Your search keyword '"Neutralizing"' showing total 16 results

1. Development of an IgG-Fc fusion COVID-19 subunit vaccine, AKS-452.

Author

Alleva, David, Delpero, Andrea, Scully, Melanie, Murikipudi, Sylaja, Ragupathy, Ramya, Greaves, Emma, Sathiyaseelan, Thillainaygam, Haworth, Jeffrey, Shah, Nishit, Rao, Vidhya, Nagre, Shashikant, Lancaster, Thomas, Webb, Sarah, Jasa, Allison, Ronca, Shannon, Green, Freedom, Elyard, Hanne, Yee, JoAnn, Klein, Jeffrey, Karnes, Larry, Sollie, Frans, and Zion, Todd

Subjects

COVID-19, Coronavirus, Fc-fusion, Infectious disease, Pandemic, Prophylaxis, Animals, Antibodies, Neutralizing, Antibodies, Viral, COVID-19, COVID-19 Vaccines, Immunoglobulin G, Mice, Primates, Rabbits, Recombinant Fusion Proteins, SARS-CoV-2, Spike Glycoprotein, Coronavirus, Vaccines, Subunit

Abstract

AKS-452 is a biologically-engineered vaccine comprising an Fc fusion protein of the SARS-CoV-2 viral spike protein receptor binding domain antigen (Ag) and human IgG1 Fc (SP/RBD-Fc) in clinical development for the induction and augmentation of neutralizing IgG titers against SARS-CoV-2 viral infection to address the COVID-19 pandemic. The Fc moiety is designed to enhance immunogenicity by increasing uptake via Fc-receptors (FcγR) on Ag-presenting cells (APCs) and prolonging exposure due to neonatal Fc receptor (FcRn) recycling. AKS-452 induced approximately 20-fold greater neutralizing IgG titers in mice relative to those induced by SP/RBD without the Fc moiety and induced comparable long-term neutralizing titers with a single dose vs. two doses. To further enhance immunogenicity, AKS-452 was evaluated in formulations containing a panel of adjuvants in which the water-in-oil adjuvant, Montanide™ ISA 720, enhanced neutralizing IgG titers by approximately 7-fold after one and two doses in mice, including the neutralization of live SARS-CoV-2 virus infection of VERO-E6 cells. Furthermore, ISA 720-adjuvanted AKS-452 was immunogenic in rabbits and non-human primates (NHPs) and protected from infection and clinical symptoms with live SARS-CoV-2 virus in NHPs (USA-WA1/2020 viral strain) and the K18 human ACE2-trangenic (K18-huACE2-Tg) mouse (South African B.1.351 viral variant). These preclinical studies support the initiation of Phase I clinical studies with adjuvanted AKS-452 with the expectation that this room-temperature stable, Fc-fusion subunit vaccine can be rapidly and inexpensively manufactured to provide billions of doses per year especially in regions where the cold-chain is difficult to maintain.

Published

2021

2. Oral and systemic HPV antibody kinetics post-vaccination among HIV-positive and HIV-negative men

Author

Pinto, Ligia A, Wilkin, Timothy J, Kemp, Troy J, Abrahamsen, Martha, Isaacs-Soriano, Kimberly, Pan, Yuanji, Webster-Cyriaque, Jennifer, Palefsky, Joel M, and Giuliano, Anna R

Subjects

Biomedical and Clinical Sciences, Immunology, HPV and/or Cervical Cancer Vaccines, Dental/Oral and Craniofacial Disease, Vaccine Related (AIDS), Prevention, Infectious Diseases, Immunization, Cancer, HIV/AIDS, Vaccine Related, Biotechnology, Sexually Transmitted Infections, Prevention of disease and conditions, and promotion of well-being, 3.4 Vaccines, Infection, Good Health and Well Being, Adult, Alphapapillomavirus, Antibodies, Neutralizing, Antibodies, Viral, Antibody Affinity, HIV Infections, Human Papillomavirus Recombinant Vaccine Quadrivalent, Types 6, 11, 16, 18, Human papillomavirus 16, Human papillomavirus 18, Humans, Kinetics, Male, Middle Aged, Mouth, Papillomavirus Infections, Vaccination, Young Adult, HPV, HIV, Oral antibodies, HPV vaccine, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Biomedical and clinical sciences, Health sciences

