Your search keyword '"Jakub K. Simon"' showing total 23 results

1. Antibodies against the Ebola virus soluble glycoprotein are associated with long-term vaccine-mediated protection of non-human primates

Author

Bronwyn M. Gunn, Ryan P. McNamara, Lianna Wood, Sabian Taylor, Anush Devadhasan, Wenyu Guo, Jishnu Das, Avlant Nilsson, Amy Shurtleff, Sheri Dubey, Michael Eichberg, Todd J. Suscovich, Erica Ollmann Saphire, Douglas Lauffenburger, Beth-Ann Coller, Jakub K. Simon, and Galit Alter

Subjects

CP: Immunology, Biology (General), QH301-705.5

Abstract

Summary: The 2013 Ebola epidemic in Central and West Africa heralded the emergence of wide-spread, highly pathogenic viruses. The successful recombinant vector vaccine against Ebola (rVSVΔG-ZEBOV-GP) will limit future outbreaks, but identifying mechanisms of protection is essential to protect the most vulnerable. Vaccine-induced antibodies are key determinants of vaccine efficacy, yet the mechanism by which vaccine-induced antibodies prevent Ebola infection remains elusive. Here, we exploit a break in long-term vaccine efficacy in non-human primates to identify predictors of protection. Using unbiased humoral profiling that captures neutralization and Fc-mediated functions, we find that antibodies specific for soluble glycoprotein (sGP) drive neutrophil-mediated phagocytosis and predict vaccine-mediated protection. Similarly, we show that protective sGP-specific monoclonal antibodies have elevated neutrophil-mediated phagocytic activity compared with non-protective antibodies, highlighting the importance of sGP in vaccine protection and monoclonal antibody therapeutics against Ebola virus.

Published

2023

2. rVSVΔG-ZEBOV-GP (also designated V920) recombinant vesicular stomatitis virus pseudotyped with Ebola Zaire Glycoprotein: Standardized template with key considerations for a risk/benefit assessment

Author

Thomas P. Monath, Patricia E. Fast, Kayvon Modjarrad, David K. Clarke, Brian K. Martin, Joan Fusco, Richard Nichols, D. Gray Heppner, Jakub K. Simon, Sheri Dubey, Sean P. Troth, Jayanthi Wolf, Vidisha Singh, Beth-Ann Coller, and James S. Robertson

Subjects

Immunologic diseases. Allergy, RC581-607

Abstract

The Brighton Collaboration Viral Vector Vaccines Safety Working Group (V3SWG) was formed to evaluate the safety and characteristics of live, recombinant viral vector vaccines. A recent publication by the V3SWG described live, attenuated, recombinant vesicular stomatitis virus (rVSV) as a chimeric virus vaccine for HIV-1 (Clarke et al., 2016). The rVSV vector system is being explored as a platform for development of multiple vaccines. This paper reviews the molecular and biological features of the rVSV vector system, followed by a template with details on the safety and characteristics of a rVSV vaccine against Zaire ebolavirus (ZEBOV). The rVSV-ZEBOV vaccine is a live, replication competent vector in which the VSV glycoprotein (G) gene is replaced with the glycoprotein (GP) gene of ZEBOV. Multiple copies of GP are expressed and assembled into the viral envelope responsible for inducing protective immunity. The vaccine (designated V920) was originally constructed by the National Microbiology Laboratory, Public Health Agency of Canada, further developed by NewLink Genetics Corp. and Merck & Co., and is now in final stages of registration by Merck. The vaccine is attenuated by deletion of the principal virulence factor of VSV (the G protein), which also removes the primary target for anti-vector immunity. The V920 vaccine caused no toxicities after intramuscular (IM) or intracranial injection of nonhuman primates and no reproductive or developmental toxicity in a rat model. In multiple studies, cynomolgus macaques immunized IM with a wide range of virus doses rapidly developed ZEBOV-specific antibodies measured in IgG ELISA and neutralization assays and were fully protected against lethal challenge with ZEBOV virus. Over 20,000 people have received the vaccine in clinical trials; the vaccine has proven to be safe and well tolerated. During the first few days after vaccination, many vaccinees experience a mild acute-phase reaction with fever, headache, myalgia, and arthralgia of short duration; this period is associated with a low-level viremia, activation of anti-viral genes, and increased levels of chemokines and cytokines. Oligoarthritis and rash appearing in the second week occur at a low incidence, and are typically mild-moderate in severity and self-limited. V920 vaccine was used in a Phase III efficacy trial during the West African Ebola epidemic in 2015, showing 100% protection against Ebola Virus Disease, and it has subsequently been deployed for emergency control of Ebola outbreaks in central Africa. The template provided here provides a comprehensive picture of the first rVSV vector to reach the final stage of development and to provide a solution to control of an alarming human disease. Keywords: Vaccines, Ebola vaccine, Vesicular stomatitis virus vector, Viral vector, Brighton collaboration, Risk/benefit assessment, Vaccine safety

Published

2019

3. Development of Pandemic Vaccines: ERVEBO Case Study

Author

Jayanthi Wolf, Risat Jannat, Sheri Dubey, Sean Troth, Matthew T. Onorato, Beth-Ann Coller, Mary E. Hanson, and Jakub K. Simon

Subjects

Ebolavirus vaccine, rVSVΔG-ZEBOV-GP, vaccine development, regulatory strategy, vaccine manufacturing, Medicine

Abstract

Preventative vaccines are considered one of the most cost-effective and efficient means to contain outbreaks and prevent pandemics. However, the requirements to gain licensure and manufacture a vaccine for human use are complex, costly, and time-consuming. The 2013–2016 Ebola virus disease (EVD) outbreak was the largest EVD outbreak to date and the third Public Health Emergency of International Concern in history, so to prevent a pandemic, numerous partners from the public and private sectors combined efforts and resources to develop an investigational Zaire ebolavirus (EBOV) vaccine candidate (rVSVΔG-ZEBOV-GP) as quickly as possible. The rVSVΔG-ZEBOV-GP vaccine was approved as ERVEBOTM by the European Medicines Authority (EMA) and the United States Food and Drug Administration (FDA) in December 2019 after five years of development. This review describes the development program of this EBOV vaccine, summarizes what is known about safety, immunogenicity, and efficacy, describes ongoing work in the program, and highlights learnings applicable to the development of pandemic vaccines.

