Your search keyword '"Demetrius Matassov"' showing total 19 results

1. Preclinical Safety Assessment of the EBS-LASV Vaccine Candidate against Lassa Fever Virus

Author

Demetrius Matassov, Lisa Evans DeWald, Stefan Hamm, Rebecca M. Nowak, Cheryl S. Gerardi, Theresa E. Latham, Rong Xu, Amara Luckay, Tracy Chen, Marc Tremblay, Jeffry Shearer, Melissa Wynn, John H. Eldridge, Kelly Warfield, and Kevin Spurgers

Subjects

Lassa virus, LASV, glycoprotein, vesicular stomatitis virus, VSV, attenuated vaccine, Medicine

Abstract

There are currently no prophylactic vaccines licensed to protect against Lassa fever caused by Lassa virus (LASV) infection. The Emergent BioSolutions (EBS) vaccine candidate, EBS-LASV, is being developed for the prevention of Lassa fever. EBS-LASV is a live-attenuated recombinant Vesicular Stomatitis Virus (rVSV)-vectored vaccine encoding the surface glycoprotein complex (GPC) from LASV and has two attenuating vector modifications: a gene shuffle of the VSV N gene and a deletion of the VSV G gene. Preclinical studies were performed to evaluate EBS-LASV’s neurovirulence potential following intracranial (IC) injection and to determine the biodistribution and vector replication following intramuscular (IM) inoculation in mice. In addition, the potential EBS-LASV toxicity was assessed using repeated-dose IM EBS-LASV administration to rabbits. All mice receiving the IC injection of EBS-LASV survived, while mice administered the unattenuated control vector did not. The vaccine was only detected in the muscle at the injection site, draining lymph nodes, and the spleen over the first week following IM EBS-LASV injection in mice, with no detectable plasma viremia. No toxicity was observed in rabbits receiving a three-dose regimen of EBS-LASV. These studies demonstrate that EBS-LASV is safe when administered to animals and supported a first-in-human dose-escalation, safety, and immunogenicity clinical study.

Published

2024

2. An introduction to the Marburg virus vaccine consortium, MARVAC

Author

Robert W. Cross, Ira M. Longini, Stephan Becker, Karin Bok, David Boucher, Miles W. Carroll, Janet V. Díaz, William E. Dowling, Ruxandra Draghia-Akli, James T. Duworko, John M. Dye, Michael A. Egan, Patricia Fast, Amy Finan, Courtney Finch, Thomas R. Fleming, Joan Fusco, Thomas W. Geisbert, Anthony Griffiths, Stephan Günther, Lisa E. Hensley, Anna Honko, Ruth Hunegnaw, Jocelyn Jakubik, Julie Ledgerwood, Kerstin Luhn, Demetrius Matassov, Jeffrey Meshulam, Emily V. Nelson, Christopher L. Parks, Roxana Rustomjee, David Safronetz, Lauren M. Schwartz, Dean Smith, Paul Smock, Ydrissa Sow, Christina F. Spiropoulou, Nancy J. Sullivan, Kelly L. Warfield, Daniel Wolfe, Courtney Woolsey, Roland Zahn, Ana María Henao-Restrepo, César Muñoz-Fontela, and Andrea Marzi

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

The emergence of Marburg virus (MARV) in Guinea and Ghana triggered the assembly of the MARV vaccine “MARVAC” consortium representing leaders in the field of vaccine research and development aiming to facilitate a rapid response to this infectious disease threat. Here, we discuss current progress, challenges, and future directions for MARV vaccines.

Published

2022

3. A highly attenuated Vesiculovax vaccine rapidly protects nonhuman primates against lethal Marburg virus challenge.

Author

Courtney Woolsey, Robert W Cross, Krystle N Agans, Viktoriya Borisevich, Daniel J Deer, Joan B Geisbert, Cheryl Gerardi, Theresa E Latham, Karla A Fenton, Michael A Egan, John H Eldridge, Thomas W Geisbert, and Demetrius Matassov

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

BackgroundMarburg virus (MARV), an Ebola-like virus, remains an eminent threat to public health as demonstrated by its high associated mortality rate (23-90%) and recent emergence in West Africa for the first time. Although a recombinant vesicular stomatitis virus (rVSV)-based vaccine (Ervebo) is licensed for Ebola virus disease (EVD), no approved countermeasures exist against MARV. Results from clinical trials indicate Ervebo prevents EVD in 97.5-100% of vaccinees 10 days onwards post-immunization.Methodology/findingsGiven the rapid immunogenicity of the Ervebo platform against EVD, we tested whether a similar, but highly attenuated, rVSV-based Vesiculovax vector expressing the glycoprotein (GP) of MARV (rVSV-N4CT1-MARV-GP) could provide swift protection against Marburg virus disease (MVD). Here, groups of cynomolgus monkeys were vaccinated 7, 5, or 3 days before exposure to a lethal dose of MARV (Angola variant). All subjects (100%) immunized one week prior to challenge survived; 80% and 20% of subjects survived when vaccinated 5- and 3-days pre-exposure, respectively. Lethality was associated with higher viral load and sustained innate immunity transcriptional signatures, whereas survival correlated with development of MARV GP-specific antibodies and early expression of predicted NK cell-, B-cell-, and cytotoxic T-cell-type quantities.Conclusions/significanceThese results emphasize the utility of Vesiculovax vaccines for MVD outbreak management. The highly attenuated nature of rVSV-N4CT1 vaccines, which are clinically safe in humans, may be preferable to vaccines based on the same platform as Ervebo (rVSV "delta G" platform), which in some trial participants induced vaccine-related adverse events in association with viral replication including arthralgia/arthritis, dermatitis, and cutaneous vasculitis.

