti-RBD IgG responses were largely stable up to 24 wpi and correlated with disease severity. Deep immunophenotyping revealed significant differences in multiple innate (NK cells, LD neutrophils, CXCR3+ monocytes) and adaptive immune populations (T helper, T follicular helper, and regulatory T cells) in convalescent individuals compared to healthy controls, which were most strongly evident at 12 and 16 wpi. RNA sequencing revealed significant perturbations to gene expression in COVID-19 convalescents until at least 6 months post-infection. We also uncovered significant differences in the transcriptome at 24 wpi of convalescents who were referred to a long COVID clinic compared to those who were not.ConclusionsVariation in the rate of recovery from infection at a cellular and transcriptional level may explain the persistence of symptoms associated with long COVID in some individuals.

Published
2022

2. SARS-CoV-2 Omicron variant escapes neutralizing antibodies and T cell responses more efficiently than other variants in mild COVID-19 convalescents

Author

Garcia-Valtanen, Pablo, Hope, Christopher M, Masavuli, Makutiro G, Yeow, Arthur Eng Lip, Balachandran, Harikrishnan, Mekonnen, Zelalem A, Al-Delfi, Zahraa, Abayasingam, Arunasingam, Agapiou, David, Stella, Alberto Ospina, Aggarwal, Anupriya, Bouras, George, Gummow, Jason, Ferguson, Catherine, O’Connor, Stephanie, McCartney, Erin M, Lynn, David J, Maddern, Guy, Gowans, Eric J, Reddi, Benjamin AJ, Shaw, David, Kok-Lim, Chuan, Beard, Michael R, Weiskopf, Daniela, Sette, Alessandro, Turville, Stuart G, Bull, Rowena A, Barry, Simon C, and Grubor-Bauk, Branka

Subjects
Infectious Diseases, Pneumonia & Influenza, Pneumonia, Prevention, Biodefense, Lung, Immunization, Vaccine Related, Emerging Infectious Diseases, Infection, Good Health and Well Being, Antibodies, Neutralizing, Antibodies, Viral, COVID-19, Humans, Reinfection, SARS-CoV-2, Spike Glycoprotein, Coronavirus, T-Lymphocytes, T cell immunity, Variant of Concern, antibody response, antigen drift, memory B cells, virus neutralization
Abstract

Coronavirus disease 2019 (COVID-19) convalescents living in regions with low vaccination rates rely on post-infection immunity for protection against re-infection with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). We evaluate humoral and T cell immunity against five variants of concern (VOCs) in mild-COVID-19 convalescents at 12 months after infection with ancestral virus. In this cohort, ancestral, receptor-binding domain (RBD)-specific antibody and circulating memory B cell levels are conserved in most individuals, and yet serum neutralization against live B.1.1.529 (Omicron) is completely abrogated and significantly reduced for other VOCs. Likewise, ancestral SARS-CoV-2-specific memory T cell frequencies are maintained in >50% of convalescents, but the cytokine response in these cells to mutated spike epitopes corresponding to B.1.1.529 and B.1.351 (Beta) VOCs were impaired. These results indicate that increased antigen variability in VOCs impairs humoral and spike-specific T cell immunity post-infection, strongly suggesting that COVID-19 convalescents are vulnerable and at risk of re-infection with VOCs, thus stressing the importance of vaccination programs.

Published
2022

4. Enhanced T Cell Responses Induced by a Necrotic Dendritic Cell Vaccine, Expressing HCV NS3

Author

Mekonnen, Zelalem A, Masavuli, Makutiro G, Yu, Wenbo, Gummow, Jason, Whelan, Dawn M, Al-Delfi, Zahraa, Torresi, Joseph, Gowans, Eric J, and Grubor-Bauk, Branka

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Digestive Diseases, Prevention, Vaccine Related, Immunization, Emerging Infectious Diseases, Hepatitis - C, Hepatitis, Chronic Liver Disease and Cirrhosis, Infectious Diseases, HIV/AIDS, Biotechnology, Liver Disease, Prevention of disease and conditions, and promotion of well-being, 3.4 Vaccines, Inflammatory and immune system, Infection, Good Health and Well Being, necrosis, HCV, cell mediated immunity, cross presentation, vaccine, hepatitis (C) virus, Environmental Science and Management, Soil Sciences, Microbiology, Medical microbiology
Abstract

