Your search keyword '"Georgia D Tomaras"' showing total 462 results

101. Subclass and avidity of circumsporozoite protein specific antibodies associate with protection status against malaria infection

Author

Erik Jongert, Richard H. C. Huntwork, S. Munir Alam, Milite Abraha, Sheetij Dutta, S. Moses Dennison, Rachel L. Spreng, Matthew Reichartz, Sarah V. Mudrak, Fernando Ulloa-Montoya, Georgia D. Tomaras, Michelle Rojas, Scott Gregory, Ulrike Wille-Reece, Margherita Coccia, Kelly E. Seaton, and Frederick Feely

Subjects

Pharmacology, Malaria vaccine, Immunology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Plasmodium falciparum, Biology, RC581-607, medicine.disease, biology.organism_classification, Vaccine efficacy, Subclass, Article, Malaria, Circumsporozoite protein, parasitic diseases, medicine, biology.protein, Infectious diseases, Pharmacology (medical), Avidity, Antibody, Immunologic diseases. Allergy, RC254-282

Abstract

RTS,S/AS01 is an advanced pre-erythrocytic malaria vaccine candidate with demonstrated vaccine efficacy up to 86.7% in controlled human malaria infection (CHMI) studies; however, reproducible immune correlates of protection (CoP) are elusive. To identify candidates of humoral correlates of vaccine mediated protection, we measured antibody magnitude, subclass, and avidity for Plasmodium falciparum (Pf) circumsporozoite protein (CSP) by multiplex assays in two CHMI studies with varying RTS,S/AS01B vaccine dose and timing regimens. Central repeat (NANP6) IgG1 magnitude correlated best with protection status in univariate analyses and was the most predictive for protection in a multivariate model. NANP6 IgG3 magnitude, CSP IgG1 magnitude, and total serum antibody dissociation phase area-under-the-curve for NANP6, CSP, NPNA3, and N-interface binding were also associated with protection status in the regimen adjusted univariate analysis. Identification of multiple immune response features that associate with protection status, such as antibody subclasses, fine specificity and avidity reported here may accelerate development of highly efficacious vaccines against P. falciparum.

Published

2021

102. SIMON: Open-Source Knowledge Discovery Platform

Author

Adriana Tomic, Ross D. Pollock, Max Kuhn, Ivan Tomic, Mark M. Davis, Stephen D. R. Harridge, Andrew J. Pollard, Ludwig Geistlinger, Jennifer Hill, Lindsay C. Dahora, Kelly E. Seaton, Norman R. Lazarus, Purvesh Khatri, Rachel L. Spreng, Levi Waldron, Georgia D. Tomaras, Niharika A. Duggal, and Janet M. Lord

Subjects

Systems biology, General Decision Sciences, 03 medical and health sciences, computational biology, 0302 clinical medicine, Software, Resource (project management), autoML, Knowledge extraction, Biomedical data, Statistical analysis, 030304 developmental biology, Graphical user interface, lcsh:Computer software, 0303 health sciences, software, business.industry, systems biology, Descriptor, data mining, bioinformatics, Modular design, artificial intelligence, Data science, 3. Good health, lcsh:QA76.75-76.765, machine learning, Open source, 030220 oncology & carcinogenesis, data science, business

Abstract

Summary Data analysis and knowledge discovery has become more and more important in biology and medicine with the increasing complexity of biological datasets, but the necessarily sophisticated programming skills and in-depth understanding of algorithms needed pose barriers to most biologists and clinicians to perform such research. We have developed a modular open-source software, SIMON, to facilitate the application of 180+ state-of-the-art machine-learning algorithms to high-dimensional biomedical data. With an easy-to-use graphical user interface, standardized pipelines, and automated approach for machine learning and other statistical analysis methods, SIMON helps to identify optimal algorithms and provides a resource that empowers non-technical and technical researchers to identify crucial patterns in biomedical data., Graphical Abstract, Highlights • SIMON is an open-source software for analysis of high-dimensional biomedical data • SIMON facilitates application of 180+ machine learning algorithms • Easy-to-use graphical use interface and no programming expertise required • SIMON empowers biomedical researchers to identify patterns in biomedical data, The Bigger Picture Over the past years, technological advances have enabled the generation of large amounts of data at multiple scales. The integration of high-dimensional data is particularly important in biomedical sciences, as they can be used to identify biological mechanisms and predict clinical outcomes well in advance of their occurrence. Because of the lack of powerful analytical tools that can be used by the average biomedical researcher, translation of such knowledge has been extremely slow. We have developed an open-source software, SIMON, to facilitate the application of machine learning to high-dimensional biomedical data. In SIMON, analysis is performed using an intuitive graphical user interface and standardized, automated machine learning approach allowing non-technical researchers to identify patterns and extract knowledge from high-dimensional data and build high-quality predictive models., Tomic et al. developed SIMON, an open-source software for application of machine learning algorithms to high-dimensional biomedical data ranging from the transcriptome to flow cytometry to the microbiome. Using a graphical user interface, standardized pipelines for predictive modeling, and automated machine learning, SIMON empowers non-technical biomedical researchers to identify patterns in their data and build high-quality predictive models.

Published

2021

103. Anti-V2 antibodies virus vulnerability revealed by envelope V1 deletion in HIV vaccine candidates

Author

Isabela Silva de Castro, Genoveffa Franchini, Rosemarie D. Mason, Dominic Paquin-Proulx, Timothy Cardozo, Margaret H. Beddall, Giacomo Gorini, Sarkis Sarkis, Celia C. LaBranche, Mohammad Arif Rahman, Michael Read, Josh Kramer, Margherita Rosati, Raffaello Verardi, Claudia Cicala, James Arthos, Matthew Breed, Richard Nguyen, Marina Tuyishime, Brandon F. Keele, Jennifer Peele, Mangala Rao, Mohammed S. Ahmadi, Stephen Whitney, Irene Kalisz, Jason Gorman, Guido Ferrari, Francesca Caccuri, Manuel Becerra-Flores, Michael A. Eller, George N. Pavlakis, Dai Fujikawa, Veronica Galli, Melvin N. Doster, Massimiliano Bissa, Georgia D. Tomaras, Susie Min, Zhanna Shubin, Barbara K. Felber, Hung V. Trinh, Anush Arakelyan, Donald Van Ryk, David Venzon, David C. Montefiori, Namal P.M. Liyanage, Juliane P. Hill, William Magnanelli, Eric Ni, Luca Schifanella, Marjorie Robert-Guroff, Kristina K. Peachman, Peter D. Kwong, Leonid Margolis, Mei Hue Liu, Mario Roederer, James D. Stamos, Monica Vaccari, and Xiaoying Shen