Abstract

Duration and functional aspects of the oral and systemic antibody responses following HPV vaccination in HIV-negative (HIV-) and HIV-positive (HIV+) men are not well characterized. Oral and systemic HPV-16 and HPV-18-specific antibody levels were evaluated over 18-months of follow-up, in HIV+ and HIV- men. Sera and oral gargles from 147 HIV- men, ages 27-45 and 75 HIV+ men, ages 22-61, who received 3-doses of quadrivalent HPV vaccine were tested for HPV-16 and HPV-18 antibodies at Day 1, Month 7 (1 month post-dose 3), and Month 18 (12 months post-dose 3) and HPV avidity (Day 1, and Month 7) using L1-VLP ELISA. All individuals seroconverted, regardless of HIV-status, following 3-doses of vaccine for HPV-16 and HPV-18. Serum HPV-16 and HPV-18 antibody geometric mean levels were >2-fold lower in HIV+ compared to HIV- men at Month 7 (HPV-16: 808.5 versus 2119.8 EU/mL, and HPV-18: 285.8 versus 611.6 EU/mL, p 3 fold lower in HIV+ men, at Months 7 and 18. In contrast, levels of HPV-16 and HPV-18 antibodies after vaccination were not inferior in baseline HPV-seropositive, HIV+ men. HPV-16 and HPV-18 avidity was lower among HIV+ compared to HIV- men at Month 7 (HPV-16: 1.95 M versus 2.12 M, p = 0.027; HPV-18: 1.50 M versus 1.72 M, p

Published

2019

3. Design, display and immunogenicity of HIV1 gp120 fragment immunogens on virus-like particles.

Author

Purwar, Mansi, Pokorski, Jonathan, Singh, Pranveer, Bhattacharyya, Sanchari, Arendt, Heather, DeStefano, Joanne, La Branche, Celia, Montefiori, David, Finn, M, and Varadarajan, Raghavan

Subjects

Immune focusing, Nanoparticles, Neutralizing antibodies, Protein stability, Vaccine, Animals, Antibodies, Neutralizing, Binding Sites, CD4 Antigens, Escherichia coli, HIV Envelope Protein gp120, Nanoparticles, Protein Stability, Rabbits, Surface Plasmon Resonance

Abstract

The broadly neutralizing antibody against HIV-1, b12, binds to the CD4 binding site (CD4bs) on the outer domain (OD) of the gp120 subunit of HIV-1 Env. We have previously reported the design of an E. coli expressed fragment of HIV-1 gp120, b122a, containing about 70% of the b12 epitope with the idea of focusing the immune response to this structure. Since the b122a structure was found to be only partially folded, as assessed by circular dichroism and protease resistance, we attempted to stabilize it by the introduction of additional disulfide bonds. One such mutant, b122a1-b showed increased stability and bound b12 with 30-fold greater affinity as compared to b122a. Various b122a and OD fragment proteins were displayed on the surface of Qβ virus-like particles. Sera raised against these particles in six-month long rabbit immunization studies could neutralize Tier1 viruses across different subtypes with the best results observed with b122a1-b displayed particles. Significantly higher amounts of antibodies directed towards the CD4bs were also elicited by particles displaying b122a1-b. This study highlights the ability of fragment immunogens to focus the antibody response to the conserved CD4bs of HIV-1.

Published

2018

4. Immune correlates of protection for dengue: State of the art and research agenda

Author

Katzelnick, Leah C, Harris, Eva, Baric, Ralph, Coller, Beth-Ann, Coloma, Josefina, Crowe, James E, Cummings, Derek AT, Dean, Hansi, de Silva, Aravinda, Diamond, Michael S, Durbin, Anna, Ferguson, Neil, Gilbert, Peter B, Gordon, Aubree, Gubler, Duane J, Guy, Bruno, Halloran, M Elizabeth, Halstead, Scott, Jackson, Nicholas, Jarman, Richard, Lok, Shee-mei, Michael, Nelson L, Ooi, Eng Eong, Papadopoulos, Athanasios, Plotkin, Stanley, Precioso, Alexander R, Reiner, Robert, Rey, Felix A, Rodríguez-Barraquer, Isabel, Rothman, Alan, Schmidt, Alexander C, Screaton, Gavin, Sette, Alessandro, Simmons, Cameron, St. John, Ashley L, Sun, Wellington, Thomas, Stephen, Torresi, Joseph, Tsang, John S, Vannice, Kirsten, Whitehead, Stephen, Wilder-Smith, Annelies, and Kyu Yoon, In

Subjects

Infectious Diseases, Vector-Borne Diseases, Rare Diseases, Vaccine Related, Biodefense, Immunization, Prevention, Emerging Infectious Diseases, Prevention of disease and conditions, and promotion of well-being, 3.4 Vaccines, Infection, Good Health and Well Being, Antibodies, Neutralizing, Antibodies, Viral, Clinical Trials, Phase II as Topic, Clinical Trials, Phase III as Topic, Congresses as Topic, Dengue, Dengue Vaccines, Dengue Virus, Humans, Severe Dengue, Dengue virus, Immune correlates of protection, Immune correlates of risk, Natural infection, Vaccine, Participants in the Summit on Dengue Immune Correlates of Protection, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology

Abstract

Dengue viruses (DENV1-4) are mosquito-borne flaviviruses estimated to cause up to ∼400 million infections and ∼100 million dengue cases each year. Factors that contribute to protection from and risk of dengue and severe dengue disease have been studied extensively but are still not fully understood. Results from Phase 3 vaccine efficacy trials have recently become available for one vaccine candidate, now licensed for use in several countries, and more Phase 2 and 3 studies of additional vaccine candidates are ongoing, making these issues all the more urgent and timely. At the "Summit on Dengue Immune Correlates of Protection", held in Annecy, France, on March 8-9, 2016, dengue experts from diverse fields came together to discuss the current understanding of the immune response to and protection from DENV infection and disease, identify key unanswered questions, discuss data on immune correlates and plans for comparison of results across assays/consortia, and propose a research agenda for investigation of dengue immune correlates, all in the context of both natural infection studies and vaccine trials.