Published

2022

4. A highly attenuated pan-filovirus VesiculoVax vaccine rapidly protects nonhuman primates against Marburg virus and three species of Ebolavirus

Author

Courtney Woolsey, Viktoriya Borisevich, Krystle N Agans, Rachel O’Toole, Karla A Fenton, Mack B Harrison, Abhishek N Prasad, Daniel J Deer, Cheryl Gerardi, Nneka Morrison, Robert W Cross, John H Eldridge, Demetrius Matassov, and Thomas W Geisbert

Subjects

Infectious Diseases, Immunology and Allergy

Abstract

Background The family Filoviridae consists of several virus members known to cause significant mortality and disease in humans. Among these, Ebola virus (EBOV), Marburg virus (MARV), Sudan virus (SUDV), and Bundibugyo virus (BDBV) are considered the deadliest. The sole US FDA approved filovirus vaccine, Ervebo®, is indicated only for EBOV infections with limited heterologous protection against other filoviruses. In clinical trials, Ervebo® was shown to rapidly protect humans against Ebola disease ten days plus post immunization. Whether multivalent formulations of similar recombinant vesicular stomatitis virus (rVSV)-based vaccines could likewise confer rapid protection is unclear. Methodology/Findings Here, we tested the ability of a highly attenuated, quadrivalent pan-filovirus Vesiculovax vaccine (rVSV-Filo) to elicit fast-acting protection against MARV, EBOV, SUDV, and BDBV. Groups of cynomolgus monkeys were vaccinated seven days before exposure to each of the four viral pathogens. All subjects (100%) immunized one-week prior survived MARV, SUDV, and BDBV challenge; 80% of subjects survived EBOV challenge. Survival correlated with lower viral load, higher glycoprotein-specific IgG titers, and the expression of B cell-, cytotoxic cell-, and antigen presentation-associated transcripts. Conclusions/Significance These results demonstrate multivalent Vesiculovax vaccines are suitable for filovirus outbreak management. The highly attenuated nature of the rVSV-Filo vaccine may be preferable to the Ervebo® “delta G” platform, which induced arthralgia, cutaneous vasculitis, and dermatitis in a subset of recipients.

Published

2023

5. Quadrivalent VesiculoVax vaccine protects nonhuman primates from viral-induced hemorrhagic fever and death

Author

Robert W. Cross, Rong Xu, Susan E. Witko, Ayuko Ota-Setlik, Lena Soukieh, Thomas W. Geisbert, Amara Luckay, Karla A. Fenton, Daniel J. Deer, Krystle N. Agans, John H. Eldridge, Theresa E. Latham, Chad E. Mire, Demetrius Matassov, Heinz Feldmann, Rebecca M. Nowak, Joan B. Geisbert, Christian T. Happi, Cheryl S. Gerardi, and Stefan Hamm

Subjects

0301 basic medicine, Genetic Vectors, Biology, Antibodies, Viral, medicine.disease_cause, Virus, 03 medical and health sciences, Lassa Fever, 0302 clinical medicine, Immune system, medicine, Animals, Humans, Vector (molecular biology), Lassa virus, Neutralizing antibody, Arenavirus, Viral Vaccines, Vesiculovirus, General Medicine, biology.organism_classification, Virology, Vaccination, Macaca fascicularis, 030104 developmental biology, Vesicular stomatitis virus, Immunoglobulin G, 030220 oncology & carcinogenesis, biology.protein, Research Article

Abstract

Recent occurrences of filoviruses and the arenavirus Lassa virus (LASV) in overlapping endemic areas of Africa highlight the need for a prophylactic vaccine that would confer protection against all of these viruses that cause lethal hemorrhagic fever (HF). We developed a quadrivalent formulation of VesiculoVax that contains recombinant vesicular stomatitis virus (rVSV) vectors expressing filovirus glycoproteins and that also contains a rVSV vector expressing the glycoprotein of a lineage IV strain of LASV. Cynomolgus macaques were vaccinated twice with the quadrivalent formulation, followed by challenge 28 days after the boost vaccination with each of the 3 corresponding filoviruses (Ebola, Sudan, Marburg) or a heterologous contemporary lineage II strain of LASV. Serum IgG and neutralizing antibody responses specific for all 4 glycoproteins were detected in all vaccinated animals. A modest and balanced cell-mediated immune response specific for the glycoproteins was also detected in most of the vaccinated macaques. Regardless of the level of total glycoprotein-specific immune response detected after vaccination, all immunized animals were protected from disease and death following lethal challenges. These findings indicate that vaccination with attenuated rVSV vectors each expressing a single HF virus glycoprotein may provide protection against those filoviruses and LASV most commonly responsible for outbreaks of severe HF in Africa.