Subjects

0301 basic medicine, Immunology, Human immunodeficiency virus (HIV), Beta sheet, Peptide, molecular structure, 02 engineering and technology, medicine.disease_cause, Virus, α4β7 integrin, Article, 03 medical and health sciences, medicine, HIV vaccine, lcsh:Science, Receptor, Cytotoxicity, Antibody-dependent cell-mediated cytotoxicity, chemistry.chemical_classification, Multidisciplinary, biology, virus diseases, 021001 nanoscience & nanotechnology, Virology, virology, 030104 developmental biology, chemistry, biology.protein, lcsh:Q, Antibody, 0210 nano-technology

Abstract

Summary The efficacy of ALVAC-based HIV and SIV vaccines in humans and macaques correlates with antibodies to envelope variable region 2 (V2). We show here that vaccine-induced antibodies to SIV variable region 1 (V1) inhibit anti-V2 antibody-mediated cytotoxicity and reverse their ability to block V2 peptide interaction with the α4β7 integrin. SIV vaccines engineered to delete V1 and favor an α helix, rather than a β sheet V2 conformation, induced V2-specific ADCC correlating with decreased risk of SIV acquisition. Removal of V1 from the HIV-1 clade A/E A244 envelope resulted in decreased binding to antibodies recognizing V2 in the β sheet conformation. Thus, deletion of V1 in HIV envelope immunogens may improve antibody responses to V2 virus vulnerability sites and increase the efficacy of HIV vaccine candidates., Graphical Abstract, Highlights • HIV vaccine candidate protects against SIVmac251 acquisition • V1 deleted envelope immunogens with V2 in α-helical conformation are protective • V2-specific ADCC as correlate of risk • Anti-V1 antibodies interfere with V2-specific ADCC, Immunology; molecular structure; virology

Published

2021

104. Lipid nanoparticle encapsulated nucleoside-modified mRNA vaccines elicit polyfunctional HIV-1 antibodies comparable to proteins in nonhuman primates

Author

Kevin O. Saunders, Norbert Pardi, Robert Parks, Sampa Santra, Zekun Mu, Laura Sutherland, Richard Scearce, Maggie Barr, Amanda Eaton, Giovanna Hernandez, Derrick Goodman, Michael J. Hogan, Istvan Tombacz, David N. Gordon, R. Wes Rountree, Yunfei Wang, Mark G. Lewis, Theodore C. Pierson, Chris Barbosa, Ying Tam, Gary R. Matyas, Mangala Rao, Zoltan Beck, Xiaoying Shen, Guido Ferrari, Georgia D. Tomaras, David C. Montefiori, Drew Weissman, and Barton F. Haynes

Subjects

0301 basic medicine, Protein vaccines, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Immunology, Human immunodeficiency virus (HIV), Biology, medicine.disease_cause, Antibodies, Article, law.invention, 03 medical and health sciences, 0302 clinical medicine, Vaccine Immunogenicity, RNA vaccines, law, medicine, Pharmacology (medical), RC254-282, Pharmacology, Vaccines, Messenger RNA, Critical question, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, virus diseases, RC581-607, Virology, 030104 developmental biology, Infectious Diseases, Immunization, 030220 oncology & carcinogenesis, Recombinant DNA, biology.protein, Immunologic diseases. Allergy, Antibody, Nucleoside

Abstract

Development of an effective AIDS vaccine remains a challenge. Nucleoside-modified mRNAs formulated in lipid nanoparticles (mRNA-LNP) have proved to be a potent mode of immunization against infectious diseases in preclinical studies, and are being tested for SARS-CoV-2 in humans. A critical question is how mRNA-LNP vaccine immunogenicity compares to that of traditional adjuvanted protein vaccines in primates. Here, we found that mRNA-LNP immunization compared to protein immunization elicited either the same or superior magnitude and breadth of HIV-1 Env-specific polyfunctional antibodies. Immunization with mRNA-LNP encoding Zika premembrane and envelope (prM-E) or HIV-1 Env gp160 induced durable neutralizing antibodies for at least 41 weeks. Doses of mRNA-LNP as low as 5 μg were immunogenic in macaques. Thus, mRNA-LNP can be used to rapidly generate single or multi-component vaccines, such as sequential vaccines needed to protect against HIV-1 infection. Such vaccines would be as or more immunogenic than adjuvanted recombinant protein vaccines in primates.

Published

2020

105. Magnitude, Specificity, and Avidity of Sporozoite-Specific Antibodies Associate With Protection Status and Distinguish Among RTS,S/AS01 Dose Regimens

Author

Milite Abraha, S. Moses Dennison, Rachel L. Spreng, Georgia D. Tomaras, S. Munir Alam, Ulrike Wille-Reece, Sheetij Dutta, Erik Jongert, and Matthew Reichartz

Subjects

0301 basic medicine, biology, business.industry, RTS,S, 03 medical and health sciences, Specific antibody, 030104 developmental biology, 0302 clinical medicine, Infectious Diseases, Oncology, parasitic diseases, Immunology, biology.protein, Medicine, Avidity, Antibody, business, 030217 neurology & neurosurgery

Abstract

Background The malaria vaccine, RTS,S/AS01, demonstrated an enhanced efficacy (86.7%) in a delayed third fractional dose (0.1.7Fx) regimen in controlled human malaria infection trials compared with a standard full-dose (0.1.2) regimen (62.5%). To understand the humoral component of the RTS,S/AS01 vaccine-induced protection against sporozoite infection in these 2 regimens, we investigated the serum antibody dynamics of 0.1.2 and 0.1.7Fx groups vaccinees. Methods The specific binding responses (magnitude) and dissociation rates (avidity) of serum antibodies interaction with a recombinant Plasmodium falciparum circumsporozoite protein (CSP) and peptides corresponding to the central repeat region (NANP6), the C-terminal region (PF16), and the N-terminal junction (N-interface) of CSP, respectively, were measured using a Biolayer Interferometry assay. Results On the day of challenge, higher NANP6-specific antibody responses were associated with protection in the 0.1.2 group. In contrast, slower antibody dissociation rates for CSP and PF16 binding were observed in the protected 0.1.7Fx group. Protected vaccinees of both groups exhibited 2- to 3-fold higher N-interface peptide binding antibody responses. Conclusions Unlike the standard dose, the delayed-fractional third dose of RTS,S/AS01 induced higher avidity CSP and PF16 binding antibodies that were associated with protection against sporozoite infection.