Published

2017

5. MicroRNA reduction of neuronal West Nile virus replication attenuates and affords a protective immune response in mice

Author

Brostoff, Terza, Pesavento, Patricia A, Barker, Christopher M, Kenney, Joan L, Dietrich, Elizabeth A, Duggal, Nisha K, Bosco-Lauth, Angela M, and Brault, Aaron C

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Infectious Diseases, Vector-Borne Diseases, Neurosciences, Prevention, Vaccine Related, Rare Diseases, Biotechnology, Genetics, West Nile Virus, Immunization, Biodefense, Emerging Infectious Diseases, Infection, 3' Untranslated Regions, Animals, Antibodies, Neutralizing, Antibodies, Viral, Brain, DNA Replication, Disease Models, Animal, Mice, MicroRNAs, Mutagenesis, Insertional, Neurons, Open Reading Frames, RNA Interference, Vaccines, Attenuated, Virus Replication, West Nile Fever, West Nile Virus Vaccines, West Nile virus, miRNA, Immunogenicity, WNV, Neurovirulence, Attenuation, Neuroinvasive, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Biomedical and clinical sciences, Health sciences

Abstract

West Nile virus (WNV) is an important agent of human encephalitis that has quickly become endemic across much of the United States since its identification in North America in 1999. While the majority (∼75%) of infections are subclinical, neurologic disease can occur in a subset of cases, with outcomes including permanent neurologic damage and death. Currently, there are no WNV vaccines approved for use in humans. This study introduces a novel vaccine platform for WNV to reduce viral replication in the central nervous system while maintaining peripheral replication to elicit strong neutralizing antibody titers. Vaccine candidates were engineered to incorporate microRNA (miRNA) target sequences for a cognate miRNA expressed only in neurons, allowing the host miRNAs to target viral transcription through endogenous RNA silencing. To maintain stability, these targets were incorporated in multiple locations within the 3'-untranslated region, flanking sequences essential for viral replication without affecting the viral open reading frame. All candidates replicated comparably to wild type WNV in vitro within cells that did not express the cognate miRNA. Insertional control viruses were also capable of neuroinvasion and neurovirulence in vivo in CD-1 mice. Vaccine viruses were safe at all doses tested and did not demonstrate mutations associated with a reversion to virulence when serially passaged in mice. All vaccine constructs were protective from lethal challenge in mice, producing 93-100% protection at the highest dose tested. Overall, this is a safe and effective attenuation strategy with broad potential application for vaccine development.

Published

2016

6. Proteomic assessment of humoral immune responses in smallpox vaccine recipients.

Author

Kennedy, Richard B., Ovsyannikova, Inna G., Haralambieva, Iana H., Grill, Diane E., and Poland, Gregory A.

Subjects

*SMALLPOX vaccines, *IMMUNOGLOBULINS, *VACCINE effectiveness, *PROTEOMICS, *VIRAL proteins, *MEMBRANE proteins

Abstract

The availability of effective smallpox vaccines was a critical element of the successful eradication of smallpox in 1980. Antibody responses play a primary role in protective immunity and neutralizing antibody is an established correlate of protection against smallpox. In this study we used a poxvirus proteome array to assess the antibody response to individual viral proteins in a cohort of 1,037 smallpox vaccine recipients. Several statistically significant differences were observed in the antibody response to immunodominant proteins between men and women, including B5R—a major target of neutralizing antibody in vaccinia immune globulin, and the membrane proteins D8L and A27L, both of which have been used as vaccine antigens providing protection in animal models. We also noted differences across racial/ethnic groups. In this cohort, which consisted of both ACAM2000 and Dryvax recipients, we noted minute differences in the antibody responses to a restricted number of viral proteins, providing additional support for the use of ACAM2000 as a replacement smallpox vaccine. Furthermore, our data indicate that poxvirus proteome microarrays can be valuable for screening and monitoring smallpox vaccine-induced humoral immune responses in large-scale serologic surveillance studies and prove useful in the guidance of developing novel smallpox candidate vaccines. [ABSTRACT FROM AUTHOR]

Published

2022

7. Defense-in-depth by mucosally administered anti-HIV dimeric IgA2 and systemic IgG1 mAbs: Complete protection of rhesus monkeys from mucosal SHIV challenge