Published

2019

6. A Brighton Collaboration standardized template with key considerations for a benefit/risk assessment for a soluble glycoprotein vaccine to prevent disease caused by Nipah or Hendra viruses

Author

Marc Gurwith, Antony S. Dimitrov, Susan Sciotto-Brown, Stefan Hamm, Robert T. Chen, Emily R. Smith, Rong Xu, Luz Hermida, Tracy Chen, Marc Tremblay, Michael A. Egan, John H. Eldridge, and Demetrius Matassov

Subjects

Disease, Risk Assessment, Hendra Virus, CEPI, Medicine, Humans, Nipah, Public acceptance, Glycoproteins, chemistry.chemical_classification, Henipavirus Infections, Vaccines, Synthetic, General Veterinary, General Immunology and Microbiology, business.industry, Protein, Public Health, Environmental and Occupational Health, virus diseases, A protein, Brighton Collaboration, Virology, Benefit/Risk, Infectious Diseases, chemistry, Molecular Medicine, Benefit risk assessment, Safety, Glycoprotein, ALUMINUM PHOSPHATE, business, Hendra, Clinical evaluation, Vaccine

Abstract

Auro Vaccines LLC has developed a protein vaccine to prevent disease from Nipah and Hendra virus infection that employs a recombinant soluble Hendra glycoprotein (HeV-sG) adjuvanted with aluminum phosphate. This vaccine is currently under clinical evaluation in a Phase 1 study. The Benefit-Risk Assessment of VAccines by TechnolOgy Working Group (BRAVATO; ex-V3SWG) has prepared a standardized template to describe the key considerations for the benefit-risk assessment of protein vaccines. This will help key stakeholders to assess potential safety issues and understand the benefit-risk of such a vaccine platform. The structured and standardized assessment provided by the template may also helpcontribute to improved public acceptance and communication of licensed protein vaccines.

Published

2021

7. Immune correlates of postexposure vaccine protection against Marburg virus

Author

Karla A. Fenton, Ilhem Messaoudi, Robert W. Cross, Daniel J. Deer, Courtney Woolsey, Cheryl S. Gerardi, Joan B. Geisbert, Viktoriya Borisevich, Thomas W. Geisbert, John H. Eldridge, Demetrius Matassov, Krystle N. Agans, Allen Jankeel, Theresa E. Latham, and Chad E. Mire

Subjects

Cytotoxicity, Immunologic, Male, LAG3, Live attenuated vaccines, lcsh:Medicine, Antibodies, Viral, 0302 clinical medicine, Marburg Virus Disease, lcsh:Science, Marburg virus, Recombination, Genetic, 0303 health sciences, Multidisciplinary, biology, T-Lymphocytes, Helper-Inducer, Viral Load, 3. Good health, Up-Regulation, Killer Cells, Natural, Vesicular stomatitis virus, Cytokines, Female, Antibody, Post-Exposure Prophylaxis, Viral load, Dose-Response Relationship, Immunologic, Down-Regulation, Article, 03 medical and health sciences, Immune system, Th2 Cells, Immunity, medicine, Animals, RNA, Messenger, 030304 developmental biology, Ebola virus and Marburg virus, Inflammation, lcsh:R, Viral Vaccines, Vesiculovirus, Th1 Cells, medicine.disease, biology.organism_classification, Virology, Macaca mulatta, Immune checkpoint, Marburgvirus, biology.protein, lcsh:Q, Interferons, Transcriptome, 030215 immunology

Abstract

Postexposure immunization can prevent disease and reduce transmission following pathogen exposure. The rapid immunostimulatory properties of recombinant vesicular stomatitis virus (rVSV)-based vaccines make them suitable postexposure treatments against the filoviruses Ebola virus and Marburg virus (MARV); however, the mechanisms that drive this protection are undefined. Previously, we reported 60–75% survival of rhesus macaques treated with rVSV vectors expressing MARV glycoprotein (GP) 20–30 minutes after a low dose exposure to the most pathogenic variant of MARV, Angola. Survival in this model was linked to production of GP-specific antibodies and lower viral load. To confirm these results and potentially identify novel correlates of postexposure protection, we performed a similar experiment, but analyzed plasma cytokine levels, frequencies of immune cell subsets, and the transcriptional response to infection in peripheral blood. In surviving macaques (80–89%), we observed induction of genes mapping to antiviral and interferon-related pathways early after treatment and a higher percentage of T helper 1 (Th1) and NK cells. In contrast, the response of non-surviving macaques was characterized by hypercytokinemia; a T helper 2 signature; recruitment of low HLA-DR expressing monocytes and regulatory T-cells; and transcription of immune checkpoint (e.g., PD-1, LAG3) genes. These results suggest dysregulated immunoregulation is associated with poor prognosis, whereas early innate signaling and Th1-skewed immunity are important for survival.

Published

2019

8. Safety and immunogenicity of a highly attenuated rVSVN4CT1-EBOVGP1 Ebola virus vaccine: a randomised, double-blind, placebo-controlled, phase 1 clinical trial

Author

David K. Clarke, Theresa E. Latham, Michael A. Egan, Amara Luckay, Lucy A. Ward, Ayuko Ota-Setlik, Terry J. Higgins, Tracy Chen, Rong Xu, Janice M. Rusnak, Marc Tremblay, Susan E. Witko, Demetrius Matassov, Susan Sciotto-Brown, Luz Hermida, Cheryl S. Gerardi, and John H. Eldridge

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Placebo, medicine.disease_cause, Vaccines, Attenuated, 03 medical and health sciences, 0302 clinical medicine, Immunogenicity, Vaccine, Double-Blind Method, Internal medicine, Medicine, Humans, 030212 general & internal medicine, Ebola Vaccines, Adverse effect, Glycoproteins, Ebola virus, business.industry, Immunogenicity, Vaccination, Hemorrhagic Fever, Ebola, Middle Aged, Ebolavirus, Healthy Volunteers, Regimen, 030104 developmental biology, Infectious Diseases, Tolerability, Female, Safety, business, Intramuscular injection