Published

2020

106. Rectal tissue and vaginal tissue from intravenous VRC01 recipients show protection against ex vivo HIV-1 challenge

Author

Yunda Huang, Yiwen Lu, Lamar Ballweber Fleming, Christina Ochsenbauer, Julie Czartoski, Sandeep Narpala, Madhu Prabhakaran, Kelly E. Seaton, Lily Zhang, John Hural, Kenneth H. Mayer, Scott M. Hammer, Lindsey R. Baden, Rena D. Astronomo, Maria P. Lemos, Georgia D. Tomaras, Katharine Westerberg, M. Juliana McElrath, Mary K Gross, Ian Frank, Hong Van Tieu, Adrian B. McDermott, Nicole Grunenberg, and Julie E. Ledgerwood

Subjects

Adult, Male, Allergy, medicine.drug_class, HIV Infections, HIV Antibodies, In Vitro Techniques, Monoclonal antibody, Andrology, Young Adult, Pharmacokinetics, In vivo, medicine, Distribution (pharmacology), Humans, Infusions, Intravenous, Mucous Membrane, business.industry, Rectum, Antibodies, Monoclonal, General Medicine, Middle Aged, medicine.disease, Vagina, HIV-1, Female, Clinical Medicine, business, Infiltration (medical), Ex vivo, Broadly Neutralizing Antibodies, Explant culture

Abstract

BACKGROUND: VRC01, a potent, broadly neutralizing monoclonal antibody, inhibits simian-HIV infection in animal models. The HVTN 104 study assessed the safety and pharmacokinetics of VRC01 in humans. We extend the clinical evaluation to determine intravenously infused VRC01 distribution and protective function at mucosal sites of HIV-1 entry. METHODS: Healthy, HIV-1–uninfected men (n = 7) and women (n = 5) receiving VRC01 every 2 months provided mucosal and serum samples once, 4–13 days after infusion. Eleven male and 8 female HIV-seronegative volunteers provided untreated control samples. VRC01 levels were measured in serum, secretions, and tissue, and HIV-1 inhibition was determined in tissue explants. RESULTS: Median VRC01 levels were quantifiable in serum (96.2 μg/mL or 1.3 pg/ng protein), rectal tissue (0.11 pg/ng protein), rectal secretions (0.13 pg/ng protein), vaginal tissue (0.1 pg/ng protein), and cervical secretions (0.44 pg/ng protein) from all recipients. VRC01/IgG ratios in male serum correlated with those in paired rectal tissue (r = 0.893, P = 0.012) and rectal secretions (r = 0.9643, P = 0.003). Ex vivo HIV-1(Bal26) challenge infected 4 of 21 rectal explants from VRC01 recipients versus 20 of 22 from controls (P = 0.005); HIV-1(Du422.1) infected 20 of 21 rectal explants from VRC01 recipients and 12 of 12 from controls (P = 0.639). HIV-1(Bal26) infected 0 of 14 vaginal explants of VRC01 recipients compared with 23 of 28 control explants (P = 0.003). CONCLUSION: Intravenous VRC01 distributes into the female genital and male rectal mucosa and retains anti–HIV-1 functionality, inhibiting a highly neutralization-sensitive but not a highly resistant HIV-1 strain in mucosal tissue. These findings lend insight into VRC01 mucosal infiltration and provide perspective on in vivo protective efficacy. FUNDING: National Institute of Allergy and Infectious Diseases and Bill & Melinda Gates Foundation.

Published

2020

107. Vi-specific serological correlates of protection for typhoid fever

Author

Lindsay C. Dahora, Rachel L. Spreng, Georgia D. Tomaras, Jennifer Hill, Elizabeth Jones, M Johnson, J K Fallon, S.M. Alam, Kelly E. Seaton, Bronwyn M. Gunn, A Nebykova, Andrew J. Pollard, Yu W-H., Galit Alter, S.M. Dennison, Malick M. Gibani, Helene B Juel, and Celina Jin

Subjects

Adult, 0301 basic medicine, Time Factors, genetic structures, Immunology, chemical and pharmacologic phenomena, Salmonella typhi, Article, Typhoid fever, Immunoglobulin G, Serology, Infectious Disease and Host Defense, 03 medical and health sciences, fluids and secretions, Immunogenicity, Vaccine, 0302 clinical medicine, medicine, Humans, Immunology and Allergy, Avidity, 030212 general & internal medicine, Typhoid Fever, 11 Medical and Health Sciences, Vaccines, Conjugate, biology, business.industry, Typhoid-Paratyphoid Vaccines, Toxoid, medicine.disease, eye diseases, Bacterial Load, Immunity, Humoral, Vaccination, 030104 developmental biology, biology.protein, sense organs, Antibody, business

Abstract

Distinct protective humoral signatures are induced by Vi-conjugate and Vi-polysaccharide vaccines. Shared humoral features across both vaccines suggest that protection against typhoid fever is mediated through a combination of qualitative features of the polyclonal humoral response (avidity and innate immune cell functional responses) in addition to antibody quantity., Typhoid Vi vaccines have been shown to be efficacious in children living in endemic regions; however, a widely accepted correlate of protection remains to be established. We applied a systems serology approach to identify Vi-specific serological correlates of protection using samples obtained from participants enrolled in an experimental controlled human infection study. Participants were vaccinated with Vi-tetanus toxoid conjugate (Vi-TT) or unconjugated Vi-polysaccharide (Vi-PS) vaccines and were subsequently challenged with Salmonella Typhi bacteria. Multivariate analyses identified distinct protective signatures for Vi-TT and Vi-PS vaccines in addition to shared features that predicted protection across both groups. Vi IgA quantity and avidity correlated with protection from S. Typhi infection, whereas higher fold increases in Vi IgG responses were associated with reduced disease severity. Targeted antibody-mediated functional responses, particularly neutrophil phagocytosis, were also identified as important components of the protective signature. These humoral markers could be used to evaluate and develop efficacious Vi-conjugate vaccines and assist with accelerating vaccine availability to typhoid-endemic regions.