Published

2021

4. Gut-homing conventional plasmablasts and CD27- plasmablasts elicited after a short time exposure to an oral live attenuated Shigella vaccine candidate in humans

Author

Franklin R. Toapanta, Jakub K. Simon, Eileen M. Barry, Marcela F. Pasetti, Myron M. Levine, Karen L. Kotloff, and Marcelo B. Sztein

Subjects

Shigella, B cells, Homing, plasmablasts, Oral Vaccine, Immunologic diseases. Allergy, RC581-607

Abstract

Currently, there is no licensed Shigella vaccine; however, various promising live attenuated vaccine candidates have emerged, including CVD1208S (ΔguaBA, Δset, Δsen S. flexneri 2a), which was shown to be safe and immunogenic in Phase 1 clinical trials. Here we report the immune responses elicited in an outpatient Phase 2 clinical trial in which subjects were vaccinated with CVD 1208S. Oral immunization with CVD 1208S elicited high anti-S. flexneri 2a LPS and IpaB antibody responses, as well as an acute plasmablast (PB) infiltration in peripheral blood 7 days after immunization. PB sorted based on their expression of homing molecules confirmed that cells expressing integrin α4β7 alone or in combination with CD62L were responsible for antibody production (as measured by ELISpot). Furthermore, using high-color flow-cytometry, on day 7 after immunization, we observed the appearance of conventional PB (CPB, CD19dim CD20- CD27+high CD38+high CD3-), as well as a PB population that did not express CD27 (CD27- PB; pre-plasmablasts). The pattern of individual or simultaneous expression of homing markers (integrin α4β7, CD62L, CXCR3 and CXCR4) suggested that CPB cells homed preferentially to the inflamed gut mucosa. In contrast, ~50% CD27- PB cells appear to home to yet to be identified peripheral lymphoid organs or were in a transition state preceding integrin α4β7 upregulation. In sum, these observations demonstrate that strong immune responses, including distinct PB subsets with the potential to home to the gut and other secondary lymphoid organs, can be elicited after a short time of exposure to a shigella oral

Published

2014

5. Association Between State Hepatitis A Vaccination Requirements and Hepatitis A Vaccination Rates

Author

Yoonyoung Choi, Alexandra Bhatti, Zhiwen Liu, Alex Ruch, Ava Skolnik, Cristina Carias, Michelle G Goveia, and Jakub K Simon

Subjects

Schools, Infectious Diseases, Adolescent, Immunization Programs, Vaccination, education, Pediatrics, Perinatology and Child Health, Humans, Immunization, General Medicine, Hepatitis A, Child, United States

Abstract

Using National Immunization Survey Child and Teen (2008-2017), we associated state vaccination requirements with hepatitis A (Hep A) vaccination rates in children and adolescents. States with school entry or both childcare and school entry requirements were associated with 35%-40% higher Hep A vaccination rates, compared with states without such requirements.

Published

2022

6. Lot-to-lot consistency, safety, tolerability, and immunogenicity of V114, a 15-valent pneumococcal conjugate vaccine, in healthy adults aged ≥50 years: A randomized phase 3 trial (PNEU-TRUE)

Author

Jakub K. Simon, Nina Breinholt Staerke, Maria Hemming-Harlo, Stacey Layle, Ron Dagan, Tulin Shekar, Alison Pedley, Patricia Jumes, Gretchen Tamms, Tina Sterling, Luwy Musey, and Ulrike K. Buchwald

Subjects

Vaccines, Conjugate, General Veterinary, General Immunology and Microbiology, Vaccination, Lot consistency, Public Health, Environmental and Occupational Health, PCV13, Pneumococcal vaccine, Middle Aged, Serogroup, Antibodies, Bacterial, Pneumococcal Infections, Pneumococcal Vaccines, Immunogenicity, Vaccine, Infectious Diseases, Humans, Adults, Molecular Medicine, 15-valent PCV, V114, Aged

Abstract

Background: Older adults are at risk of pneumococcal disease and associated morbidity and mortality. This phase 3 study (V114-020) assessed lot-to-lot consistency across safety and immunogenicity outcomes for V114, a 15-valent pneumococcal conjugate vaccine (PCV), in healthy adults aged ≥ 50 years. Methods: Adults were randomized in a 3:3:3:1 ratio to receive a single dose of one of three lots of V114 or 13-valent PCV (PCV13), stratified by age (50–64 years, 65–74 years, and ≥ 75 years). Serotype-specific opsonophagocytic activity (OPA) and immunoglobulin G (IgG) antibodies were evaluated at baseline (Day 1) and 30 days post-vaccination. Non-serious and serious adverse events (AEs) were evaluated post-vaccination through 14 days and Month 6, respectively. Results: Of 2340 participants enrolled, 2282 (97.5%) completed the study. Proportions of participants experiencing ≥ 1 AE were 81.0%, 77.4%, and 78.0% for V114 lots 1, 2, and 3, respectively. Comparison of V114 combined lots with PCV13 showed that proportions of participants experiencing AEs, solicited AEs, and serious AEs were comparable for both vaccines, with the exception of injection-site pain (more frequently reported with V114). OPA geometric mean titers (GMTs) and IgG geometric mean concentrations (GMCs) at 30 days post-vaccination were comparable across V114 lots, and all lots met predefined equivalence criteria for all 15 vaccine serotypes (lower and upper limits of the 95% confidence intervals of serotype-specific OPA GMT ratios for all possible pairwise comparisons across the three lots were within the equivalence margin of 0.5–2.0). Serotype-specific OPA GMTs and IgG GMCs were comparable in the V114 combined lots and PCV13 groups for the 13 shared serotypes and higher in the V114 group for serotypes unique to V114 (22F and 33F). Conclusions: V114 is well tolerated with a consistent safety profile and immune response across manufacturing lots. Clinical trials registration: NCT03950856 (www.clinicaltrials.gov); 2018-004266-33 (EudraCT).