Author

Sholukh, Anton M, Watkins, Jennifer D, Vyas, Hemant K, Gupta, Sandeep, Lakhashe, Samir K, Thorat, Swati, Zhou, Mingkui, Hemashettar, Girish, Bachler, Barbara C, Forthal, Donald N, Villinger, Francois, Sattentau, Quentin J, Weiss, Robin A, Agatic, Gloria, Corti, Davide, Lanzavecchia, Antonio, Heeney, Jonathan L, and Ruprecht, Ruth M

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Prevention, Vaccine Related, Vaccine Related (AIDS), Pediatric Research Initiative, HIV/AIDS, Immunization, Infectious Diseases, Infection, Good Health and Well Being, Administration, Intravenous, Administration, Mucosal, Animals, Antibodies, Monoclonal, Antibodies, Neutralizing, HIV Antibodies, HIV-1, Humans, Immunity, Cellular, Immunity, Mucosal, Immunization, Passive, Immunoglobulin A, Immunoglobulin G, Macaca mulatta, Mucous Membrane, RNA, Viral, Simian Acquired Immunodeficiency Syndrome, Simian Immunodeficiency Virus, T-Lymphocytes, IgA, IgG, Complete protection, Passive immunization, Rhesus monkey, SHIV-C mucosal challenge, Simian immunodeficiency virus, (6 max), Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Biomedical and clinical sciences, Health sciences

Abstract

Although IgA is the most abundantly produced immunoglobulin in humans, its role in preventing HIV-1 acquisition, which occurs mostly via mucosal routes, remains unclear. In our passive mucosal immunizations of rhesus macaques (RMs), the anti-HIV-1 neutralizing monoclonal antibody (nmAb) HGN194, given either as dimeric IgA1 (dIgA1) or dIgA2 intrarectally (i.r.), protected 83% or 17% of the RMs against i.r. simian-human immunodeficiency virus (SHIV) challenge, respectively. Data from the RV144 trial implied that vaccine-induced plasma IgA counteracted the protective effector mechanisms of IgG1 with the same epitope specificity. We thus hypothesized that mucosal dIgA2 might diminish the protection provided by IgG1 mAbs targeting the same epitope. To test our hypothesis, we administered HGN194 IgG1 intravenously (i.v.) either alone or combined with i.r. HGN194 dIgA2. We enrolled SHIV-exposed, persistently aviremic RMs protected by previously administered nmAbs; RM anti-human IgG responses were undetectable. However, low-level SIV Gag-specific proliferative T-cell responses were found. These animals resemble HIV-exposed, uninfected humans, in which local and systemic cellular immune responses have been observed. HGN194 IgG1 and dIgA2 used alone and the combination of the two neutralized the challenge virus equally well in vitro. All RMs given only i.v. HGN194 IgG1 became infected. In contrast, all RMs given HGN194 IgG1+dIgA2 were completely protected against high-dose i.r. SHIV-1157ipEL-p challenge. These data imply that combining suboptimal defenses at the mucosal and systemic levels can completely prevent virus acquisition. Consequently, active vaccination should focus on defense-in-depth, a strategy that seeks to build up defensive fall-back positions well behind the fortified frontline.

Published

2015

8. Endpoint and epitope-specific antibody responses as correlates of vaccine-mediated protection of mice against ricin toxin.

Author

Slyke, Greta Van, Ehrbar, Dylan J., Doering, Jennifer, Yates, Jennifer L., Vitetta, Ellen S., Donini, Oreola, and Mantis, Nicholas J.

Subjects

*ANTIBODY formation, *TOXINS, *MICE, *MONOCLONAL antibodies, *STATISTICAL power analysis

Abstract

The successful licensure of vaccines for biodefense is contingent upon the availability of well-established correlates of protection (CoP) in at least two animal species that can be applied to humans, without the need to assess efficacy in the clinic. In this report we describe a multivariate model that combines pre-challenge serum antibody endpoint titers (EPT) and values derived from an epitope profiling immune-competition capture (EPICC) assay as a predictor in mice of vaccine-mediated immunity against ricin toxin (RT), a Category B biothreat. EPICC is a modified competition ELISA in which serum samples from vaccinated mice were assessed for their ability to inhibit the capture of soluble, biotinylated (b)-RT by a panel of immobilized monoclonal antibodies (mAbs) directed against four immunodominant toxin-neutralizing regions on the enzymatic A chain (RTA) of RT. In a test cohort of mice (n = 40) vaccinated with suboptimal doses of the RTA subunit vaccine, RiVax®, we identified two mAbs, PB10 and SyH7, which had EPICC inhibition values in pre-challenge serum samples that correlated with survival following a challenge with 5 × LD 50 of RT administered by intraperitoneal (IP) injection. Analysis of a larger cohort of mice (n = 645) revealed that a multivariate model combining endpoint titers and EPICC values for PB10 and SyH7 as predictive variables had significantly higher statistical power than any one of the independent variables alone. Establishing the correlates of vaccine-mediated protection in mice represents an important steppingstone in the development of RiVax® as a medical countermeasure under the United States Food and Drug Administration's "Animal Rule." [ABSTRACT FROM AUTHOR]

Published

2020

9. Deciphering the domain specificity of C. difficile toxin neutralizing antibodies.

Author

Cole, Leah E., Li, Lu, Jetley, Utsav, Zhang, Jinrong, Pacheco, Kristl, Ma, Fuqin, Zhang, Jianxin, Mundle, Sophia, Yan, Yanhua, Barone, Lucianna, Rogers, Christopher, Beltraminelli, Nicola, Quemeneur, Laurence, Kleanthous, Harry, Anderson, Stephen F., and Anosova, Natalie G.