Published

2020

108. Structure-guided changes at the V2 apex of HIV-1 clade C trimer enhance elicitation of autologous neutralizing and broad V1V2-scaffold antibodies

Author

Anusmita Sahoo, Edgar A. Hodge, Celia C. LaBranche, Tiffany M. Styles, Xiaoying Shen, Narayanaiah Cheedarla, Ayalnesh Shiferaw, Gabriel Ozorowski, Wen-Hsin Lee, Andrew B. Ward, Georgia D. Tomaras, David C. Montefiori, Darrell J. Irvine, Kelly K. Lee, and Rama Rao Amara

Subjects

AIDS Vaccines, HIV Antigens, HIV Seropositivity, HIV-1, env Gene Products, Human Immunodeficiency Virus, Animals, HIV Infections, Rabbits, HIV Antibodies, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology

Abstract

HIV-1 clade C envelope immunogens that elicit both neutralizing and non-neutralizing V1V2-scaffold-specific antibodies (protective correlates from RV144 human trial) are urgently needed due to the prevalence of this clade in the most impacted regions worldwide. To achieve this, we introduce structure-guided changes followed by consensus-C-sequence-guided optimizations at the V2 region to generate UFO-v2-RQH

Published

2022

109. Innate immune signatures to a partially-efficacious HIV vaccine predict correlates of HIV-1 infection risk

Author

Lamar Ballweber Fleming, Craig Innes, Valentin Voillet, Lindsay N. Carpp, Anneta F Naidoo, M. Juliana McElrath, Peter B. Gilbert, Glenda Gray, Guido Ferrari, Nicole Grunenberg, Linda-Gail Bekker, Fatima Laher, Georgia D. Tomaras, Erica Andersen-Nissen, James G. Kublin, Ying Huang, Andrew Fiore-Gartland, and Michael S. Harper

Subjects

CD4-Positive T-Lymphocytes, HIV Antigens, Physiology, Gene Expression, Antibody Response, HIV Infections, HIV Antibodies, Biochemistry, White Blood Cells, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine, Public and Occupational Health, Biology (General), HIV vaccine, Immune Response, AIDS Vaccines, 0303 health sciences, Vaccines, Innate Immune System, Immune System Proteins, biology, T Cells, Vaccination and Immunization, medicine.anatomical_structure, Infectious diseases, Cytokines, Antibody, Cellular Types, Research Article, Risk, Medical conditions, QH301-705.5, T cell, Immune Cells, Immunology, Microbiology, Antibodies, 03 medical and health sciences, Immune system, Immunity, Virology, Infectious disease control, Vaccine Development, Genetics, Humans, Molecular Biology, 030304 developmental biology, Medicine and health sciences, Innate immune system, Blood Cells, Biology and life sciences, business.industry, Viral vaccines, Antibody-Dependent Cell Cytotoxicity, HIV vaccines, Proteins, Cell Biology, RC581-607, Molecular Development, Vaccine efficacy, Antibodies, Neutralizing, Immunity, Innate, Immunization, Immune System, biology.protein, HIV-1, Leukocytes, Mononuclear, Parasitology, Preventive Medicine, Immunologic diseases. Allergy, business, 030217 neurology & neurosurgery, Developmental Biology

Abstract

The pox-protein regimen tested in the RV144 trial is the only vaccine strategy demonstrated to prevent HIV-1 infection. Subsequent analyses identified antibody and cellular immune responses as correlates of risk (CoRs) for HIV infection. Early predictors of these CoRs could provide insight into vaccine-induced protection and guide efforts to enhance vaccine efficacy. Using specimens from a phase 1b trial of the RV144 regimen in HIV-1-uninfected South Africans (HVTN 097), we profiled innate responses to the first ALVAC-HIV immunization. PBMC transcriptional responses peaked 1 day post-vaccination. Type I and II interferon signaling pathways were activated, as were innate pathways critical for adaptive immune priming. We then identified two innate immune transcriptional signatures strongly associated with adaptive immune CoR after completion of the 4-dose regimen. Day 1 signatures were positively associated with antibody-dependent cellular cytotoxicity and phagocytosis activity at Month 6.5. Conversely, a signature present on Days 3 and 7 was inversely associated with Env-specific CD4+ T cell responses at Months 6.5 and 12; rapid resolution of this signature was associated with higher Env-specific CD4+ T-cell responses. These are the first-reported early immune biomarkers of vaccine-induced responses associated with HIV-1 acquisition risk in humans and suggest hypotheses to improve HIV-1 vaccine regimens., Author summary The innate immune response is the body’s initial defense against pathogens and is linked to and shapes the subsequent adaptive immune response, which can confer long-lasting protection. For a vaccine with partial efficacy, such as the RV144 HIV vaccine regimen, identifying early innate responses that are linked with adaptive responses—particularly those for which evidence has accumulated that they might be important for protection—could help a more efficacious version be developed. In the HVTN 097 study, the RV144 prime-boost (ALVAC-HIV and AIDSVAX B/E) vaccine regimen was given to South African participants. We characterized the innate response to the first dose of ALVAC-HIV in these participants and identified gene expression signatures present within the first few days that were associated with antibody and T-cell responses to the full vaccine regimen measured up to 1 year later. As these antibody and T-cell responses have previously been implicated in protection, our findings suggest ways of refining the RV144 regimen and also have broader applications to vaccine development.

Published

2020

110. RhCMV serostatus and vaccine adjuvant impact immunogenicity of RhCMV/SIV vaccines

Author

Ellen E. Sparger, Peter A. Barry, Hung T. Kieu, Luis D. Castillo, Dennis J. Hartigan-O'Connor, Xiaoying Shen, Barbara L. Shacklett, Jesse D. Deere, W. L. William Chang, Georgia D. Tomaras, and Kawthar Machmach

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, and promotion of well-being, animal diseases, viruses, Cytomegalovirus, lcsh:Medicine, CD8-Positive T-Lymphocytes, medicine.disease_cause, Antibodies, Viral, 0302 clinical medicine, Immunologic, Medicine, Innate, Viral, lcsh:Science, Vaccines, Multidisciplinary, Immunogenicity, Simian immunodeficiency virus, virus diseases, Viral Load, Vaccination, Infectious Diseases, 3.4 Vaccines, HIV/AIDS, Infectious diseases, Simian Immunodeficiency Virus, Infection, Viral load, Biotechnology, gag, Gene Products, gag, Viremia, Antibodies, Article, Vaccine Related, 03 medical and health sciences, Interferon-gamma, Immune system, Adjuvants, Immunologic, Immunity, Gene Products, Animals, Humans, Adjuvants, Vaccine Related (AIDS), business.industry, Prevention, lcsh:R, Viral Vaccines, Vaccine efficacy, medicine.disease, Prevention of disease and conditions, Virology, Macaca mulatta, Immunity, Innate, 030104 developmental biology, Good Health and Well Being, Immunization, lcsh:Q, business, 030217 neurology & neurosurgery