A vaccine that induces potent, broad and sustained cell-mediated immunity, resulting in effective memory has the potential to restrict hepatitis C (HCV) virus infection. Early, multi-functional CD4+ and CD8+ T cell responses against non-structural protein 3 (NS3) have been associated with HCV clearance. Necrotic cells generate strong immune responses and represent a major antigenic source used by dendritic cells (DC) for processing and presentation, but there is conflicting evidence as to their immunogenicity in vaccination. Immunization with DC loaded with viral antigens has been done in the past, but to date the immunogenicity of live vs. necrotic DC vaccines has not been investigated. We developed a DC2.4 cell line stably expressing HCV NS3, and compared the NS3-specific responses of live vs. necrotic NS3 DC. Vaccination of mice with necrotic NS3 DC increased the breadth of T-cell responses and enhanced the production of IL-2, TNF-α, and IFN-γ by effector memory CD4+ and CD8+T cells, compared to mice vaccinated with live NS3 DC. A single dose of necrotic NS3 DC vaccine induced a greater influx and activation of cross-presenting CD11c+ CD8α+ DC and necrosis-sensing Clec9A+ DC in the draining lymph nodes. Furthermore, using a hydrodynamic challenge model necrotic NS3 DC vaccination resulted in enhanced clearance of NS3-positive hepatocytes from the livers of vaccinated mice. Taken together, the data demonstrate that necrotic DC represent a novel and exciting vaccination strategy capable of inducing broad and multifunctional T cell memory.

Published
2020

5. A systems immunology study comparing innate and adaptive immune responses in adults to COVID-19 mRNA and adenovirus vectored vaccines

Author

Ryan, Feargal J., Norton, Todd S., McCafferty, Conor, Blake, Stephen J., Stevens, Natalie E., James, Jane, Eden, Georgina L., Tee, Yee C., Benson, Saoirse C., Masavuli, Makutiro G., Yeow, Arthur E.L., Abayasingam, Arunasingam, Agapiou, David, Stevens, Hannah, Zecha, Jana, Messina, Nicole L., Curtis, Nigel, Ignjatovic, Vera, Monagle, Paul, Tran, Huyen, McFadyen, James D., Bull, Rowena A., Grubor-Bauk, Branka, Lynn, Miriam A., Botten, Rochelle, Barry, Simone E., and Lynn, David J.

Published
2023
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6. Single-Dose Vaccination with a Hepatotropic Adeno-associated Virus Efficiently Localizes T Cell Immunity in the Liver with the Potential To Confer Rapid Protection against Hepatitis C Virus.

Author

Mekonnen, Zelalem A, Grubor-Bauk, Branka, English, Kieran, Leung, Preston, Masavuli, Makutiro G, Shrestha, Ashish C, Bertolino, Patrick, Bowen, David G, Lloyd, Andrew R, Gowans, Eric J, and Wijesundara, Danushka K

Subjects
DNA vaccine, adeno-associated virus vaccine, cytotoxic T cells, helper T cells, hepatitis C virus vaccine, liver immunity, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology
Abstract