Subjects

*IMMUNOGLOBULINS, *TOXINS, *CLOSTRIDIOIDES difficile, *BACTERIAL toxins, *ANTIBODY formation

Abstract

Clostridium difficile infection (CDI) is the principal cause of nosocomial diarrhea and pseudomembranous colitis associated with antibiotic therapy. The pathological effects of CDI are primarily attributed to toxins A (TcdA) and B (TcdB). Adequate toxin-specific antibody responses are associated with asymptomatic carriage, whereas insufficient humoral responses are associated with recurrent CDI. While the data supporting the importance of anti-toxin antibodies are substantial, clarity about the toxin domain specificity of these antibodies is more limited. To investigate this matter, combinations of human mAbs targeting multiple domains of TcdB were assessed using toxin neutralization assays. These data revealed that a combination of mAbs specific to all major toxin domains had improved neutralizing potency when compared to equivalent concentrations of a single mAb or a combination of mAbs against one or two domains. The function and toxin domain binding specificity of serum antibodies elicited by immunization of hamsters with a toxoid vaccine candidate was also assessed. Immunization with a toxoid vaccine candidate provoked toxin neutralizing antibodies specific to multiple domains of both TcdA and TcdB. When assessed in a toxin neutralization assay, polyclonal sera displayed greater activity against elevated concentrations of toxins than equivalent concentrations of individual mAbs. These data suggest a potential benefit of any antibody based therapeutic or prophylactic treatment that targets multiple toxin domains. [ABSTRACT FROM AUTHOR]

Published

2019

10. Immunoglobulin GM and KM genes and measles vaccine-induced humoral immunity.

Author

Ovsyannikova, Inna G., Larrabee, Beth R., Schaid, Daniel J., and Poland, Gregory A.

Subjects

*THERAPEUTIC use of immunoglobulins, *MEASLES prevention, *VIRAL vaccines, *HUMORAL immunity, *GENETIC polymorphisms

Abstract

Identifying genetic polymorphisms that explain variations in humoral immunity to live measles virus vaccine is of great interest. Immunoglobulin GM (heavy chain) and KM (light chain) allotypes are genetic markers known to be associated with susceptibility to several infectious diseases. We assessed associations between GM and KM genotypes and measles vaccine humoral immunity (neutralizing antibody titers) in a combined cohort (n = 1796) of racially diverse healthy individuals (age 18–41 years). We did not discover any significant associations between GM and/or KM genotypes and measles vaccine-induced neutralizing antibody titers. African-American subjects had higher neutralizing antibody titers than Caucasians (1260 mIU/mL vs. 740 mIU/mL, p = 7.10 × 10 −13 ), and those titers remained statistically significant (p = 1.68 × 10 −09 ) after adjusting for age at enrollment and time since last vaccination. There were no statistically significant sex-specific differences in measles-induced neutralizing antibody titers in our study (p = 0.375). Our data indicate a surprising lack of evidence for an association between GM and KM genotypes and measles-specific neutralizing antibody titers, despite the importance of these immune response genes. [ABSTRACT FROM AUTHOR]

Published

2017

11. Rotavirus VP6 preparations as a non-replicating vaccine candidates.

Author

Jalilvand, Somayeh, Marashi, Sayed Mahdi, and Shoja, Zabihollah

Subjects

*ROTAVIRUS diseases, *VIRAL vaccines, *CYTOSKELETAL proteins, *IMMUNE response, *CROSS reactions (Immunology), *VACCINE research

Abstract

Rotavirus (RV) structural proteins VP4 and VP7, located on the surface of viral particles, elicit neutralizing antibodies (Abs) and are therefore considered to be important components of RV vaccines. However, despite inducing neutralizing Abs, limits of cross-neutralizing activity and lack of full correlation with protection limit the usefulness of these proteins as protective agents against RV disease. VP6 protein, which forms the middle layer of RV particles, is discussed as an alternative vaccine candidate since it can induce cross-protective immune responses against different RV strains although the Ab raised is not neutralizing. This report reviews different functions of VP6 that can lead to considering it as an alternative vaccine against RV disease. [ABSTRACT FROM AUTHOR]

Published

2015

12. Antigenic analysis of divergent genotypes human Enterovirus 71 viruses by a panel of neutralizing monoclonal antibodies: Current genotyping of EV71 does not reflect their antigenicity