Abstract

Rhesus cytomegalovirus (RhCMV) strain 68-1-vectored simian immunodeficiency virus (RhCMV/SIV) vaccines are associated with complete clearance of pathogenic SIV challenge virus, non-canonical major histocompatibility complex restriction, and absent antibody responses in recipients previously infected with wild-type RhCMV. This report presents the first investigation of RhCMV/SIV vaccines in RhCMV-seronegative macaques lacking anti-vector immunity. Fifty percent of rhesus macaques (RM) vaccinated with a combined RhCMV-Gag, -Env, and -Retanef (RTN) vaccine controlled pathogenic SIV challenge despite high peak viremia. However, kinetics of viral load control by vaccinated RM were considerably delayed compared to previous reports. Impact of a TLR5 agonist (flagellin; FliC) on vaccine efficacy and immunogenicity was also examined. An altered vaccine regimen containing an SIV Gag-FliC fusion antigen instead of Gag was significantly less immunogenic and resulted in reduced protection. Notably, RhCMV-Gag and RhCMV-Env vaccines elicited anti-Gag and anti-Env antibodies in RhCMV-seronegative RM, an unexpected contrast to vaccination of RhCMV-seropositive RM. These findings confirm that RhCMV-vectored SIV vaccines significantly protect against SIV pathogenesis. However, pre-existing vector immunity and a pro-inflammatory vaccine adjuvant may influence RhCMV/SIV vaccine immunogenicity and efficacy. Future investigation of the impact of pre-existing anti-vector immune responses on protective immunity conferred by this vaccine platform is warranted.

Published

2020

111. Impact of vaccine type on HIV-1 vaccine elicited antibody durability and B cell gene signature

Author

Fatima Laher, James J. Kobie, Juilee Thakar, Michael S. Piepenbrink, Harriet L. Robinson, Glenda Gray, Susan Buchbinder, Michael C. Keefer, Yunda Huang, Kelly E. Seaton, John Hural, Gavin J. Churchyard, Georgia D. Tomaras, Holly Janes, Paul A. Goepfert, and Rohith Palli

Subjects

Modified vaccinia Ankara, Protein vaccines, Immunization, Secondary, lcsh:Medicine, Receptors, Antigen, B-Cell, HIV Infections, Vaccinia virus, HIV Antibodies, Lymphocyte Activation, CD19, Article, Antibodies, DNA vaccines, medicine, Humans, Adjuvants, lcsh:Science, B cell, AIDS Vaccines, B-Lymphocytes, Clinical Trials as Topic, Multidisciplinary, CD40, biology, business.industry, Gene Expression Profiling, lcsh:R, Vaccination, Gene signature, Regulatory networks, medicine.anatomical_structure, HIV Antigens, Gene Expression Regulation, Immunology, Antibody Formation, biology.protein, HIV-1, Linear Models, lcsh:Q, Antibody, business, Half-Life, Signal Transduction

Abstract

Efficacious HIV-1 vaccination requires elicitation of long-lived antibody responses. However, our understanding of how different vaccine types elicit durable antibody responses is lacking. To assess the impact of vaccine type on antibody responses, we measured IgG isotypes against four consensus HIV antigens from 2 weeks to 10 years post HIV-1 vaccination and used mixed effects models to estimate half-life of responses in four human clinical trials. Compared to protein-boosted regimens, half-lives of gp120-specific antibodies were longer but peak magnitudes were lower in Modified Vaccinia Ankara (MVA)-boosted regimens. Furthermore, gp120-specific B cell transcriptomics from MVA-boosted and protein-boosted vaccines revealed a distinct signature at a peak (2 weeks after last vaccination) including CD19, CD40, and FCRL2-5 activation along with increased B cell receptor signaling. Additional analysis revealed contributions of RIG-I-like receptor pathway and genes such as SMAD5 and IL-32 to antibody durability. Thus, this study provides novel insights into vaccine induced antibody durability and B-cell receptor signaling.

Published

2020

112. Co-immunization of DNA and Protein in the Same Anatomical Sites Induces Superior Protective Immune Responses against SHIV Challenge

Author

Sherry Stanfield-Oakley, Wes Rountree, Guido Ferrari, George M. Shaw, Margaret E. Ackerman, Christopher A.L. Remmel, Steven G. Reed, Georgia D. Tomaras, Yunfei Wang, Zhongyan Lu, Barton F. Haynes, Nathan Vandergrift, Faith Schiro, Galit Alter, Margherita Rosati, Hung V. Trinh, Celia C. LaBranche, Katelyn Faircloth, Mangala Rao, Xiaoying Shen, Ronald S. Veazey, Wilton B. Williams, Munir Alam, David Venzon, Xintao Hu, Kevin O. Saunders, Bapi Pahar, George N. Pavlakis, Jason Dufour, Preston A. Marx, Pyone P. Aye, Joshua A. Weiner, Jishnu Das, Antonio Valentin, Margaret C. Carpenter, Barbara K. Felber, and David C. Montefiori

Subjects

0301 basic medicine, Cellular immunity, viruses, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Immune system, Animals, Humans, HIV vaccine, Antibody-dependent cell-mediated cytotoxicity, biology, Immunogenicity, virus diseases, Proteins, DNA, Virology, 030104 developmental biology, chemistry, Humoral immunity, biology.protein, Macaca, Immunization, Simian Immunodeficiency Virus, Antibody, 030217 neurology & neurosurgery

Abstract

Summary We compare immunogenicity and protective efficacy of an HIV vaccine comprised of env and gag DNA and Env (Envelope) proteins by co-administration of the vaccine components in the same muscles or by separate administration of DNA + protein in contralateral sites in female rhesus macaques. The 6-valent vaccine includes gp145 Env DNAs, representing six sequentially isolated Envs from the HIV-infected individual CH505, and matching GLA-SE-adjuvanted gp120 Env proteins. Interestingly, only macaques in the co-administration vaccine group are protected against SHIV CH505 acquisition after repeated low-dose intravaginal challenge and show 67% risk reduction per exposure. Macaques in the co-administration group develop higher Env-specific humoral and cellular immune responses. Non-neutralizing Env antibodies, ADCC, and antibodies binding to FcγRIIIa are associated with decreased transmission risk. These data suggest that simultaneous recognition, processing, and presentation of DNA + Env protein in the same draining lymph nodes play a critical role in the development of protective immunity.