Abstract

Summary Background The safety and immunogenicity of a highly attenuated recombinant vesicular stomatitis virus (rVSV) expressing HIV-1 gag (rVSVN4CT1-HIV-1gag1) was shown in previous phase 1 clinical studies. An rVSV vector expressing Ebola virus glycoprotein (EBOV-GP) in place of HIV-1 gag (rVSVN4CT1-EBOVGP1) showed single-dose protection from lethal challenge with low passage Ebola virus in non-human primates. We aimed to evaluate the safety and immunogenicity of the rVSVN4CT1-EBOVGP1 vaccine in healthy adults. Methods We did a randomised double-blind, placebo-controlled, phase 1 dose-escalation study at a single clinical site (Optimal Research) in Melbourne, FL, USA. Eligible participants were healthy men and non-pregnant women aged 18–60 years, with a body-mass index (BMI) of less than 40 kg/m2, no history of filovirus infection, VSV infection, or receipt of rVSV in previous studies, and who had not visited regions where Ebola virus outbreaks have occurred. Three cohorts were enrolled to assess a low (2·5 × 104 plaque forming units [PFU]), intermediate (2 × 105 PFU), or high dose (1·8 × 106 PFU) of the vaccine. Participants within each cohort were randomly allocated (10:3) to receive vaccine or placebo by intramuscular injection in a homologous prime and boost regimen, with 4 weeks between doses. All syringes were masked with syringe sleeves; participants and study site staff were not blinded to dose level but were blinded to active vaccine and placebo. The primary outcomes were safety and tolerability; immunogenicity, assessed as GP-specific humoral immune response (at 2 weeks after each dose) and cellular immune response (at 1 and 2 weeks after each dose), was a secondary outcome. All randomised participants were included in primary and safety analyses. This trial is registered with ClinicalTrials.gov , NCT02718469 . Findings Between Dec 22, 2015, and Sept 15, 2016, 39 individuals (18 [46%] men and 21 [54%] women, mean age 51 years [SD 10]) were enrolled, with ten participants receiving the vaccine and three participants receiving placebo in each of three cohorts. One participant in the intermediate dose cohort was withdrawn from the study because of a diagnosis of invasive ductal breast carcinoma 24 days after the first vaccination, which was considered unrelated to the vaccine. No severe adverse events were observed. Solicited local adverse events occurred in ten (26%) of 39 participants after the first dose and nine (24%) of 38 participants after the second dose; the events lasted 3 days or less, were predominantly injection site tenderness (17 events) and injection site pain (ten events), and were either mild (19 events) or moderate (ten events) in intensity. Systemic adverse events occurred in 13 (33%) of 39 participants after the first dose and eight (21%) of 38 participants after the second dose; the events were mild (45 events) or moderate (11 events) in severity, and the most common events were malaise or fatigue (13 events) and headache (12 events). Arthritis and maculopapular, vesicular, or purpuric rash distal to the vaccination site(s) were not reported. A GP-specific IgG response was detected in all vaccine recipients after two doses (and IgG response frequency was 100% after a single high dose), and an Ebola virus neutralising response was detected in 100% of participants in the high-dose cohort. Interpretation The rVSVN4CT1-EBOVGP1 vaccine was well tolerated at all dose levels tested and was immunogenic despite a high degree of attenuation. The combined safety and immunogenicity profile of the rVSVN4CT1-EBOVGP1 vaccine vector support phase 1–2 clinical evaluation. Funding US Department of Defense Joint Program Executive Office for Chemical, Biological, Radiological and Nuclear Defense: Joint Project Manager for Chemical, Biological, Radiological and Nuclear Medical.

Published

2019

9. Postexposure Efficacy of Recombinant Vesicular Stomatitis Virus Vectors Against High and Low Doses of Marburg Virus Variant Angola in Nonhuman Primates

Author

Thomas W. Geisbert, Krystle N. Agans, Chad E. Mire, Viktoriya Borisevich, Courtney Woolsey, Robert W. Cross, Demetrius Matassov, John H. Eldridge, Karla A. Fenton, Daniel J. Deer, and Joan B. Geisbert

Subjects

0301 basic medicine, Male, filovirus, Genetic Vectors, Supplement Articles, Vesicular stomatitis Indiana virus, Biology, law.invention, Marburg virus, 03 medical and health sciences, law, vaccine, Immunology and Allergy, Animals, Marburg Virus Disease, recombinant vesicular stomatitis virus, chemistry.chemical_classification, Vaccines, Synthetic, Musoke, Low dose, Viral Vaccines, biology.organism_classification, Virology, Macaca mulatta, 3. Good health, Treatment, 030104 developmental biology, Infectious Diseases, chemistry, Marburgvirus, Angola, Vesicular stomatitis virus, Recombinant DNA, Female, Vesiculovirus, Glycoprotein, Ravn virus

Abstract

A recombinant vesicular stomatitis virus (rVSV) expressing the Marburg virus (MARV) Musoke variant glycoprotein fully protects macaques against 2 MARV variants and Ravn virus as a preventive vaccine and MARV variant Musoke as a postexposure treatment. To evaluate postexposure efficacy against the most pathogenic MARV variant, Angola, we engineered rVSVs expressing homologous Angola glycoprotein. Macaques were challenged with high or low doses of variant Angola and treated 20–30 minutes after exposure. A total of 25% and 60%–75% of treated macaques survived the high-dose and low-dose challenges, respectively. The more rapid disease progression of variant Angola versus variant Musoke may account for the incomplete protection observed.