Author

Chen, Yixin, Li, Chuan, He, Delei, Cheng, Tong, Ge, Shengxiang, Shih, James Wai-Kuo, Zhao, Qinjian, Chen, Pei-Jer, Zhang, Jun, and Xia, Ningshao

Subjects

*ANTIGENS, *ENTEROVIRUSES, *MONOCLONAL antibodies, *HAND, foot & mouth disease, *VIRAL vaccines, *DRUG development, *PUBLIC health

Abstract

Abstract: In recent year, Enterovirus 71 (EV71)-associated hand, foot and mouth disease (HFMD) has become an important public health issue in China. EV71 has been classified into genotypes A, B1–B5 and C1–C5. With such genetic diversity, whether the convalescent or recovery antibody responses can cross-protect infections from other genotypes remains a question. Understanding of the antigenicity of such diverse genetic EV71 isolates is crucial for the EV71 vaccine development. Here, a total of 186 clones anti-EV71 MAbs was generated and characterized with Western blot and cell-based neutralization assay. Forty neutralizing anti-EV71 MAbs were further used to analyze the antigenic properties of 18 recent EV71 isolates representing seven genotypes in neutralization assay. We found that most neutralizing anti-EV71 MAbs are specific to conformational epitopes. We also classified the 40 neutralizing anti-EV71 MAbs into two classes according to their reactivity patterns with 18 EV71 isolates. Class I MAb can neutralize all isolates, suggesting conserved epitopes are present among EV71. Class II MAb includes four subclasses (IIa–IId) and neutralizes only subgroups of EV71 strains. Conversely, 18 EV71 strains were grouped into antigenic types 1 and four antigenic subtypes (2.1–2.4). These results suggest that the current genotyping of EV71 does not reflect their antigenicity which may be important in the selection of EV71 vaccine strains. This panel of neutralizing anti-EV71 MAbs may be useful for the recognition of emerging antigenic variants of EV71 and vaccine development. [Copyright &y& Elsevier]

Published

2013

13. Protective immunity to ricin toxin conferred by antibodies against the toxin's binding subunit (RTB)

Author

Yermakova, Anastasiya and Mantis, Nicholas J.

Subjects

*RICIN, *BOTULINUM toxin, *MONOCLONAL antibodies, *ANTIBODY-toxin conjugates, *LABORATORY mice, *HYBRIDOMAS

Abstract

Abstract: The B subunit (RTB) of ricin toxin is a galactose-/N-acetyl galactosamine-specific lectin that promotes attachment and entry of ricin into host cells. RTB is also the archetype of the so-called R-type lectin family, whose members include haemagglutinins of botulinum neurotoxin (BoNT) progenitor toxins, as well as the binding subunits of cytolethal distending toxins. Although RTB is an appealing subunit vaccine candidate, as well as a potential target for immunotherapeutics, the degree to which RTB immunization elicits protective antibodies against ricin toxin remains unresolved. To address this issue, groups of mice were immunized with RTB and then challenged with 5×LD50s of ricin administered intraperitoneally. Despite high RTB-specific serum antibody titers, groups of RTB immunized mice were only partially immune to ricin challenge. Analysis of a collection of RTB-specific B cell hybridomas suggested that only a small fraction of antibodies against RTB have demonstrable neutralizing activity. Two RTB-specific neutralizing monoclonal IgG1 antibodies, 24B11 and SylH3, when passively administered to mice, were sufficient to protect the animals against a 5×LD50 dose of ricin. Both 24B11 and SylH3 blocked ricin attachment to terminal galactose residues and prevented toxin binding to the surfaces of bone marrow-derived macrophages (BMM), suggesting that they function by steric hindrance and recognize epitopes located on RTB''s carbohydrate recognition sub-domains (1α or 2γ). These data raise the possibility of using specific RTB sub-domains, rather than RTB itself, as antigens to more efficiently elicit neutralizing antibodies and protective immunity against ricin. [Copyright &y& Elsevier]

Published

2011

14. Intradermal vaccination with un-adjuvanted sub-unit vaccines triggers skin innate immunity and confers protective respiratory immunity in domestic swine

Author

Florence Boudet, Bertrand Dubois, Jean-Benoît Le Luduec, Philippe Emile Fernand Laurent, Fabienne Piras, Sabine Debeer, Christine Andreoni, Dominique Kaiserlian, Mucosal Immunity, Vaccination, and Biometrics -- Immunité des muqueuses, vaccinations et biothérapies, Centre International de Recherche en Infectiologie (CIRI), École normale supérieure de Lyon (ENS de Lyon)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Université Jean Monnet - Saint-Étienne (UJM)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-École normale supérieure de Lyon (ENS de Lyon)-Université Claude Bernard Lyon 1 (UCBL), Université de Lyon-Université de Lyon-Université Jean Monnet - Saint-Étienne (UJM)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Sanofi Pasteur [Marcy-l'Étoile, France], Mérial [Lyon], Mérial, and BD Medical – Pharmaceutical Systems [Le Pont de Claix, France]