Published

2020

113. A phase 1b randomized study of the safety and immunological responses to vaccination with H4:IC31, H56:IC31, and BCG revaccination in Mycobacterium tuberculosis-uninfected adolescents in Cape Town, South Africa

Author

Anthony Williams, Georgia D. Tomaras, Andrew Fiore-Gartland, One B. Dintwe, Kathryn Tucker Rutkowski, Aeras A Protocol Team, Peter Andersen, Keren Middelkoop, Hvtn, Kelly E. Seaton, M. Juliana McElrath, Linda-Gail Bekker, Erica Andersen-Nissen, James G. Kublin, Ann M. Ginsberg, Dereck Tait, Stephen C. De Rosa, Ingrid Kromann, Julia Hutter, Carlos A. DiazGranados, April K. Randhawa, Morten Ruhwald, and Maurine D. Miner

Subjects

Research paper, Tuberculosis, 01 natural sciences, QuantiFERON, Mycobacterium tuberculosis, 03 medical and health sciences, 0302 clinical medicine, Antigen, Medicine, BCG, 030212 general & internal medicine, H56:IC31, 0101 mathematics, lcsh:R5-920, biology, business.industry, Immunogenicity, 010102 general mathematics, General Medicine, Vaccine efficacy, medicine.disease, biology.organism_classification, Vaccination, Immunology, biology.protein, Antibody, business, lcsh:Medicine (General), H4:IC31

Abstract

Background: Tuberculosis (TB) remains the leading cause of infectious disease-related death. Recently, a trial of BCG revaccination and vaccination with H4:IC31, a recombinant protein vaccine, in South African adolescents (Aeras C-040-404) showed efficacy in preventing sustained QuantiFERON (QFT) conversion, a proxy for Mycobacterium tuberculosis (M.tb) infection. A phase 1b trial of 84 South African adolescents was conducted, concurrent with Aeras C-040-404, to assess the safety and immunogenicity of H4:IC31, H56:IC31 and BCG revaccination, and to identify and optimize immune assays for identification of candidate correlates of protection in efficacy trials. Methods: Two doses of H4:IC31 and H56:IC31 vaccines were administered intramuscularly (IM) 56 days apart, and a single dose of BCG (2–8 × 105 CFU) was administered intradermally (ID). T-cell and antibody responses were measured using intracellular cytokine staining and binding antibody assays, respectively. Binding antibodies and CD4+/CD8+ T-cell responses to H4- and H56-matched antigens were measured in samples from all participants. The study was designed to characterize safety and immunogenicity and was not powered for group comparisons. (Clinicaltrials.gov NCT02378207). Findings: In total, 481 adolescents (mean age 13·9 years) were screened; 84 were enrolled (54% female). The vaccines were generally safe and well-tolerated, with no reported severe adverse events related to the study vaccines. H4:IC31 and H56:IC31 elicited CD4+ T cells recognizing vaccine-matched antigens and H4- and H56-specific IgG binding antibodies. The highest vaccine-induced CD4+ T-cell response rates were for those recognizing Ag85B in the H4:IC31 and H56:IC31 vaccinated groups. BCG revaccination elicited robust, polyfunctional BCG-specific CD4+ T cells, with no increase in H4- or H56-specific IgG binding antibodies. There were few antigen-specific CD8+ T-cell responses detected in any group. Interpretation: BCG revaccination administered as a single dose ID and both H4:IC31 and H56:IC31 administered as 2 doses IM had acceptable safety profiles in healthy, QFT-negative, previously BCG-vaccinated adolescents. Characterization of the assays and the immunogenicity of these vaccines may help to identify valuable markers of protection for upcoming immune correlates analyses of C-040-404 and future TB vaccine efficacy trials. Funding: NIAID and Aeras. Keywords: Mycobacterium tuberculosis, H4:IC31, H56:IC31, BCG

Published

2020

114. Impact of T h 1 CD4 Follicular Helper T Cell Skewing on Antibody Responses to an HIV-1 Vaccine in Rhesus Macaques

Author

Korey A. Walter, Hung V. Trinh, Celia C. LaBranche, Sonny R. Elizaldi, Yashavanth Shaan Lakshmanappa, Donald N. Forthal, Nancy Nguyen, Smita S. Iyer, Ashok Reddy Dinasarapu, Brian A. Schmidt, Keith A. Reimann, Rama Rao Amara, Gary R. Matyas, Pamela A. Kozlowski, Zoltan Beck, Mangala Rao, David H. Foehl, Niharika N. Rane, Georgia D. Tomaras, Johannes S. Gach, Xiaoying Shen, and Anil Verma

Subjects

0303 health sciences, biology, medicine.medical_treatment, T cell, Immunology, Antibody titer, Germinal center, Microbiology, Vaccination, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Virology, Insect Science, medicine, biology.protein, Avidity, Antibody, Adjuvant, B cell, 030304 developmental biology, 030215 immunology

Abstract

Generating durable humoral immunity through vaccination depends upon effective interactions of follicular helper T (Tfh) cells with germinal center (GC) B cells. Th1 polarization of Tfh cells is an important process shaping the success of Tfh-GC B cell interactions by influencing costimulatory and cytokine-dependent Tfh help to B cells. However, the question remains as to whether adjuvant-dependent modulation of Tfh cells enhances HIV-1 vaccine-induced antienvelope (anti-Env) antibody responses. We investigated whether an HIV-1 vaccine platform designed to increase the number of Th1-polarized Tfh cells enhances the magnitude and quality of anti-Env antibodies. Utilizing a novel interferon-induced protein 10 (IP-10)-adjuvanted HIV-1 DNA prime followed by a monophosphoryl lipid A and QS-21 (MPLA+QS-21)-adjuvanted Env protein boost (DIP-10 PALFQ) in macaques, we observed higher anti-Env serum IgG titers with greater cross-clade reactivity, specificity for V1V2, and effector functions than in macaques primed with DNA lacking IP-10 and boosted with MPLA-plus-alum-adjuvanted Env protein (DPALFA) The DIP-10 PALFQ vaccine regimen elicited higher anti-Env IgG1 and lower IgG4 antibody levels in serum, showing for the first time that adjuvants can dramatically impact the IgG subclass profile in macaques. The DIP-10 PALFQ regimen also increased vaginal and rectal IgA antibodies to a greater extent. Within lymph nodes, we observed augmented GC B cell responses and the promotion of Th1 gene expression profiles in GC Tfh cells. The frequency of GC Tfh cells correlated with both the magnitude and avidity of anti-Env serum IgG. Together, these data suggest that adjuvant-induced stimulation of Th1-Tfh cells is an effective strategy for enhancing the magnitude and quality of anti-Env antibody responses.IMPORTANCE The results of the RV144 trial demonstrated that vaccination could prevent HIV transmission in humans and that longevity of anti-Env antibodies may be key to this protection. Efforts to improve upon the prime-boost vaccine regimen used in RV144 have indicated that booster immunizations can increase serum anti-Env antibody titers but only transiently. Poor antibody durability hampers efforts to develop an effective HIV-1 vaccine. This study was designed to identify the specific elements involved in the immunological mechanism necessary to produce robust HIV-1-specific antibodies in rhesus macaques. By clearly defining immune-mediated pathways that improve the magnitude and functionality of the anti-HIV-1 antibody response, we will have the foundation necessary for the rational development of an HIV-1 vaccine.