Published

2022

7. Effects of Gamma Irradiation of Human Serum Samples from rVSVΔG-ZEBOV-GP (V920) Ebola Virus Vaccine Recipients on Plaque-Reduction Neutralization Assays

Author

Joseph M. Antonello, Rick Nichols, Rebecca J. Grant-Klein, Sheri Dubey, and Jakub K. Simon

Subjects

Phases of clinical research, Antibodies, Viral, medicine.disease_cause, Neutralization, Immunogenicity, Vaccine, Viral Envelope Proteins, Neutralization Tests, Virology, parasitic diseases, Humans, Medicine, Prospective Studies, Ebola Vaccines, Neutralizing antibody, Ebola virus, biology, business.industry, Immune Sera, Vaccination, Articles, Vesiculovirus, Hemorrhagic Fever, Ebola, Ebolavirus, Serum samples, Antibodies, Neutralizing, Healthy Volunteers, Target dose, Titer, Infectious Diseases, biology.protein, population characteristics, Parasitology, business, human activities, Gamma irradiation

Abstract

Gamma irradiation (GI) is included in the CDC guidance on inactivation procedures to render a group of select agents and toxins nonviable. The Ebola virus falls within this group because it potentially poses a severe threat to public health and safety. To evaluate the impact of GI at a target dose of 50 kGy on neutralizing antibody titers induced by the rVSVΔG-ZEBOV-GP vaccine (V920), we constructed a panel of 48 paired human serum samples (GI-treated versus non–GI-treated) from healthy participants selected from a phase 3 study of V920 (study V920-012; NCT02503202). Neutralizing antibody titers were determined using a validated plaque-reduction neutralization test. GI of sera from V920 recipients was associated with approximately 20% reduction in postvaccination neutralizing antibody titers. GI was not associated with any change in pre-vaccination neutralizing antibody titers.

Published

2021

8. Serostatus cutoff levels and fold increase to define seroresponse to recombinant vesicular stomatitis virus – Zaire Ebola virus envelope glycoprotein vaccine: An evidence-based analysis

Author

Rebecca J. Grant-Klein, Sheri Dubey, Stephen B. Kennedy, Jakub K. Simon, Rick Nichols, and Joseph M. Antonello

Subjects

030231 tropical medicine, Antibodies, Viral, Placebo, medicine.disease_cause, law.invention, 03 medical and health sciences, 0302 clinical medicine, Immune system, law, Animals, Humans, Medicine, 030212 general & internal medicine, Ebola Vaccines, Ebola virus, General Veterinary, General Immunology and Microbiology, biology, business.industry, Public Health, Environmental and Occupational Health, Hemorrhagic Fever, Ebola, Ebolavirus, biology.organism_classification, Virology, Vaccination, Titer, Infectious Diseases, Vesicular stomatitis virus, Viral Envelope, Democratic Republic of the Congo, Recombinant DNA, Molecular Medicine, Vesicular Stomatitis, business, Serostatus

Abstract

The recombinant vesicular stomatitis virus - Zaire Ebola virus envelope glycoprotein (rVSVΔG-ZEBOV-GP) vaccine is a live recombinant vesicular stomatitis virus (VSV) where the VSV G protein is replaced with ZEBOV-GP. To better understand the immune response after receiving the rVSVΔG-ZEBOV-GP vaccine, the current analyses evaluated different definitions of seroresponse that differentiate vaccine and placebo recipients enrolled in a placebo-controlled clinical trial (PREVAIL; NCT02344407) in which a subset of the study participants had elevated baseline titers. Alternative values for serostatus cutoff (SSCO; 200-500 EU/mL) and/or fold rise (two- to five-fold) were applied to compare their ability to distinguish between participants receiving rVSVΔG-ZEBOV-GP or placebo. The results indicate that an SSCO of 200 EU/mL can be used to define seropositivity at baseline (i.e. pre-vaccination). The use of dual criteria of the same SSCO (200 EU/mL) together with a two-fold rise in antibody level from baseline provided the definition of seroresponse that maximized the statistical significance between vaccine recipients and placebo recipients post-vaccination. Clinical trial registration: NCT02344407.

Published

2020

9. Immunogenicity of rVSVΔG-ZEBOV-GP Ebola vaccine (ERVEBO®) in African clinical trial participants by age, sex, and baseline GP-ELISA titer: A post hoc analysis of three Phase 2/3 trials

Author

Jakub K. Simon, Stephen B. Kennedy, Barbara E. Mahon, Sheri A. Dubey, Rebecca J. Grant-Klein, Ken Liu, Jonathan Hartzel, Beth-Ann G. Coller, Carolee Welebob, Mary E. Hanson, and Rebecca F. Grais

Subjects

Adult, Male, General Veterinary, General Immunology and Microbiology, Adolescent, Public Health, Environmental and Occupational Health, Enzyme-Linked Immunosorbent Assay, Middle Aged, Hemorrhagic Fever, Ebola, Antibodies, Viral, Ebolavirus, Antibodies, Neutralizing, Young Adult, Infectious Diseases, Immunogenicity, Vaccine, Viral Envelope Proteins, Immunoglobulin G, Molecular Medicine, Humans, Female, Ebola Vaccines, Glycoproteins