Published

2018

10. Single-dose attenuated Vesiculovax vaccines protect primates against Ebola Makona virus

Author

Rong Xu, Karla A. Fenton, Ayuko Ota-Setlik, Krystle N. Agans, John H. Eldridge, Chad E. Mire, Demetrius Matassov, Theresa E. Latham, David K. Clarke, Michael A. Egan, Thomas W. Geisbert, and Joan B. Geisbert

Subjects

Male, Zaire ebolavirus, Genetic Vectors, Filoviridae, Antibodies, Viral, Vaccines, Attenuated, medicine.disease_cause, Article, medicine, Animals, Humans, Ebola Vaccines, Ebolavirus, Multidisciplinary, Ebola virus, Attenuated vaccine, Ebola vaccine, biology, Vaccination, Vesiculovirus, Hemorrhagic Fever, Ebola, biology.organism_classification, Survival Analysis, Virology, Africa, Western, Kinetics, Macaca fascicularis, Vesicular stomatitis virus, Immunoglobulin G, Immunology, Democratic Republic of the Congo, Female

Abstract

The family Filoviridae contains three genera, Ebolavirus (EBOV), Marburg virus, and Cuevavirus1. Some members of the EBOV genus, including Zaire ebolavirus (ZEBOV), can cause lethal hemorrhagic fever in humans. During 2014 an unprecedented ZEBOV outbreak occurred in West Africa and is still ongoing, resulting in nearly 10,000 deaths, and causing global concern of uncontrolled disease. To meet this challenge a rapid acting vaccine is needed. Many vaccine approaches have shown promise in being able to protect nonhuman primate (NHPs) against ZEBOV2. In response to the current ZEBOV outbreak several of these vaccines have been fast tracked for human use. However, it is not known whether any of these vaccines can provide protection against the new outbreak Makona strain of ZEBOV. One of these approaches is a first generation recombinant vesicular stomatitis virus (rVSV)-based vaccine expressing the ZEBOV glycoprotein (GP) (rVSV/ZEBOV). To address safety concerns associated with this vector, we developed two candidate, further attenuated rVSV/ZEBOV vaccines. Both attenuated vaccines produced an approximately ten-fold lower vaccine-associated viremia compared to the first generation vaccine and both provided complete, single dose protection of macaques from lethal challenge with the Makona outbreak strain of ZEBOV.

Published

2015

11. Single-Dose Trivalent VesiculoVax Vaccine Protects Macaques from Lethal Ebolavirus and Marburgvirus Challenge

Author

Krystle N. Agans, Michael A. Egan, Theresa E. Latham, Ayuko Ota-Setlik, Amanda Burnaugh, Thomas L. Rudge, Chad E. Mire, Carol L. K. Sabourin, Morgan Q. S. Wendling, Rong Xu, David K. Clarke, Joan B. Geisbert, John H. Eldridge, Dean J. Kobs, Thomas W. Geisbert, and Demetrius Matassov

Subjects

0301 basic medicine, Zaire ebolavirus, Immunology, Sudan ebolavirus, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Microbiology, Injections, Intramuscular, 03 medical and health sciences, Mice, Viral Proteins, Virology, Vaccines and Antiviral Agents, medicine, Animals, Marburg Virus Disease, Glycoproteins, Ebolavirus, Vaccines, Synthetic, Ebola virus, biology, Vaccination, Viral Vaccines, Vesiculovirus, Hemorrhagic Fever, Ebola, Marburgvirus, biology.organism_classification, Macaca fascicularis, 030104 developmental biology, Marburg marburgvirus, Vesicular stomatitis virus, architecture, Insect Science, Immunoglobulin G, architecture.house

Abstract

Previous studies demonstrated that a single intramuscular (i.m.) dose of an attenuated recombinant vesicular stomatitis virus (rVSV) vector (VesiculoVax vector platform; rVSV-N4CT1) expressing the glycoprotein (GP) from the Mayinga strain of Zaire ebolavirus (EBOV) protected nonhuman primates (NHPs) from lethal challenge with EBOV strains Kikwit and Makona. Here, we studied the immunogenicities of an expanded range of attenuated rVSV vectors expressing filovirus GP in mice. Based on data from those studies, an optimal attenuated trivalent rVSV vector formulation was identified that included rVSV vectors expressing EBOV, Sudan ebolavirus (SUDV), and the Angola strain of Marburg marburgvirus (MARV) GPs. NHPs were vaccinated with a single dose of the trivalent formulation, followed by lethal challenge 28 days later with each of the three corresponding filoviruses. At day 14 postvaccination, a serum IgG response specific for all three GPs was detected in all the vaccinated macaques. A modest and balanced cell-mediated immune response specific for each GP was also detected in a majority of the vaccinated macaques. No matter the level of total GP-specific immune response detected postvaccination, all the vaccinated macaques were protected from disease and death following lethal challenge with each of the three filoviruses. These findings indicate that vaccination with a single dose of attenuated rVSV-N4CT1 vectors each expressing a single filovirus GP may provide protection against the filoviruses most commonly responsible for outbreaks of hemorrhagic fever in sub-Saharan Africa. IMPORTANCE The West African Ebola virus Zaire outbreak in 2013 showed that the disease was not only a regional concern, but a worldwide problem, and highlighted the need for a safe and efficacious vaccine to be administered to the populace. However, other endemic pathogens, like Ebola virus Sudan and Marburg, also pose an important health risk to the public and therefore require development of a vaccine prior to the occurrence of an outbreak. The significance of our research was the development of a blended trivalent filovirus vaccine that elicited a balanced immune response when administered as a single dose and provided complete protection against a lethal challenge with all three filovirus pathogens.