Published

2020

115. Effect of HIV Envelope Vaccination on the Subsequent Antibody Response to HIV Infection

Author

Carolyn Williamson, Kenneth H. Mayer, Glenda Gray, Zoe Moodie, Koleka Mlisana, Nonhlanhla N. Mkhize, Shelly Karuna, Linda-Gail Bekker, Penny L. Moore, Peter B. Gilbert, Gavin J. Churchyard, Georgia D. Tomaras, Cecilia Morgan, Michael Yin, David C. Montefiori, Michael C. Keefer, Lynn Morris, and Zanele Ditse

Subjects

Male, 0301 basic medicine, HIV breakthrough infections, lcsh:QR1-502, HIV Infections, HIV Antibodies, lcsh:Microbiology, Neutralization, 0302 clinical medicine, Medicine, Neutralizing antibody, AIDS Vaccines, biology, env Gene Products, Human Immunodeficiency Virus, virus diseases, Middle Aged, Viral Load, QR1-502, HIV Envelope Protein gp41, rAd5, 3. Good health, Vaccination, 030220 oncology & carcinogenesis, Female, Antibody, Research Article, Adult, Enzyme-Linked Immunosorbent Assay, Gp41, Microbiology, Virus, Young Adult, 03 medical and health sciences, Immune system, Antigen, Neutralization Tests, Humans, HIV-specific binding antibodies, Molecular Biology, business.industry, broadly neutralizing antibodies, HIV vaccines, Therapeutics and Prevention, Antibodies, Neutralizing, Virology, HIV-1 envelope, binding antibody epitopes, 030104 developmental biology, Antibody Formation, HIV-1, biology.protein, DNA/MVA vaccines, business

Abstract

There is a wealth of information on HIV-specific vaccine-induced immune responses among HIV-uninfected participants; however, data on immune responses among participants who acquire HIV after vaccination are limited. Here we show that HIV-specific binding antibody responses in individuals with breakthrough HIV infections were not affected by prior vaccination with HIV envelope-containing immunogens. We also found that these vectored vaccines did not prime tier 2 virus-neutralizing antibody responses, which are thought to be required for prevention against HIV acquisition, or accelerate the development of neutralization breadth. Although this study is limited, such studies can provide insights into whether vaccine-elicited antibody responses are boosted by HIV infection to acquire broader neutralizing activity, which may help to identify antigens relevant to the design of more effective vaccines., Analysis of breakthrough HIV-1 infections could elucidate whether prior vaccination primes relevant immune responses. Here, we measured HIV-specific antibody responses in 14 South African volunteers who acquired HIV infection after participating in phase 1/2 trials of envelope-containing immunogens. Serum samples were collected annually following HIV-1 infection from participants in trials HVTN 073 (subtype C, DNA/MVA, phase 1 trial, n = 1), HVTN 086 (subtype C, DNA/MVA/gp140 protein, phase 1 trial, n = 2), and HVTN 204 (multisubtype, DNA/adenovirus serotype 5 [Ad5], phase 2 trial, n = 7) and 4 placebo recipients. Binding and neutralizing antibody responses to Env proteins and peptides were determined pre- and post-HIV infection using an enzyme-linked immunosorbent assay and the TZM-bl cell neutralization assay, respectively. HIV-infected South African individuals served as unvaccinated controls. Binding antibodies to gp41, V3, V2, the membrane-proximal external region (MPER), and the CD4 binding site were detected from the first year of HIV-1 subtype C infection, and the levels were similar in vaccinated and placebo recipients. Neutralizing antibody responses against tier 1A viruses were detected in all participants, with the highest titers being to a subtype C virus, MW965.26. No responses were observed just prior to infection, indicating that vaccine-primed HIV-specific antibodies had waned. Sporadic neutralization activity against tier 2 isolates was observed after 2 to 3 years of HIV infection, but these responses were similar in the vaccinated and placebo groups as well as the unvaccinated controls. Our data suggest that prior vaccination with these immunogens did not alter the antibody responses to HIV-1 infection, nor did it accelerate the development of HIV neutralization breadth. IMPORTANCE There is a wealth of information on HIV-specific vaccine-induced immune responses among HIV-uninfected participants; however, data on immune responses among participants who acquire HIV after vaccination are limited. Here we show that HIV-specific binding antibody responses in individuals with breakthrough HIV infections were not affected by prior vaccination with HIV envelope-containing immunogens. We also found that these vectored vaccines did not prime tier 2 virus-neutralizing antibody responses, which are thought to be required for prevention against HIV acquisition, or accelerate the development of neutralization breadth. Although this study is limited, such studies can provide insights into whether vaccine-elicited antibody responses are boosted by HIV infection to acquire broader neutralizing activity, which may help to identify antigens relevant to the design of more effective vaccines.

Published

2020

116. Robust antibody and cellular responses induced by DNA-only vaccination for HIV

Author

David B. Weiner, Yiwen Lu, Michael Pensiero, Matthew P. Morrow, Mark L. Bagarazzi, Niranjan Y. Sardesai, Yunda Huang, Georgia D. Tomaras, Megan C. Wise, Marnie Elizaga, Edith Swann, Xue Han, Lawrence Corey, Srilatha Edupuganti, Scott R. White, Laura Polakowski, Jian Yan, Janine Maenza, Guido Ferrari, Michael C. Keefer, Stephen C. De Rosa, Laurent Humeau, David C. Montefiori, M. Juliana McElrath, Jean D. Boyer, Amir S. Khan, and Spyros A. Kalams

Subjects

0301 basic medicine, Adult, HIV Infections, CD8-Positive T-Lymphocytes, DNA vaccination, 03 medical and health sciences, Young Adult, 0302 clinical medicine, Immune system, Vaccines, DNA, Medicine, Humans, HIV vaccine, AIDS Vaccines, biology, business.industry, Immunogenicity, Vaccination, General Medicine, DNA, Middle Aged, United States, Immunity, Humoral, 030104 developmental biology, Tolerability, 030220 oncology & carcinogenesis, Immunology, biology.protein, HIV-1, Antibody, Clinical Medicine, business, CD8