Subjects

0301 basic medicine, Swine, medicine.medical_treatment, Antibodies, Viral, Monocytes, 0302 clinical medicine, Viral Envelope Proteins, Immunologic, Innate, Viral, Neutralizing, Skin, Vaccines, Immunity, Cellular, Viral Vaccine, Vaccination, Humoral, Respiratory infection, Infectious Diseases, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, Vaccines, Subunit, [SDV.IMM]Life Sciences [q-bio]/Immunology, Cytokines, Molecular Medicine, Female, Adjuvant, Subunit, Injections, Intradermal, Biology, Antibodies, Injections, 03 medical and health sciences, Immune system, Adjuvants, Immunologic, Immunity, Intradermal, medicine, Anti-viral immunity, Animals, Adjuvants, Pseudorabies, Innate immune system, General Veterinary, General Immunology and Microbiology, Public Health, Environmental and Occupational Health, Viral Vaccines, Dendritic Cells, [SDV.MP.BAC]Life Sciences [q-bio]/Microbiology and Parasitology/Bacteriology, Antibodies, Neutralizing, Virology, Immunity, Innate, Immunity, Humoral, Intradermal vaccination, 030104 developmental biology, Immunization, Immunology, Cellular, 030215 immunology

Abstract

International audience; Intradermal (ID) vaccination constitutes a promising approach to induce anti-infectious immunity. This route of immunization has mostly been studied with influenza split-virion vaccines. However, the efficacy of ID vaccination for sub-unit vaccines in relation to underlying skin innate immunity remains to be explored for wider application in humans. Relevant animal models that more closely mimic human skin immunity than the widely used mouse models are therefore necessary. Here, we show in domestic swine, which shares striking anatomic and functional properties with human skin, that a single ID delivery of pseudorabies virus (PRV) glycoproteins without added adjuvant is sufficient to trigger adaptive cellular and humoral immune responses, and to confer protection from a lethal respiratory infection with PRV. Analysis of early events at the skin injection site revealed up-regulation of pro-inflammatory cytokine and chemokine genes, recruitment of neutrophils and monocytes and accumulation of inflammatory DC. We further show that the sustained induction of pro-inflammatory cytokine genes results from the combined effects of skin puncture, liquid injection in the dermis and viral antigens. These data highlight that immune protection against respiratory infection can be induced by ID vaccination with a subunit vaccine and reveal that adjuvant requirements are circumvented by the mechanical and antigenic stress caused by ID injection, which triggers innate immunity and mobilization of inflammatory DC at the immunization site. ID vaccination with sub-unit vaccines may thus represent a safe and efficient solution for protection against respiratory infections in swine and possibly also in humans, given the similarity of skin structure and function in both species.

Published

2016

15. Defense-in-depth by mucosally administered anti-HIV dimeric IgA2 and systemic IgG1 mAbs: Complete protection of rhesus monkeys from mucosal SHIV challenge

Author

Robin A. Weiss, Donald N. Forthal, Jennifer D. Watkins, Antonio Lanzavecchia, Ruth M. Ruprecht, Samir K. Lakhashe, Barbara C. Bachler, Mingkui Zhou, Girish Hemashettar, Francois Villinger, Anton M Sholukh, Sandeep Gupta, Davide Corti, Swati Thorat, Quentin J. Sattentau, Gloria Agatic, Jonathan L. Heeney, Hemant K. Vyas, Heeney, Jonathan [0000-0003-2702-1621], and Apollo - University of Cambridge Repository

Subjects

T-Lymphocytes, Simian Acquired Immunodeficiency Syndrome, (6 max), HIV Antibodies, Passive, Medical and Health Sciences, Epitope, Monoclonal, Administration, Mucosal, Viral, SHIV-C mucosal challenge, Neutralizing, Immunity, Cellular, Mucosal, Effector, Simian immunodeficiency virus, Antibodies, Monoclonal, Biological Sciences, Vaccination, Infectious Diseases, Administration, RNA, Viral, HIV/AIDS, Molecular Medicine, Administration, Intravenous, Simian Immunodeficiency Virus, Antibody, Intravenous, Infection, IgA, Pediatric Research Initiative, IgG, medicine.drug_class, Biology, Monoclonal antibody, Article, Antibodies, Virus, Vaccine Related, Immune system, Virology, Immunology and Microbiology(all), medicine, Animals, Humans, Complete protection, Vaccine Related (AIDS), Immunity, Mucosal, Mucous Membrane, Agricultural and Veterinary Sciences, General Veterinary, General Immunology and Microbiology, Prevention, Passive immunization, Immunization, Passive, Immunity, Public Health, Environmental and Occupational Health, Antibodies, Neutralizing, Macaca mulatta, veterinary(all), In vitro, Immunoglobulin A, Good Health and Well Being, Immunoglobulin G, Immunology, HIV-1, Rhesus monkey, biology.protein, RNA, Immunization, Cellular