Published

2017

12. Recombinant Isfahan Virus and Vesicular Stomatitis Virus Vaccine Vectors Provide Durable, Multivalent, Single-Dose Protection against Lethal Alphavirus Challenge

Author

Stefan Hamm, Theresa E. Latham, David K. Clarke, John H. Eldridge, Scott C. Weaver, Robert L. Seymour, Grace Leal, Demetrius Matassov, Rebecca M. Nowak, Farooq Nasar, Robert B. Tesh, and Rodion Gorchakov

Subjects

0301 basic medicine, Encephalomyelitis, Equine, Eastern equine encephalitis virus, Immunology, Alphavirus, medicine.disease_cause, Recombinant virus, Antibodies, Viral, Microbiology, Encephalitis Virus, Venezuelan Equine, 03 medical and health sciences, Mice, Virology, Vaccines and Antiviral Agents, medicine, Animals, Vector (molecular biology), Neutralizing antibody, Glycoproteins, Drug Carriers, Vaccines, Synthetic, biology, Immunogenicity, Membrane Proteins, Viral Vaccines, Vesiculovirus, biology.organism_classification, Antibodies, Neutralizing, Survival Analysis, Disease Models, Animal, 030104 developmental biology, Vesicular stomatitis virus, Insect Science, Venezuelan equine encephalitis virus, biology.protein, Encephalitis Virus, Eastern Equine

Abstract

The demonstrated clinical efficacy of a recombinant vesicular stomatitis virus (rVSV) vaccine vector has stimulated the investigation of additional serologically distinct Vesiculovirus vectors as therapeutic and/or prophylactic vaccine vectors to combat emerging viral diseases. Among these viral threats are the encephalitic alphaviruses Venezuelan equine encephalitis virus (VEEV) and Eastern equine encephalitis virus (EEEV), which have demonstrated potential for natural disease outbreaks, yet no licensed vaccines are available in the event of an epidemic. Here we report the rescue of recombinant Isfahan virus (rISFV) from genomic cDNA as a potential new vaccine vector platform. The rISFV genome was modified to attenuate virulence and express the VEEV and EEEV E2/E1 surface glycoproteins as vaccine antigens. A single dose of the rISFV vaccine vectors elicited neutralizing antibody responses and protected mice from lethal VEEV and EEEV challenges at 1 month postvaccination as well as lethal VEEV challenge at 8 months postvaccination. A mixture of rISFV vectors expressing the VEEV and EEEV E2/E1 glycoproteins also provided durable, single-dose protection from lethal VEEV and EEEV challenges, demonstrating the potential for a multivalent vaccine formulation. These findings were paralleled in studies with an attenuated form of rVSV expressing the VEEV E2/E1 glycoproteins. Both the rVSV and rISFV vectors were attenuated by using an approach that has demonstrated safety in human trials of an rVSV/HIV-1 vaccine. Vaccines based on either of these vaccine vector platforms may present a safe and effective approach to prevent alphavirus-induced disease in humans. IMPORTANCE This work introduces rISFV as a novel vaccine vector platform that is serologically distinct and phylogenetically distant from VSV. The rISFV vector has been attenuated by an approach used for an rVSV vector that has demonstrated safety in clinical studies. The vaccine potential of the rISFV vector was investigated in a well-established alphavirus disease model. The findings indicate the feasibility of producing a safe, efficacious, multivalent vaccine against the encephalitic alphaviruses VEEV and EEEV, both of which can cause fatal disease. This work also demonstrates the efficacy of an attenuated rVSV vector that has already demonstrated safety and immunogenicity in multiple HIV-1 phase I clinical studies. The absence of serological cross-reactivity between rVSV and rISFV and their phylogenetic divergence within the Vesiculovirus genus indicate potential for two stand-alone vaccine vector platforms that could be used to target multiple bacterial and/or viral agents in successive immunization campaigns or as heterologous prime-boost agents.

Published

2017

13. mTOR/p70S6K signaling distinguishes routine, maintenance-level autophagy from autophagic cell death during influenza A infection

Author

Antonella Tinari, Alireza Shirazian, Shawna Benjamin, Demetrius Matassov, Walter Malorni, Richard A. Lockshin, Zahra Zakeri, Emmanuel Datan, and Adolfo García-Sastre

Subjects

Cell death, Programmed cell death, Cell, Apoptosis, Mechanistic Target of Rapamycin Complex 2, mTORC1, Mechanistic Target of Rapamycin Complex 1, Biology, mTORC2, Article, Phosphatidylinositol 3-Kinases, 03 medical and health sciences, 0302 clinical medicine, Virology, Influenza, Human, Autophagy, medicine, Humans, Rapamycin, p70S6K, PI3K/AKT/mTOR pathway, 030304 developmental biology, Torin1, 0303 health sciences, TOR Serine-Threonine Kinases, Ribosomal Protein S6 Kinases, 70-kDa, mTORC1/2, Influenza, 3. Good health, Cell biology, medicine.anatomical_structure, Influenza A virus, Multiprotein Complexes, 030220 oncology & carcinogenesis, biological phenomena, cell phenomena, and immunity, Signal transduction, Signal Transduction

Abstract

Autophagy, a stress response activated in influenza A virus infection helps the cell avoid apoptosis. However, in the absence of apoptosis infected cells undergo vastly expanded autophagy and nevertheless die in the presence of necrostatin but not of autophagy inhibitors. Combinations of inhibitors indicate that the controls of protective and lethal autophagy are different. Infection that triggers apoptosis also triggers canonical autophagy signaling exhibiting transient PI3K and mTORC1 activity. In terminal autophagy phospho-mTOR(Ser2448) is suppressed while mTORC1, PI3K and mTORC2 activities increase. mTORC1 substrate p70S6K becomes highly phosphorylated while its activity, now regulated by mTORC2, is required for LC3-II formation. Inhibition of mTORC2/p70S6K, unlike that of PI3K/mTORC1, blocks expanded autophagy in the absence of apoptosis but not moderate autophagy. Inhibitors of expanded autophagy limit virus reproduction. Thus expanded, lethal autophagy is activated by a signaling mechanism different from autophagy that helps cells survive toxic or stressful episodes.