Hepatitis C virus (HCV) is a significant contributor to the global disease burden, and development of an effective vaccine is required to eliminate HCV infections worldwide. CD4+ and CD8+ T cell immunity correlates with viral clearance in primary HCV infection, and intrahepatic CD8+ tissue-resident memory T (TRM) cells provide lifelong and rapid protection against hepatotropic pathogens. Consequently, we aimed to develop a vaccine to elicit HCV-specific CD4+ and CD8+ T cells, including CD8+ TRM cells, in the liver, given that HCV primarily infects hepatocytes. To achieve this, we vaccinated wild-type BALB/c mice with a highly immunogenic cytolytic DNA vaccine encoding a model HCV (genotype 3a) nonstructural protein (NS5B) and a mutant perforin (pVAX-NS5B-PRF), as well as a recombinant adeno-associated virus (AAV) encoding NS5B (rAAV-NS5B). A novel fluorescent target array (FTA) was used to map immunodominant CD4+ T helper (TH) cell and cytotoxic CD8+ T cell epitopes of NS5B in vivo, which were subsequently used to design a KdNS5B451-459 tetramer and analyze NS5B-specific T cell responses in vaccinated mice in vivo The data showed that intradermal prime/boost vaccination with pVAX-NS5B-PRF was effective in eliciting TH and cytotoxic CD8+ T cell responses and intrahepatic CD8+ TRM cells, but a single intravenous dose of hepatotropic rAAV-NS5B was significantly more effective. As a T-cell-based vaccine against HCV should ideally result in localized T cell responses in the liver, this study describes primary observations in the context of HCV vaccination that can be used to achieve this goal.IMPORTANCE There are currently at least 71 million individuals with chronic HCV worldwide and almost two million new infections annually. Although the advent of direct-acting antivirals (DAAs) offers highly effective therapy, considerable remaining challenges argue against reliance on DAAs for HCV elimination, including high drug cost, poorly developed health infrastructure, low screening rates, and significant reinfection rates. Accordingly, development of an effective vaccine is crucial to HCV elimination. An HCV vaccine that elicits T cell immunity in the liver will be highly protective for the following reasons: (i) T cell responses against nonstructural proteins of the virus are associated with clearance of primary infection, and (ii) long-lived liver-resident T cells alone can protect against malaria infection of hepatocytes. Thus, in this study we exploit promising vaccination platforms to highlight strategies that can be used to evoke highly functional and long-lived T cell responses in the liver for protection against HCV.

Published
2019

7. Cytolytic Perforin as an Adjuvant to Enhance the Immunogenicity of DNA Vaccines.

Author

Shrestha, Ashish C, Wijesundara, Danushka K, Masavuli, Makutiro G, Mekonnen, Zelalem A, Gowans, Eric J, and Grubor-Bauk, Branka

Subjects
DNA vaccine, HCV, HIV, adjuvants, bicistronic, cytolytic, perforin, plasmid, vaccine delivery
Abstract

DNA vaccines present one of the most cost-effective platforms to develop global vaccines, which have been tested for nearly three decades in preclinical and clinical settings with some success in the clinic. However, one of the major challenges for the development of DNA vaccines is their poor immunogenicity in humans, which has led to refinements in DNA delivery, dosage in prime/boost regimens and the inclusion of adjuvants to enhance their immunogenicity. In this review, we focus on adjuvants that can enhance the immunogenicity of DNA encoded antigens and highlight the development of a novel cytolytic DNA platform encoding a truncated mouse perforin. The application of this innovative DNA technology has considerable potential in the development of effective vaccines.

Published
2019

8. Toward DNA-Based T-Cell Mediated Vaccines to Target HIV-1 and Hepatitis C Virus: Approaches to Elicit Localized Immunity for Protection.

Author

Mekonnen, Zelalem A, Grubor-Bauk, Branka, Masavuli, Makutiro G, Shrestha, Ashish C, Ranasinghe, Charani, Bull, Rowena A, Lloyd, Andrew R, Gowans, Eric J, and Wijesundara, Danushka K

Subjects
DNA vaccine, HCV, HIV/AIDS, T cell immunity, hepatitis C, human immunodeficiency virus, tissue-resident memory, Drug Discovery, HIV Infections, Hepatitis C, Humans, T-Lymphocytes, Vaccines, DNA, Vaccinology, Viral Vaccines, Vaccines, DNA, Biochemistry and Cell Biology, Microbiology
Abstract