Abstract

ERVEBO®, a live recombinant vesicular stomatitis virus (VSV) vaccine containing the Zaire ebolavirus glycoprotein (GP) in place of the VSV GP (rVSVΔG-ZEBOV-GP), was advanced through clinical development by MerckCo., Inc., Rahway, NJ, USA in collaboration with multiple partners to prevent Ebola virus disease (EVD) and has been approved for human use in several countries.We evaluated data from three Phase 2/3 clinical trials conducted in Liberia (PREVAIL), Guinea (FLW), and Sierra Leone (STRIVE) during the 2013-2016 West African EVD outbreak to assess immune responses using validated assays. We performed a post hoc analysis of the association of vaccine response with sex, age (18-50 yrs50 yrs), and baseline (BL) GP-enzyme-linked immunosorbent assay (ELISA) titer (200≥200 EU/mL), including individual study (PREVAIL, FLW, or STRIVE) data and pooled data from all 3 studies. The endpoints were total IgG antibody response (EU/mL) measured by the GP-ELISA and neutralizing antibody response measured by the plaque reduction neutralization test (PRNT) to rVSVΔG-ZEBOV-GP at Days 28, 180, and 365 postvaccination.In the overall pooled population, in all subgroups, and in each trial independently, GP-ELISA and PRNT geometric mean titers increased from BL, generally peaking at Day 28 and persisting through Day 365. Immune responses were greater in women and participants with BL GP-ELISA ≥ 200 EU/mL, but did not differ across age groups.These data demonstrate that rVSVΔG-ZEBOV-GP elicits a robust and durable immune response through 12 months postvaccination in participants regardless of age, sex, or BL GP-ELISA titer. The higher immune responses observed in women and participants with pre-existing immunity are consistent with those described previously and for other vaccines. Trials were registered as follows: PREVAIL: ClinicalTrials.gov NCT02344407; FLW: Pan African Clinical Trials Registry PACTR201503001057193; STRIVE: ClinicalTrials.gov NCT02378753. Protocols V920-009, 011, and 018.

Published

2022

10. Lipopolysaccharide-specific memory B cell responses to an attenuated live cholera vaccine are associated with protection against Vibrio cholerae infection

Author

Marc Gurwith, Mitchell B. Cohen, Beth D. Kirkpatrick, Jakub K. Simon, Marcelo B. Sztein, Douglas Haney, Jason B. Harris, Glenn Ishioka, Myron M. Levine, Caroline E. Lyon, Wilbur H. Chen, and Michael Lock

Subjects

Adult, Lipopolysaccharides, 0301 basic medicine, Cholera Toxin, Time Factors, Administration, Oral, Vaccines, Attenuated, medicine.disease_cause, Article, 03 medical and health sciences, Cholera, medicine, Humans, Seroconversion, Memory B cell, B-Lymphocytes, Attenuated vaccine, General Veterinary, General Immunology and Microbiology, business.industry, Cholera toxin, Vibrio cholerae O1, Public Health, Environmental and Occupational Health, Cholera Vaccines, medicine.disease, Antibodies, Bacterial, Immunoglobulin A, Vaccination, 030104 developmental biology, Infectious Diseases, Vibrio cholerae, Immunoglobulin G, Immunology, Molecular Medicine, Cholera vaccine, business, Immunologic Memory

Abstract

Background The single-dose live attenuated vaccine CVD 103-HgR protects against experimental Vibrio cholerae infection in cholera-naive adults for at least 6 months after vaccination. While vaccine-induced vibriocidal seroconversion is associated with protection, vibriocidal titers decline rapidly from their peak 1–2 weeks after vaccination. Although vaccine-induced memory B cells (MBCs) might mediate sustained protection in individuals without detectable circulating antibodies, it is unknown whether oral cholera vaccination induces a MBC response. Methods In a study that enrolled North American adults, we measured lipopolysaccharide (LPS)- and cholera toxin (CtxB)-specific MBC responses to PXVX0200 (derived from the CVD 103-HgR strain) and assessed stool volumes following experimental Vibrio cholerae infection. We then evaluated the association between vaccine-induced MBC responses and protection against cholera. Results There was a significant increase in % CT-specific IgG, % LPS-specific IgG, and % LPS-specific IgA MBCs which persisted 180 days after vaccination as well as a significant association between vaccine-induced increase in % LPS-specific IgA MBCs and lower post-challenge stool volume (r = −0.56, p Discussion Oral cholera vaccination induces antigen-specific MBC responses, and the anamnestic LPS-specific responses may contribute to long-term protection and provide correlates of the duration of vaccine-induced protection. Clinical trials registration: NCT01895855.

Published

2018

11. Safety and immunogenicity of single-dose live oral cholera vaccine strain CVD 103-HgR in healthy adults age 18–45

Author

James M. McCarty, Kristin Hunt, Marc Gurwith, Jakub K. Simon, and Michael Lock

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, 030231 tropical medicine, Administration, Oral, Placebo, Young Adult, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Cholera, Internal medicine, medicine, Humans, 030212 general & internal medicine, Seroconversion, Adverse effect, Vibrio cholerae, General Veterinary, General Immunology and Microbiology, business.industry, Immunogenicity, Vaccination, Australia, Public Health, Environmental and Occupational Health, Cholera Vaccines, Middle Aged, medicine.disease, Antibodies, Bacterial, Healthy Volunteers, United States, Clinical trial, Infectious Diseases, Immunoglobulin G, Molecular Medicine, Female, Cholera vaccine, business

Abstract

The attenuated recombinant Vibrio cholerae O1 vaccine strain CVD 103-HgR, re-developed as PXVX0200, elicits a rapid serum vibriocidal antibody (SVA) response and protects against cholera diarrhea in volunteer challenge studies. We performed a phase 3, placebo controlled, double blind, multi-center study to further assess the safety, immunogenicity, and lot-to-lot consistency of PXVX0200. Adult volunteers 18–45 years of age were randomized 8:1 to receive a single dose of 1 × 109 CFU of PXVX0200 from three production lots or saline placebo. Immunogenicity endpoints included SVA and anti-cholera toxin (CT) antibody levels on days 1, 11, 29, 91 and 181. Safety was assessed by comparing solicited signs and symptoms on days 1–8, unsolicited adverse events through day 29 and serious adverse events through day 181. A total of 3146 participants were enrolled, including 2795 vaccine and 351 placebo recipients. The SVA seroconversion rates at day 11 were 94% and 4% in the PXVX0200 and placebo recipients, respectively (P Clinical Trials Registration: Clinicaltrials.gov NCT02094586.