Published

2014

14. A Novel Intranasal Virus-Like Particle (VLP) Vaccine Designed to Protect against the Pandemic 1918 Influenza A Virus (H1N1)

Author

Albert Cupo, Demetrius Matassov, and Jose M. Galarza

Subjects

viruses, Immunology, Hemagglutinins, Viral, Neuraminidase, Nose, Antibodies, Viral, medicine.disease_cause, Virus, Microbiology, Placebos, Viral Matrix Proteins, Mice, Viral Proteins, Influenza A Virus, H1N1 Subtype, Adjuvants, Immunologic, Orthomyxoviridae Infections, Virus-like particle, Virology, Influenza, Human, Influenza A virus, medicine, Animals, Humans, Lung, Administration, Intranasal, Mice, Inbred BALB C, biology, Body Weight, Antibody titer, Viral Vaccines, Vaccine efficacy, Vaccines, Virosome, Titer, Oligodeoxyribonucleotides, Influenza Vaccines, biology.protein, Molecular Medicine, Female, Antibody

Abstract

We have prepared a virus-like particle (VLP) vaccine bearing the surface glycoproteins HA and NA of the 1918 influenza A virus by infecting Sf9 cells with a quadruple recombinant baculovirus that expresses the four influenza proteins (HA, NA, M1, and M2) required for the assembly and budding of the VLPs. The presence of HA and M1 in the purified VLPs was confirmed by Western blot, and that of NA by a neuraminidase enzymatic assay. For in vivo studies, the 1918 VLP vaccine was formulated with or without an oligonucleotide containing two CpG motifs and administered in two doses 2 wk apart via the intranasal route. The antibody titers in mice immunized with VLP vaccines were higher than in mice vaccinated with an inactivated swine virus (H1N1) control, when CHO cells expressing 1918 HA were used as antigen. The opposite result was obtained when disrupted swine virus was the antigen for the ELISA test. Vaccine efficacy was evaluated by challenging immunized mice with the 1918 antigenically related influenza virus A/swine/Iowa/15/30 (H1N1) and measuring viral titers in the upper and lower respiratory tract. Mice immunized with VLP vaccine plus CpG demonstrated significantly lower viral titers in the nose and lungs than did the control on days 2 and 4 postchallenge and completely cleared the virus by day 6. Furthermore, they did not show symptoms of disease although there was a minor decrease in body weight. Mice vaccinated with VLP alone also demonstrated significantly lower viral titers in the nose and lungs than did the placebo group as well as the inactivated virus group on days 4 and 6 postchallenge. These results suggest that it is feasible to make a safe and immunogenic vaccine to protect against the extremely virulent 1918 virus, using a novel and safe cell-based technology.

Published

2007

15. Vaccination With a Highly Attenuated Recombinant Vesicular Stomatitis Virus Vector Protects Against Challenge With a Lethal Dose of Ebola Virus

Author

Ayuko Ota-Setlik, Andrea Marzi, John H. Eldridge, Demetrius Matassov, Heinz Feldmann, Michael A. Egan, Friederike Feldmann, Stefan Hamm, Joan B. Geisbert, Becky Nowak, Terri Latham, David K. Clarke, Rong Xu, Thomas W. Geisbert, and Chad E. Mire

Subjects

Male, Genetic Vectors, Guinea Pigs, Biology, Vesicular stomatitis Indiana virus, medicine.disease_cause, Antibodies, Viral, Vaccines, Attenuated, Vesicular Stomatitis, Mice, Viral Proteins, Immune system, medicine, Immunology and Allergy, Animals, Ebola and Marburg Viruses-Research, Outbreak Management, Epidemiology and Ecology, Glycoproteins, Ebolavirus, Immunity, Cellular, Mice, Inbred BALB C, Ebola virus, Ebola vaccine, Viral Vaccine, Vaccination, Viral Vaccines, Vesiculovirus, Hemorrhagic Fever, Ebola, biology.organism_classification, Virology, Macaca mulatta, Immunity, Humoral, Infectious Diseases, Vesicular stomatitis virus, Female

Abstract

Previously, recombinant vesicular stomatitis virus (rVSV) pseudotypes expressing Ebolavirus glycoproteins (GPs) in place of the VSV G protein demonstrated protection of nonhuman primates from lethal homologous Ebolavirus challenge. Those pseudotype vectors contained no additional attenuating mutations in the rVSV genome. Here we describe rVSV vectors containing a full complement of VSV genes and expressing the Ebola virus (EBOV) GP from an additional transcription unit. These rVSV vectors contain the same combination of attenuating mutations used previously in the clinical development pathway of an rVSV/human immunodeficiency virus type 1 vaccine. One of these rVSV vectors (N4CT1-EBOVGP1), which expresses membrane-anchored EBOV GP from the first position in the genome (GP1), elicited a balanced cellular and humoral GP-specific immune response in mice. Guinea pigs immunized with a single dose of this vector were protected from any signs of disease following lethal EBOV challenge, while control animals died in 7-9 days. Subsequently, N4CT1-EBOVGP1 demonstrated complete, single-dose protection of 2 macaques following lethal EBOV challenge. A single sham-vaccinated macaque died from disease due to EBOV infection. These results demonstrate that highly attenuated rVSV vectors expressing EBOV GP may provide safer alternatives to current EBOV vaccines.