Human immunodeficiency virus (HIV)-1 and hepatitis C virus (HCV) are major contributors to the global disease burden with many experts recognizing the requirement of an effective vaccine to bring a durable end to these viral epidemics. The most promising vaccine candidates that have advanced into pre-clinical models and the clinic to eliminate or provide protection against these chronic viruses are viral vectors [e.g., recombinant cytomegalovirus, Adenovirus, and modified vaccinia Ankara (MVA)]. This raises the question, is there a need to develop DNA vaccines against HIV-1 and HCV? Since the initial study from Wolff and colleagues which showed that DNA represents a vector that can be used to express transgenes durably in vivo, DNA has been regularly evaluated as a vaccine vector albeit with limited success in large animal models and humans. However, several recent studies in Phase I-IIb trials showed that vaccination of patients with recombinant DNA represents a feasible therapeutic intervention to even cure cervical cancer, highlighting the potential of using DNA for human vaccinations. In this review, we will discuss the limitations and the strategies of using DNA as a vector to develop prophylactic T cell-mediated vaccines against HIV-1 and HCV. In particular, we focus on potential strategies exploiting DNA vectors to elicit protective localized CD8+ T cell immunity in the liver for HCV and in the cervicovaginal mucosa for HIV-1 as localized immunity will be an important, if not critical component, of an efficacious vaccine against these viral infections.

Published
2019

9. Immune profiling of COVID-19 vaccine responses in people with multiple sclerosis on B cell-depleting therapy

Author

Perkins, Griffith B., primary, Hope, Christopher M., additional, Chai, Cheng Sheng, additional, Tunbridge, Matthew J., additional, Sterling, Sebastian, additional, Webb, Kevin, additional, Yap, Joey, additional, Yeow, Arthur Eng Lip, additional, Masavuli, Makutiro G., additional, Kireta, Svjetlana, additional, Zuiani, James D., additional, Akerman, Anouschka, additional, Aggarwal, Anupriya, additional, Milogiannakis, Vanessa, additional, Roberts, Matthew B., additional, Wilson, William, additional, Hurtado, Plinio R., additional, Turville, Stuart, additional, Grubor-Bauk, Branka, additional, Barry, Simon C., additional, Coates, P. Toby, additional, Ravindran, Janakan, additional, and Hissaria, Pravin, additional

Published
2023
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10. Myeloperoxidase creates a permissive microenvironmental niche for the progression of multiple myeloma

Author

Williams, Connor M. D., primary, Noll, Jacqueline E., additional, Bradey, Alanah L., additional, Duggan, Jvaughn, additional, Wilczek, Vicki J., additional, Masavuli, Makutiro G., additional, Grubor‐Bauk, Branka, additional, Panagopoulos, Romana A., additional, Hewett, Duncan R., additional, Mrozik, Krzysztof M., additional, Zannettino, Andrew C. W., additional, Vandyke, Kate, additional, and Panagopoulos, Vasilios, additional

Published
2023
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11. A systems immunology study comparing innate and adaptive immune responses in adults to COVID-19 mRNA (BNT162b2/mRNA-1273) and adenovirus vectored vaccines (ChAdOx1-S) after the first, second and third doses

Author

Ryan, Feargal J., primary, Norton, Todd S., additional, McCafferty, Conor, additional, Blake, Stephen J., additional, Stevens, Natalie E., additional, James, Jane, additional, Eden, Georgina L., additional, Tee, Yee C., additional, Benson, Saoirse C., additional, Masavuli, Makutiro G., additional, Yeow, Arthur EL, additional, Abayasingam, Arunasingam, additional, Agapiou, David, additional, Stevens, Hannah, additional, Zecha, Jana, additional, Messina, Nicole L., additional, Curtis, Nigel, additional, Ignjatovic, Vera, additional, Monagle, Paul, additional, Tran, Huyen, additional, McFadyen, James D., additional, Bull, Rowena A., additional, Grubor-Bauk, Branka, additional, Lynn, Miriam A., additional, Botten, Rochelle, additional, Barry, Simone E., additional, and Lynn, David J., additional

Published
2022
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12. Concurrent vaccination of kidney transplant recipients and close household cohabitants against COVID-19