Published

2018

12. Clinical development of a recombinant Ebola vaccine in the midst of an unprecedented epidemic

Author

Waterbury Julie Ann, Susan VanRheenen, Jayanthi J. Wolf, Sean P. Troth, Sheri Dubey, Swati B. Gupta, Rick Nichols, Rituparna Das, Ashley Wivel, Jeffrey T. Blue, Beth-Ann Coller, Lynn Finelli, Tracy Kemp, Kenneth Liu, D. Gray Heppner, Rebecca J. Grant-Klein, Thomas P. Monath, Frans A. Helmond, and Jakub K. Simon

Subjects

Adult, 0301 basic medicine, Zaire ebolavirus, Adolescent, Context (language use), Vaccines, Attenuated, medicine.disease_cause, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Viral Envelope Proteins, Humans, Medicine, 030212 general & internal medicine, Ebola Vaccines, Seroconversion, Child, Epidemics, Duck embryo vaccine, Clinical Trials as Topic, Vaccines, Synthetic, General Veterinary, General Immunology and Microbiology, Ebola vaccine, business.industry, Immunogenicity, Public Health, Environmental and Occupational Health, Outbreak, Vesiculovirus, Hemorrhagic Fever, Ebola, Ebolavirus, Vaccine efficacy, Virology, United States, Europe, Treatment Outcome, 030104 developmental biology, Infectious Diseases, Africa, Immunology, Molecular Medicine, business

Abstract

The 2014-2016 Ebola outbreak caused over 28,000 cases and 11,000 deaths. Merck & Co. Inc., Kenilworth, NJ USA and NewLink Genetics are working with private and public partners to develop and license an Ebola vaccine that was evaluated extensively during the outbreak. The vaccine referred to as V920 is a recombinant vesicular stomatitis virus (rVSV) in which the VSV-G envelope glycoprotein (GP) is completely replaced by the Zaire ebolavirus GP (rVSVΔG-ZEBOV-GP). Eight Phase I and four Phase II/III clinical trials enrolling approximately 17,000 subjects were conducted in parallel to the outbreak to assess the safety, immunogenicity, and/or efficacy of V920. Immunogenicity data demonstrate that anti-GP antibodies are generally detectable by ELISA by 14days postvaccination with up to 100% seroconversion observed by 28days post dose. In addition, the results of a ring vaccination trial conducted by the WHO and their partners in Guinea suggest robust vaccine efficacy within 10days of receipt of a single dose of vaccine. The vaccine is generally well-tolerated when administered to healthy, non-pregnant adults. The development of this vaccine candidate in the context of this unprecedented epidemic has involved the close cooperation of large number of international partners and highlights what we as a public health community can accomplish when working together towards a common goal. Study identification: V920-001 to V920-012. CLINICALTRIALS.GOV identifiers: NCT02269423; NCT02280408; NCT02374385; NCT02314923; NCT02287480; NCT02283099; NCT02296983; NCT02344407; NCT02378753; NCT02503202.

Published

2017

13. Safety, tolerability, and immunogenicity of inactivated trivalent seasonal influenza vaccine administered with a needle-free disposable-syringe jet injector

Author

Marcela F. Pasetti, James D. Campbell, Jakub K. Simon, Marcelo B. Sztein, Mihaela Carter, Myron M. Levine, Bruce G. Weniger, and Karen L. Kotloff

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Erythema, Influenza vaccine, Antibodies, Viral, medicine.disease_cause, Injections, Intramuscular, Gastroenterology, Influenza A Virus, H1N1 Subtype, Double-Blind Method, Internal medicine, Influenza, Human, Jet injector, medicine, Influenza A virus, Humans, Seroconversion, Adverse effect, Hemagglutination assay, General Veterinary, General Immunology and Microbiology, business.industry, Influenza A Virus, H3N2 Subtype, Immunogenicity, Public Health, Environmental and Occupational Health, Middle Aged, Influenza B virus, Infectious Diseases, Vaccines, Inactivated, Influenza Vaccines, Immunology, Injections, Jet, Molecular Medicine, Female, medicine.symptom, business

Abstract

Background Jet injectors (JIs) avoid safety drawbacks of needle–syringe (N–S) while generating similar immune responses. A new generation of disposable-syringe jet injectors (DSJIs) overcomes the cross-contamination risk of multi-use-nozzle devices used in 20th-century campaigns. In the first study in humans, the newly-US-licensed LectraJet® model M3 RA DSJI was compared to N–S. Methods Sixty healthy adults received one 0.5 mL intramuscular dose of the 2009–2010 seasonal, trivalent, inactivated influenza vaccine (TIV) in randomized, double-masked fashion by either DSJI (n = 30) or N–S (n = 30). Adverse reactions were monitored for 90 days after injection, and serologic responses assayed by hemagglutination inhibition (HI) at days 28 and 90. Results There were no related serious adverse events (SAEs), nor differing rates of unsolicited AEs between DSJI and N–S. Solicited erythema and induration occurred more often after DSJI, but were transient and well-tolerated; a trend was noted for fewer systemic reactions by DSJI. Pre-vaccination HI geometric mean titers (GMT) increased by 28 days for H1N1, H3N2, and B antigens by 13-, 14-, and 8-fold via DSJI, and by 7-, 10-, and 7-fold for N–S, respectively. No trending differences in GMT, seroconversion, or seroprotection were noted; sample sizes precluded non-inferiority assessment. Conclusions DSJI delivery of TIV is well-tolerated and immunogenic.