Abstract

Although IgA is the most abundantly produced immunoglobulin in humans, its role in preventing HIV-1 acquisition, which occurs mostly via mucosal routes, remains unclear. In our passive mucosal immunizations of rhesus macaques (RMs), the anti-HIV-1 neutralizing monoclonal antibody (nmAb) HGN194, given either as dimeric IgA1 (dIgA1) or dIgA2 intrarectally (i.r.), protected 83% or 17% of the RMs against i.r. simian-human immunodeficiency virus (SHIV) challenge, respectively. Data from the RV144 trial implied that vaccine-induced plasma IgA counteracted the protective effector mechanisms of IgG1 with the same epitope specificity. We thus hypothesized that mucosal dIgA2 might diminish the protection provided by IgG1 mAbs targeting the same epitope. To test our hypothesis, we administered HGN194 IgG1 intravenously (i.v.) either alone or combined with i.r. HGN194 dIgA2. We enrolled SHIV-exposed, persistently aviremic RMs protected by previously administered nmAbs; RM anti-human IgG responses were undetectable. However, low-level SIV Gag-specific proliferative T-cell responses were found. These animals resemble HIV-exposed, uninfected humans, in which local and systemic cellular immune responses have been observed. HGN194 IgG1 and dIgA2 used alone and the combination of the two neutralized the challenge virus equally well in vitro. All RMs given only i.v. HGN194 IgG1 became infected. In contrast, all RMs given HGN194 IgG1 + dIgA2 were completely protected against high-dose i.r. SHIV-1157ipEL-p challenge. These data imply that combining suboptimal defenses at the mucosal and systemic levels can completely prevent virus acquisition. Consequently, active vaccination should focus on defense-in-depth, a strategy that seeks to build up defensive fall-back positions well behind the fortified frontline.

Published

2015

16. Neutralizing and cross-neutralizing antibody titres induced by bivalent and quadrivalent human papillomavirus vaccines in the target population of organized vaccination programmes

Author

Giorgia Marcati, Luisa Barzon, Laura Squarzon, Monia Pacenti, Liliana Gabrielli, Serena Masiero, Tiziana Lazzarotto, Antonella Caputo, Maria Grazia Pascucci, Barbara Mantelli, Giorgio Palù, Barzon, Luisa, Squarzon, Laura, Masiero, Serena, Pacenti, Monia, Marcati, Giorgia, Mantelli, Barbara, Gabrielli, Liliana, Pascucci, Maria Grazia, Lazzarotto, Tiziana, Caputo, Antonella, and Palù, Giorgio

Subjects

Cross-neutralizing antibody, Immunology and Microbiology (all), Cross Protection, HPV31, Antibodies, Viral, Human Papillomavirus Recombinant Vaccine Quadrivalent, Human Papillomavirus Recombinant Vaccine Quadrivalent, Types 6, 11, 16, 18, Medicine, Viral, Neutralizing antibody, Child, Neutralizing, Papillomavirus Vaccine, Bivalent HPV vaccine, Human papillomavirus 16, biology, Human papillomavirus 18, Immunization Program, Vaccination, Titer, Infectious Diseases, Veterinary (all), Molecular Medicine, Female, Public Health, Neutralization Test, Antibody, Human, medicine.drug, HPV16, Cervical cancer prevention, Adolescent, HPV18, Quadrivalent HPV vaccine, Infectious Disease, HPV vaccines, Antibodies, NO, Pseudovirion, Neutralization Tests, Humans, Papillomavirus Vaccines, Papillomavirus Infection, General Veterinary, General Immunology and Microbiology, Pseudovirion-based neutralization assay, business.industry, Immunization Programs, Gardasil, Environmental and Occupational Health, Papillomavirus Infections, Public Health, Environmental and Occupational Health, HPV45, Virology, Antibodies, Neutralizing, Immunology, Types 6, biology.protein, Cervarix, business

Abstract

Aim of this investigator-initiated study was to evaluate and compare the titres of neutralizing and cross-neutralizing antibodies (NAbs) induced by the bivalent (Cervarix(®)) and quadrivalent (Gardasil(®)) HPV vaccines in a cohort of girls aged 11-13 years from organized vaccination programmes. To this aim, HPV16 and HPV18 NAbs were measured by pseudovirion-based neutralization assays in serum collected at 1-6 months after the third vaccine dose in 107 girls vaccinated with Cervarix(®) and 126 vaccinated with Gardasil(®), while HPV31 and HPV45 cross-NAbs were tested in the first 50 consecutive girls of both vaccine groups. The results of this study demonstrated that all vaccinated girls developed HPV16 and HPV18 NAbs, with the exception of two Gardasil(®) vaccinees with undetectable HPV18 NAbs. Geometric mean titres (GMTs) of both HPV16 and HPV18 NAbs were significantly higher in Cervarix(®) than in Gardasil(®) vaccinees [HPV16 NAb GMT 22,136 (95% CI, 18,811-26,073) vs 5092 (4230-6151), respectively; P

Published

2014