Author

Perkins, Griffith B., Tunbridge, Matthew, Salehi, Tania, Chai, Cheng Sheng, Kireta, Svjetlana, Johnston, Julie, Penko, Daniella, Nitschke, Jodie, Yeow, Arthur Eng Lip, Al-Delfi, Zahraa, Drogemuller, Christopher J., Garcia-Valtanen, Pablo, Masavuli, Makutiro G., Hope, Christopher M., Singer, Julian, Aggarwal, Anupriya, Ospina Stella, Alberto, Turville, Stuart G., Hurtado, Plinio R., Barry, Simon C., Hissaria, Pravin, Grubor-Bauk, Branka, Chadban, Steven J., and Coates, P. Toby

Published
2022
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13. Additional file 10 of Long-term perturbation of the peripheral immune system months after SARS-CoV-2 infection

Author

Ryan, Feargal J., Hope, Christopher M., Masavuli, Makutiro G., Lynn, Miriam A., Mekonnen, Zelalem A., Yeow, Arthur Eng Lip, Garcia-Valtanen, Pablo, Al-Delfi, Zahraa, Gummow, Jason, Ferguson, Catherine, O���Connor, Stephanie, Reddi, Benjamin A. J., Hissaria, Pravin, Shaw, David, Kok-Lim, Chuan, Gleadle, Jonathan M., Beard, Michael R., Barry, Simon C., Grubor-Bauk, Branka, and Lynn, David J.

Abstract

Additional file 10. Symptom questionnaire sent to patients to assess presence of long COVID associated symptoms.

Published
2022
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14. Additional file 3 of Long-term perturbation of the peripheral immune system months after SARS-CoV-2 infection

Author

Ryan, Feargal J., Hope, Christopher M., Masavuli, Makutiro G., Lynn, Miriam A., Mekonnen, Zelalem A., Yeow, Arthur Eng Lip, Garcia-Valtanen, Pablo, Al-Delfi, Zahraa, Gummow, Jason, Ferguson, Catherine, O���Connor, Stephanie, Reddi, Benjamin A. J., Hissaria, Pravin, Shaw, David, Kok-Lim, Chuan, Gleadle, Jonathan M., Beard, Michael R., Barry, Simon C., Grubor-Bauk, Branka, and Lynn, David J.

Abstract

Additional file 3: Figure S3: Adjusting for differences in immune cell populations. We repeated the differential expression analysis multiple times, each time adjusting for differences in the frequency of major immune cell populations among individuals. Each panel shows the enrichment of selected pathways (same as those shown in Fig. 4F) among genes identified as being significantly up-regulated in each analysis (FDR 1.25-fold). None = no immune cell population adjustment.

Published
2022
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15. Additional file 2 of Long-term perturbation of the peripheral immune system months after SARS-CoV-2 infection

Author

Ryan, Feargal J., Hope, Christopher M., Masavuli, Makutiro G., Lynn, Miriam A., Mekonnen, Zelalem A., Yeow, Arthur Eng Lip, Garcia-Valtanen, Pablo, Al-Delfi, Zahraa, Gummow, Jason, Ferguson, Catherine, O���Connor, Stephanie, Reddi, Benjamin A. J., Hissaria, Pravin, Shaw, David, Kok-Lim, Chuan, Gleadle, Jonathan M., Beard, Michael R., Barry, Simon C., Grubor-Bauk, Branka, and Lynn, David J.

Abstract

Additional file 2: Figure S2: Expression of genes in two pathways identified as downregulated in COVID-19 convalescents and healthy controls. (A) Reactome pathway R-HSA-76002 ���Platelet activation, signaling and aggregation��� and (B) KEGG pathway hsa00190 ���Oxidative phosphorylation���. Oxidative phosphorylation genes are sub-divided into nuclear and mitochondrially encoded, with the same x axis order of samples in each panel. Only differentially expressed genes (FDR 1.25-fold) within each pathway are shown. (C) Serum CRP levels in samples collected from healthy controls (HC) and COVID-19 convalescent individuals at 12, 16 and 24 weeks post infection.