Published

2011

14. Antigen-specific IgA B memory cell responses to Shigella antigens elicited in volunteers immunized with live attenuated Shigella flexneri 2a oral vaccine candidates

Author

Karen L. Kotloff, Myron M. Levine, Rezwanul Wahid, Milton Maciel, Wendy L. Picking, Jakub K. Simon, E D Weld, Marcelo B. Sztein, and Marcela F. Pasetti

Subjects

Adult, Lipopolysaccharides, Immunoglobulin A, Integrins, Adolescent, Immunology, B-Lymphocyte Subsets, Administration, Oral, Vaccines, Attenuated, medicine.disease_cause, Article, Shigella flexneri, Microbiology, Feces, Young Adult, Immune system, Blood serum, Bacterial Proteins, Shigella Vaccines, Antigen, Antigens, CD, Immunity, medicine, Humans, Immunology and Allergy, Shigella, Lymphocyte Count, Antigens, Immunity, Mucosal, Sequence Deletion, biology, Vaccination, Middle Aged, biology.organism_classification, Immunoglobulin G, Antibody Formation, Humoral immunity, Leukocytes, Mononuclear, biology.protein

Abstract

We studied the induction of antigen-specific IgA memory B cells (B(M)) in volunteers who received live attenuated Shigella flexneri 2a vaccines. Subjects ingested a single oral dose of 10(7), 10(8) or 10(9) CFU of S. flexneri 2a with deletions in guaBA (CVD 1204) or in guaBA, set and sen (CVD 1208). Antigen-specific serum and stool antibody responses to LPS and Ipa B were measured on days 0, 7, 14, 28 and 42. IgA B(M) cells specific to LPS, Ipa B and total IgA were assessed on days 0 and 28. We show the induction of significant LPS-specific IgA B(M) cells in anti-LPS IgA seroresponders. Positive correlations were found between anti-LPS IgA B(M) cells and anti-LPS IgA in serum and stool; IgA B(M) cell responses to IpaB were also observed. These B(M) cell responses are likely play an important role in modulating the magnitude and longevity of the humoral response.

Published

2011

15. Antigen-specific B memory cell responses to lipopolysaccharide (LPS) and invasion plasmid antigen (Ipa) B elicited in volunteers vaccinated with live-attenuated Shigella flexneri 2a vaccine candidates

Author

Myron M. Levine, Milton Maciel, Karen L. Kotloff, Jakub K. Simon, Wendy L. Picking, Rezwanul Wahid, and Marcelo B. Sztein

Subjects

Adult, Lipopolysaccharides, Male, Volunteers, Shigellosis, Adolescent, Lipopolysaccharide, Administration, Oral, Vaccines, Attenuated, medicine.disease_cause, Article, Shigella flexneri, Microbiology, Young Adult, chemistry.chemical_compound, Immune system, Antigen, Antibody Specificity, medicine, Humans, Shigella, Dysentery, Bacillary, Antigens, Bacterial, B-Lymphocytes, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, Middle Aged, medicine.disease, biology.organism_classification, Antibodies, Bacterial, Bacterial vaccine, Vaccination, Infectious Diseases, chemistry, Bacterial Vaccines, Immunology, Molecular Medicine, Female, Immunization, Immunologic Memory, Plasmids

Abstract

We evaluated B memory responses in healthy adult volunteers who received one oral dose of live-attenuated Shigella flexneri 2a vaccine. LPS-specific B(M) cells increased from a median of 0 at baseline to 20 spot forming cells (SFC)/10(6) expanded cells following vaccination (p=0.008). A strong correlation was found between post-vaccination anti-LPS B(M) cell counts and peak serum anti-LPS IgG titers (rs=0.95, p=0.0003). Increases in B(M) specific for IpaB approaching significance were also observed. In sum, oral vaccination with live-attenuated S. flexneri 2a elicits B(M) cells to LPS and IpaB, suggesting that B(M) responses to Shigella antigens should be further studied as a suitable surrogate of protection in shigellosis.

Published

2009

16. Gut-Homing Conventional Plasmablasts and CD27− Plasmablasts Elicited after a Short Time of Exposure to an Oral Live-Attenuated Shigella Vaccine Candidate in Humans

Author

Franklin R. Toapanta, Jakub K. Simon, Eileen M. Barry, Marcela F. Pasetti, Myron M. Levine, Karen L. Kotloff, and Marcelo B. Sztein

Subjects

lcsh:Immunologic diseases. Allergy, Population, Immunology, chemical and pharmacologic phenomena, plasmablasts, CD38, CXCR3, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunology and Allergy, Medicine, Shigella vaccine, education, 030304 developmental biology, Original Research, 0303 health sciences, education.field_of_study, B cells, Attenuated vaccine, business.industry, ELISPOT, 3. Good health, Shigella, homing, business, lcsh:RC581-607, oral vaccine, 030215 immunology, Homing (hematopoietic)

Abstract

Currently, there is no licensed Shigella vaccine; however, various promising live-attenuated vaccine candidates have emerged, including CVD1208S (ΔguaBA, Δset, Δsen S. flexneri 2a), which was shown to be safe and immunogenic in Phase 1 clinical trials. Here, we report the immune responses elicited in an outpatient Phase 2 clinical trial in which subjects were vaccinated with CVD 1208S. Oral immunization with CVD 1208S elicited high anti-S. flexneri 2a LPS and IpaB antibody responses as well as an acute plasmablast (PB) infiltration in peripheral blood 7 days after immunization. PB sorted based on their expression of homing molecules confirmed that cells expressing integrin α4β7 alone or in combination with CD62L were responsible for antibody production (as measured by ELISpot). Furthermore, using high-color flow-cytometry, on day 7 after immunization, we observed the appearance of conventional PB (CPB, CD19(dim) CD20(-) CD27(+high) CD38(+high) CD3(-)), as well as a PB population that did not express CD27 (CD27(-) PB; pre-plasmablasts). The pattern of individual or simultaneous expression of homing markers (integrin α4β7, CD62L, CXCR3, and CXCR4) suggested that CPB cells homed preferentially to the inflamed gut mucosa. In contrast, ~50% CD27(-) PB cells appear to home to yet to be identified peripheral lymphoid organs or were in a transition state preceding integrin α4β7 upregulation. In sum, these observations demonstrate that strong immune responses, including distinct PB subsets with the potential to home to the gut and other secondary lymphoid organs, can be elicited after a short time of exposure to a shigella oral vaccine.