Published

2015

16. Influenza A Virus Lacking the NS1 Gene Replicates in Interferon-Deficient Systems

Author

Adolfo García-Sastre, David E. Levy, Peter Palese, Demetrius Matassov, Thomas Muster, Sabine Brandt, Andrej Egorov, and Joan E. Durbin

Subjects

viruses, Virulence, Chick Embryo, Viral Nonstructural Proteins, Biology, Kidney, Transfection, Virus Replication, medicine.disease_cause, H5N1 genetic structure, Antigenic drift, Cell Line, Mice, Dogs, Orthomyxoviridae Infections, Interferon, Virology, Chlorocebus aethiops, Influenza A virus, medicine, Animals, Vero Cells, Gene, Mice, Knockout, Genetics, Mice, Inbred BALB C, virus diseases, biochemical phenomena, metabolism, and nutrition, Reverse genetics, DNA-Binding Proteins, Mice, Inbred C57BL, STAT1 Transcription Factor, Viral replication, Trans-Activators, Gene Deletion, Signal Transduction, medicine.drug

Abstract

The NS1 protein is the only nonstructural protein encoded by influenza A virus. It has been proposed that the NS1 performs several regulatory functions during the viral replication cycle, including the regulation of synthesis, transport, splicing, and translation of mRNAs. Through the use of reverse genetics, a viable transfectant influenza A virus (delNS1) which lacks the NS1 gene has been generated. Our results indicate that the NS1 of influenza A virus is an auxiliary (virulence) factor which plays a crucial role in inhibiting interferon-mediated antiviral responses of the host.

Published

1998

17. Measurement of apoptosis by DNA fragmentation

Author

Demetrius, Matassov, Terri, Kagan, Julie, Leblanc, Marianna, Sikorska, and Zahra, Zakeri

Subjects

Electrophoresis, Apoptosis, DNA, DNA Fragmentation

Abstract

Classical apoptotic cell death can be defined by certain morphological and biochemical characteristics that distinguish it from other forms of cell death. One such feature, which is a hallmark of apoptosis, is DNA fragmentation. In dying cells, DNA is cleaved by an endonuclease that fragments the chromatin into nucleosomal units, which are multiples of about 180-bp oligomers and appear as a DNA ladder when run on an agarose gel. Here, we present commonly used methods such as conventional agarose gel electrophoresis to analyze fragmented nuclei in cells. The various methods used are dependent on the extent of fragmentation or the amount of fragmented nuclei in a sample. Determining whether a cell exhibits DNA fragmentation can provide information about the type of cell death occurring and the pathways activated in the dying cell.

Published

2004

18. Measurement of Apoptosis by DNA Fragmentation

Author

Zahra Zakeri, Terri Kagan, Marianna Sikorska, Demetrius Matassov, and J LeBlanc

Subjects

chemistry.chemical_compound, Programmed cell death, Apoptosis, Chemistry, Agarose gel electrophoresis, Apoptotic DNA fragmentation, DNA fragmentation, Fragmentation (cell biology), DNA, Chromatin, Cell biology

Abstract

Classical apoptotic cell death can be defined by certain morphological and biochemical characteristics that distinguish it from other forms of cell death. One such feature, which is a hallmark of apoptosis, is DNA fragmentation. In dying cells, DNA is cleaved by an endonuclease that fragments the chromatin into nucleosomal units, which are multiples of about 180-bp oligomers and appear as a DNA ladder when run on an agarose gel. Here, we present commonly used methods such as conventional agarose gel electrophoresis to analyze fragmented nuclei in cells. The various methods used are dependent on the extent of fragmentation or the amount of fragmented nuclei in a sample. Determining whether a cell exhibits DNA fragmentation can provide information about the type of cell death occurring and the pathways activated in the dying cell.

Published

2004

19. A Novel Intranasal Virus-Like Particle (VLP) Vaccine Designed to Protect against the Pandemic 1918 Influenza A Virus (H1N1).

Author

Demetrius Matassov, Albert Cupo, and Jose M. Galarza

Subjects

*INTRANASAL medication, *INFLUENZA A virus, *PREVENTIVE medicine, *VACCINATION

Abstract

We have prepared a virus-like particle (VLP) vaccine bearing the surface glycoproteins HA and NA of the 1918 influenza A virus by infecting Sf9 cells with a quadruple recombinant baculovirus that expresses the four influenza proteins (HA, NA, M1, and M2) required for the assembly and budding of the VLPs. The presence of HA and M1 in the purified VLPs was confirmed by Western blot, and that of NA by a neuraminidase enzymatic assay. For in vivostudies, the 1918 VLP vaccine was formulated with or without an oligonucleotide containing two CpG motifs and administered in two doses 2 wk apart via the intranasal route. The antibody titers in mice immunized with VLP vaccines were higher than in mice vaccinated with an inactivated swine virus (H1N1) control, when CHO cells expressing 1918 HA were used as antigen. The opposite result was obtained when disrupted swine virus was the antigen for the ELISA test. Vaccine efficacy was evaluated by challenging immunized mice with the 1918 antigenically related influenza virus AswineIowa1530 (H1N1) and measuring viral titers in the upper and lower respiratory tract. Mice immunized with VLP vaccine plus CpG demonstrated significantly lower viral titers in the nose and lungs than did the control on days 2 and 4 postchallenge and completely cleared the virus by day 6. Furthermore, they did not show symptoms of disease although there was a minor decrease in body weight. Mice vaccinated with VLP alone also demonstrated significantly lower viral titers in the nose and lungs than did the placebo group as well as the inactivated virus group on days 4 and 6 postchallenge. These results suggest that it is feasible to make a safe and immunogenic vaccine to protect against the extremely virulent 1918 virus, using a novel and safe cell-based technology. [ABSTRACT FROM AUTHOR]

Published

2007