Published
2022
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16. Long-term perturbation of the peripheral immune system months after SARS-CoV-2 infection

Author

Ryan, Feargal J., primary, Hope, Christopher M., additional, Masavuli, Makutiro G., additional, Lynn, Miriam A., additional, Mekonnen, Zelalem A., additional, Lip Yeow, Arthur Eng, additional, Garcia-Valtanen, Pablo, additional, Al-Delfi, Zahraa, additional, Gummow, Jason, additional, Ferguson, Catherine, additional, O’Connor, Stephanie, additional, Reddi, Benjamin AJ, additional, Shaw, David, additional, Kok-Lim, Chuan, additional, Gleadle, Jonathan M., additional, Beard, Michael R., additional, Barry, Simon C., additional, Grubor-Bauk, Branka, additional, and Lynn, David J., additional

Published
2021
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17. 'One Year Later' - SARS-CoV-2-Specific Immunity in Mild Cases of COVID-19

Author

Garcia Valtanen, Pablo, primary, Hope, Christopher M., additional, Masavuli, Makutiro G, additional, Yeow, Arthur Eng Lip, additional, Balachandran, Harikrishnan, additional, Mekonnen, Zelalem A., additional, Al-Delfi, Zahraa, additional, Abayasingam, Arunasingam, additional, Agapiou, David, additional, Gummow, Jason, additional, Ferguson, Catherine, additional, O’Connor, Stephanie, additional, McCartney, Erin M., additional, Lynn, David J, additional, Maddern, Guy, additional, Gowans, Eric J, additional, Reddi, Benjamin AJ, additional, Shaw, David, additional, Chuan, Kok-Lim, additional, Beard, Michael, additional, Weiskopf, Daniela, additional, Sette, Alessandro, additional, Bull, Rowena Anne, additional, Barry, Simon C., additional, and Grubor-Bauk, Branka, additional

Published
2021
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20. Safety Profile of a Multi-Antigenic DNA Vaccine Against Hepatitis C Virus

Author

Zelalem A Mekonnen, Branka Grubor-Bauk, Ilia Voskoboinik, Ashish C. Shrestha, Makutiro Ghislain Masavuli, Eric J. Gowans, Jason Gummow, Danushka K. Wijesundara, Yanrui Li, Gummow, Jason, Masavuli, Makutiro G, Mekonnen, Zelalem A, Li, Yanrui, Wijesundara, Danushka K, Shrestha, Ashish C, Voskoboinik, Ilia, Gowans, Eric J, and Grubor-Bauk, Branka

Subjects
hepatitis C virus, 0301 basic medicine, DNA vaccine, immune breadth, Hepatitis C Virus, pre-clinical, Hepatitis C virus, Immunology, lcsh:Medicine, medicine.disease_cause, Article, DNA vaccination, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immunity, Drug Discovery, medicine, Pharmacology (medical), NS5B, perforin, Pharmacology, Reactogenicity, biology, business.industry, ELISPOT, lcsh:R, Hepatitis C, medicine.disease, Virology, digestive system diseases, 030104 developmental biology, Infectious Diseases, cell death, chemistry, Perforin, Pre-clinical, biology.protein, 030211 gastroenterology & hepatology, pathology, business, toxicology
Abstract

Despite direct acting antivirals (DAAs) curing &gt, 95% of individuals infected with hepatitis C (HCV), in order to achieve the World Health Organization HCV Global Elimination Goals by 2030 there are still major challenges that need to be overcome. DAAs alone are unlikely to eliminate HCV in the absence of a vaccine that can limit viral transmission. Consequently, a prophylactic HCV vaccine is necessary to relieve the worldwide burden of HCV disease. DNA vaccines are a promising vaccine platform due to their commercial viability and ability to elicit robust T-cell-mediated immunity (CMI). We have developed a novel cytolytic DNA vaccine that encodes non-structural HCV proteins and a truncated mouse perforin (PRF), which is more immunogenic than the respective canonical DNA vaccine lacking PRF. Initially we assessed the ability of the HCV pNS3-PRF and pNS4/5-PRF DNA vaccines to elicit robust long-term CMI without any adverse side-effects in mice. Interferon-&gamma, (IFN-&gamma, ) enzyme-linked immunosorbent spot (ELISpot) assay was used to evaluate CMI against NS3, NS4 and NS5B in a dose-dependent manner. This analysis showed a dose-dependent bell-curve of HCV-specific responses in vaccinated animals. We then thoroughly examined the effects associated with reactogenicity of cytolytic DNA vaccination with the multi-antigenic HCV DNA vaccine (pNS3/4/5B). Hematological, biochemical and histological studies were performed in male Sprague Dawley rats with a relative vaccine dose 10&ndash, 20-fold higher than the proposed dose in Phase I clinical studies. The vaccine was well tolerated, and no toxicity was observed. Thus, the cytolytic multi-antigenic DNA vaccine is safe and elicits broad memory CMI.