Published

2014

17. A clinical study to assess the safety and immunogenicity of attenuated measles vaccine administered intranasally to healthy adults

Author

Myron M. Levine, Alma Muñoz, James D. Campbell, Jakub K. Simon, Robert Mischler, Rosanna Lagos, Marcela F. Pasetti, and Jean-François Viret

Subjects

Adult, Male, Adolescent, Immunology, Measles Vaccine, Antibodies, Viral, Vaccines, Attenuated, Measles, Double-Blind Method, Neutralization Tests, Medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Viral shedding, Administration, Intranasal, Reactogenicity, business.industry, Immunogenicity, Middle Aged, medicine.disease, Virus Shedding, Titer, Infectious disease (medical specialty), Measles virus, Nasal administration, Female, Measles vaccine, business

Abstract

Despite the availability of a safe and effective vaccine for over four decades, measles remains one of the most common infectious disease killers of children in the world. Mucosal administration of currently licensed measles vaccine has been proposed to address issues of needle safety and improve vaccine uptake.Healthy adult volunteers were randomized to receive live-attenuated monovalent measles virus vaccine (Moraten Berna) via the standard subcutaneous (SQ) or the experimental intranasal (IN) route in a randomized, double-masked fashion. Safety, reactogenicity, immunogenicity, and shedding were assessed.Safety, reactogenicity, and viral shedding were not significantly different in the two study groups. Immunogenicity was markedly lower in the group of volunteers that received vaccine via the IN route. Plaque reduction neutralization (PRN) geometric mean titers (GMT) were 125 (95% confidence interval [CI] 68-228) milli International Units per milliliter (mIU/mL) on day 28 in recipients of IN vaccine versus 645 (95% CI 468-889) mIU/mL in recipients of vaccine SQ; p0.001 by Mann-Whitney Rank Sum. 50% of measles non-immune individuals mounted titers above the protective threshold of PRN 200 mIU/mL after IN administration versus 100% of volunteers who received the vaccine SQ.Intranasal administration of live-attenuated measles vaccine was safe and well tolerated, but failed to mount significant immune responses when compared to subcutaneous administration. It is possible that higher doses or smaller particle size are necessary for successful intranasal measles vaccination and boosting.

Published

2007

18. Intramedullary abscess of the spinal cord in children: a case report and review of the literature.

Author

JAKUB K. SIMON, JORGE A. LAZAREFF, MICHAEL J. DIAMENT, and WILLIAM A. KENNEDY

Published

2003

19. Immune responses to O-specific polysaccharide (OSP) in North American adults infected with Vibrio cholerae O1 Inaba.

Author

Motaher Hossain, Kamrul Islam, Meagan Kelly, Leslie M Mayo Smith, Richelle C Charles, Ana A Weil, Taufiqur Rahman Bhuiyan, Pavol Kováč, Peng Xu, Stephen B Calderwood, Jakub K Simon, Wilbur H Chen, Michael Lock, Caroline E Lyon, Beth D Kirkpatrick, Mitchell Cohen, Myron M Levine, Marc Gurwith, Daniel T Leung, Andrew S Azman, Jason B Harris, Firdausi Qadri, and Edward T Ryan

Subjects

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

Abstract

BackgroundAntibodies targeting O-specific polysaccharide (OSP) of Vibrio cholerae may protect against cholera; however, little is known about this immune response in infected immunologically naïve humans.MethodologyWe measured serum anti-OSP antibodies in adult North American volunteers experimentally infected with V. cholerae O1 Inaba El Tor N16961. We also measured vibriocidal and anti-cholera toxin B subunit (CtxB) antibodies and compared responses to those in matched cholera patients in Dhaka, Bangladesh, an area endemic for cholera.Principal findingsWe found prominent anti-OSP antibody responses following initial cholera infection: these responses were largely IgM and IgA, and highest to infecting serotype with significant cross-serotype reactivity. The anti-OSP responses peaked 10 days after infection and remained elevated over baseline for ≥ 6 months, correlated with vibriocidal responses, and may have been blunted in blood group O individuals (IgA anti-OSP). We found significant differences in immune responses between naïve and endemic zone cohorts, presumably reflecting previous exposure in the latter.ConclusionsOur results define immune responses to O-specific polysaccharide in immunologically naive humans with cholera, find that they are largely IgM and IgA, may be blunted in blood group O individuals, and differ in a number of significant ways from responses in previously humans. These differences may explain in part varying degrees of protective efficacy afforded by cholera vaccination between these two populations.Trial registration numberClinicalTrials.gov NCT01895855.

Published

2019

20. Anti-O-specific polysaccharide (OSP) immune responses following vaccination with oral cholera vaccine CVD 103-HgR correlate with protection against cholera after infection with wild-type Vibrio cholerae O1 El Tor Inaba in North American volunteers.