Published
2020
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21. Enhanced T Cell Responses Induced by a Necrotic Dendritic Cell Vaccine, Expressing HCV NS3

Author

Zelalem A. Mekonnen, Makutiro G. Masavuli, Wenbo Yu, Jason Gummow, Dawn M. Whelan, Zahraa Al-Delfi, Joseph Torresi, Eric J. Gowans, Branka Grubor-Bauk, Mekonnen, Zelalem A, Masavuli, Makutiro G, Yu, Wenbo, Gummow, Jason, Whelan, Dawn M, Al-Delfi, Zahraa, Torresi, Joseph, Gowans, Eric J, and Grubor-Bauk, Branka

Subjects
and promotion of well-being, viruses, lcsh:QR1-502, lcsh:Microbiology, necrosis, Hepatitis, 0302 clinical medicine, vaccine, Original Research, 0303 health sciences, Immunogenicity, Liver Disease, Cross-presentation, virus diseases, Vaccination, medicine.anatomical_structure, Infectious Diseases, 3.4 Vaccines, 030220 oncology & carcinogenesis, HCV, HIV/AIDS, Infection, Biotechnology, Microbiology (medical), Environmental Science and Management, T cell, Chronic Liver Disease and Cirrhosis, Biology, hepatitis (C) virus, Microbiology, DNA vaccination, Vaccine Related, 03 medical and health sciences, Immune system, Antigen, cell mediated immunity, Hepatitis - C, medicine, 030304 developmental biology, cross presentation, Prevention, Inflammatory and immune system, biochemical phenomena, metabolism, and nutrition, Prevention of disease and conditions, Virology, digestive system diseases, Emerging Infectious Diseases, Good Health and Well Being, Soil Sciences, Immunization, Digestive Diseases, CD8
Abstract

A vaccine that induces potent, broad and sustained cell-mediated immunity, resulting in effective memory has the potential to restrict hepatitis C (HCV) virus infection. Early, multi-functional CD4+ and CD8+ T cell responses against non-structural protein 3 (NS3) have been associated with HCV clearance. Necrotic cells generate strong immune responses and represent a major antigenic source used by dendritic cells (DC) for processing and presentation, but there is conflicting evidence as to their immunogenicity in vaccination. Immunization with DC loaded with viral antigens has been done in the past, but to date the immunogenicity of live vs. necrotic DC vaccines has not been investigated. We developed a DC2.4 cell line stably expressing HCV NS3, and compared the NS3-specific responses of live vs. necrotic NS3 DC. Vaccination of mice with necrotic NS3 DC increased the breadth of T-cell responses and enhanced the production of IL-2, TNF-α, and IFN-γ by effector memory CD4+ and CD8+T cells, compared to mice vaccinated with live NS3 DC. A single dose of necrotic NS3 DC vaccine induced a greater influx and activation of cross-presenting CD11c+ CD8α+ DC and necrosis-sensing Clec9A+ DC in the draining lymph nodes. Furthermore, using a hydrodynamic challenge model necrotic NS3 DC vaccination resulted in enhanced clearance of NS3-positive hepatocytes from the livers of vaccinated mice. Taken together, the data demonstrate that necrotic DC represent a novel and exciting vaccination strategy capable of inducing broad and multifunctional T cell memory.

Published
2020

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