Author

Kamrul Islam, Motaher Hossain, Meagan Kelly, Leslie M Mayo Smith, Richelle C Charles, Taufiqur Rahman Bhuiyan, Pavol Kováč, Peng Xu, Regina C LaRocque, Stephen B Calderwood, Jakub K Simon, Wilbur H Chen, Douglas Haney, Michael Lock, Caroline E Lyon, Beth D Kirkpatrick, Mitchell Cohen, Myron M Levine, Marc Gurwith, Jason B Harris, Firdausi Qadri, and Edward T Ryan

Subjects

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

Abstract

BACKGROUND:Cholera is an acute voluminous dehydrating diarrheal disease caused by toxigenic strains of Vibrio cholerae O1 and occasionally O139. A growing body of evidence indicates that immune responses targeting the O-specific polysaccharide (OSP) of V. cholerae are involved in mediating protection against cholera. We therefore assessed whether antibody responses against OSP occur after vaccination with live attenuated oral cholera vaccine CVD 103-HgR, and whether such responses correlate with protection against cholera. METHODOLOGY:We assessed adult North American volunteers (n = 46) who were vaccinated with 5 × 108 colony-forming units (CFU) of oral cholera vaccine CVD 103-HgR and then orally challenged with approximately 1 × 105 CFU of wild-type V. cholerae O1 El Tor Inaba strain N16961, either 10 or 90 days post-vaccination. PRINCIPAL FINDINGS:Vaccination was associated with induction of significant serum IgM and IgA anti-OSP and vibriocidal antibody responses within 10 days of vaccination. There was significant correlation between anti-OSP and vibriocidal antibody responses. IgM and IgA anti-OSP responses on day 10 following vaccination were associated with lower post-challenge stool volume (r = -0.44, P = 0.002; r = -0.36, P = 0.01; respectively), and none of 27 vaccinees who developed a ≥1.5 fold increase in any antibody isotype targeting OSP on day 10 following vaccination compared to baseline developed moderate or severe cholera following experimental challenge, while 5 of 19 who did not develop such anti-OSP responses did (P = 0.01). CONCLUSION:Oral vaccination with live attenuated cholera vaccine CVD 103-HgR induces antibodies that target V. cholerae OSP, and these anti-OSP responses correlate with protection against diarrhea following experimental challenge with V. cholerae O1. TRIAL REGISTRATION:ClinicalTrials.gov NCT01895855.

Published

2018

21. Correction: A clinically parameterized mathematical model of Shigella immunity to inform vaccine design.

Author

Courtney L Davis, Rezwanul Wahid, Franklin R Toapanta, Jakub K Simon, and Marcelo B Sztein

Subjects

Medicine, Science

Abstract

[This corrects the article DOI: 10.1371/journal.pone.0189571.].

Published

2018

22. A clinically parameterized mathematical model of Shigella immunity to inform vaccine design.

Author

Courtney L Davis, Rezwanul Wahid, Franklin R Toapanta, Jakub K Simon, and Marcelo B Sztein

Subjects

Medicine, Science

Abstract

We refine and clinically parameterize a mathematical model of the humoral immune response against Shigella, a diarrheal bacteria that infects 80-165 million people and kills an estimated 600,000 people worldwide each year. Using Latin hypercube sampling and Monte Carlo simulations for parameter estimation, we fit our model to human immune data from two Shigella EcSf2a-2 vaccine trials and a rechallenge study in which antibody and B-cell responses against Shigella's lipopolysaccharide (LPS) and O-membrane proteins (OMP) were recorded. The clinically grounded model is used to mathematically investigate which key immune mechanisms and bacterial targets confer immunity against Shigella and to predict which humoral immune components should be elicited to create a protective vaccine against Shigella. The model offers insight into why the EcSf2a-2 vaccine had low efficacy and demonstrates that at a group level a humoral immune response induced by EcSf2a-2 vaccine or wild-type challenge against Shigella's LPS or OMP does not appear sufficient for protection. That is, the model predicts an uncontrolled infection of gut epithelial cells that is present across all best-fit model parameterizations when fit to EcSf2a-2 vaccine or wild-type challenge data. Using sensitivity analysis, we explore which model parameter values must be altered to prevent the destructive epithelial invasion by Shigella bacteria and identify four key parameter groups as potential vaccine targets or immune correlates: 1) the rate that Shigella migrates into the lamina propria or epithelium, 2) the rate that memory B cells (BM) differentiate into antibody-secreting cells (ASC), 3) the rate at which antibodies are produced by activated ASC, and 4) the Shigella-specific BM carrying capacity. This paper underscores the need for a multifaceted approach in ongoing efforts to design an effective Shigella vaccine.

Published

2018

23. Applying mathematical tools to accelerate vaccine development: modeling Shigella immune dynamics.

Author

Courtney L Davis, Rezwanul Wahid, Franklin R Toapanta, Jakub K Simon, Marcelo B Sztein, and Doron Levy

Subjects

Medicine, Science

Abstract

We establish a mathematical framework for studying immune interactions with Shigella, a bacteria that kills over one million people worldwide every year. The long-term goal of this novel approach is to inform Shigella vaccine design by elucidating which immune components and bacterial targets are crucial for establishing Shigella immunity. Our delay differential equation model focuses on antibody and B cell responses directed against antigens like lipopolysaccharide in Shigella's outer membrane. We find that antibody-based vaccines targeting only surface antigens cannot elicit sufficient immunity for protection. Additional boosting prior to infection would require a four-orders-of-magnitude increase in antibodies to sufficiently prevent epithelial invasion. However, boosting anti-LPS B memory can confer protection, which suggests these cells may correlate with immunity. We see that IgA antibodies are slightly more effective per molecule than IgG, but more total IgA is required due to spatial functionality. An extension of the model reveals that targeting both LPS and epithelial entry proteins is a promising avenue to advance vaccine development. This paper underscores the importance of multifaceted immune targeting in creating an effective Shigella vaccine. It introduces mathematical models to the Shigella vaccine development effort and lays a foundation for joint theoretical/experimental/clinical approaches to Shigella vaccine design.

Published

2013