Abstract

BACKGROUND: HVTN 098, a randomized, double-blind, placebo-controlled trial, evaluated the safety, tolerability, and immunogenicity of PENNVAX-GP HIV DNA vaccine, administered with or without plasmid IL-12 (pIL-12), via intradermal (ID) or intramuscular (IM) electroporation (EP) in healthy, HIV-uninfected adults. The study tested whether PENNVAX-GP delivered via ID/EP at one-fifth the dose could elicit equivalent immune responses to delivery via IM/EP and whether inclusion of pIL-12 provided additional benefit. METHODS: Participants received DNA encoding HIV-1 env/gag/pol in 3 groups: 1.6 mg ID (ID no IL-12 group, n = 20), 1.6 mg ID + 0.4 mg pIL-12 (ID + IL-12 group, n = 30), 8 mg IM + 1 mg pIL-12 (IM + IL-12 group, n = 30), or placebo (n = 9) via EP at 0, 1, 3, and 6 months. Results of cellular and humoral immunogenicity assessments are reported. RESULTS: Following vaccination, the frequency of responders (response rate) to any HIV protein based on CD4(+) T cells expressing IFN-γ or IL-2 was 96% for both the ID + IL-12 and IM + IL-12 groups; CD8(+) T cell response rates were 64% and 44%, respectively. For ID delivery, the inclusion of pIL-12 increased CD4(+) T cell response rate from 56% to 96%. The frequency of responders was similar (≥90%) for IgG binding antibody to gp140 consensus Env across all groups, but the magnitude was higher in the ID + IL-12 group compared with the IM + IL-12 group. CONCLUSION: PENNVAX-GP DNA induced robust cellular and humoral immune responses, demonstrating that immunogenicity of DNA vaccines can be enhanced by EP route and inclusion of pIL-12. ID/EP was dose sparing, inducing equivalent, or in some aspects superior, immune responses compared with IM/EP. TRIAL REGISTRATION: ClinicalTrials.gov NCT02431767. FUNDING: This work was supported by National Institute of Allergy and Infectious Diseases (NIAID), U.S. Public Health Service grants, an HIV Vaccine Design and Development Team contract, Integrated Preclinical/Clinical AIDS Vaccine Development Program, and an NIH award.

Published

2020

117. HIV-1 Vaccine Sequences Impact V1V2 Antibody Responses: A Comparison of Two Poxvirus Prime gp120 Boost Vaccine Regimens

Author

Xiaoying Shen, Fatima Laher, Zoe Moodie, Rachel L. Spreng, Georgia D. Tomaras, Sanjay Phogat, Vijay L. Mehra, Michael Pensiero, Susan W. Barnett, Nicole Grunenberg, M. Juliana McElrath, Peter B. Gilbert, Mary Allen, Glenda Gray, Nicole L. Yates, Linda-Gail Bekker, Lawrence Corey, Olivier Van Der Meeren, Arthur S. McMillan, and Ying Huang

Subjects

0301 basic medicine, Male, Immunogen, Canarypox, Immunization, Secondary, lcsh:Medicine, Biology, HIV Envelope Protein gp120, Antibodies, Viral, Epitope, Article, Canarypox virus, 03 medical and health sciences, Epitopes, 0302 clinical medicine, Clinical trials, Antibody Specificity, Humans, Multiplex, 030212 general & internal medicine, lcsh:Science, AIDS Vaccines, Multidisciplinary, Linear epitope, lcsh:R, Translational research, biology.organism_classification, Virology, 3. Good health, Vaccination, 030104 developmental biology, Immunization, Antibody Formation, biology.protein, HIV-1, lcsh:Q, Female, Antibody, HIV infections

Abstract

In the RV144 trial, vaccine-induced V1V2 IgG correlated with decreased HIV-1 risk. We investigated circulating antibody specificities in two phase 1 poxvirus prime-protein boost clinical trials conducted in South Africa: HVTN 097 (subtype B/E) and HVTN 100 (subtype C). With cross-subtype peptide microarrays and multiplex binding assays, we probed the magnitude and breadth of circulating antibody responses to linear variable loop 2 (V2) and conformational V1V2 specificities. Antibodies targeting the linear V2 epitope, a correlate of decreased HIV-1 risk in RV144, were elicited up to 100% and 61% in HVTN 097 and HVTN 100, respectively. Despite higher magnitude of envelope-specific responses in HVTN 100 compared to HVTN 097 (p’s

Published

2020

118. Safety and immune responses after a 12-month booster in healthy HIV-uninfected adults in HVTN 100 in South Africa: A randomized double-blind placebo-controlled trial of ALVAC-HIV (vCP2438) and bivalent subtype C gp120/MF59 vaccines

Author

Kathryn Therese. Mngadi, Vijay L. Mehra, Kristen W. Cohen, Glenda Gray, Shannon Grant, Zoe Moodie, Brodie Daniels, Marguerite Koutsoukos, Sanjay Phogat, Peter B. Gilbert, M. Juliana McElrath, Nonhlanhla N. Mkhize, Chenchen Yu, Georgia D. Tomaras, Olivier Van Der Meeren, Linda-Gail Bekker, James G. Kublin, Nicole Frahm, Carlos A. DiazGranados, Mary Allen, Lawrence Corey, Fatima Laher, Carter Bentley, Mookho Malahleha, Michael Pensiero, Lynn Morris, Kevin O. Saunders, Nicole L. Yates, Nicole Grunenberg, David C. Montefiori, and Craig Innes

Subjects

CD4-Positive T-Lymphocytes, Male, Physiology, Human Immunodeficiency Virus Proteins, Placebo-controlled study, Antibody Response, HIV Infections, 030204 cardiovascular system & hematology, Gastroenterology, Biochemistry, Memory T cells, law.invention, White Blood Cells, South Africa, 0302 clinical medicine, Immunogenicity, Vaccine, Randomized controlled trial, law, Animal Cells, Immune Physiology, Medicine and Health Sciences, Public and Occupational Health, 030212 general & internal medicine, Booster Doses, Immune Response, Not evaluated, AIDS Vaccines, Vaccines, Immune System Proteins, T Cells, Headache, General Medicine, Vaccination and Immunization, Arthralgia, 3. Good health, Vaccination, Infectious Diseases, Medicine, Female, Cellular Types, Research Article, Adult, medicine.medical_specialty, Infectious Disease Control, Immune Cells, Immunology, Immunization, Secondary, Placebo, Injections, Intramuscular, Antibodies, 03 medical and health sciences, Young Adult, Double-Blind Method, Internal medicine, Injection site reaction, medicine, Humans, Adverse effect, Blood Cells, business.industry, Biology and Life Sciences, Proteins, Cell Biology, medicine.disease, Antibodies, Neutralizing, Injection Site Reaction, Regimen, Immunoglobulin G, Preventive Medicine, business

Abstract

Background HVTN 100 evaluated the safety and immunogenicity of an HIV subtype C pox-protein vaccine regimen, investigating a 12-month booster to extend vaccine-induced immune responses. Methods and findings A phase 1–2 randomized double-blind placebo-controlled trial enrolled 252 participants (210 vaccine/42 placebo; median age 23 years; 43% female) between 9 February 2015 and 26 May 2015. Vaccine recipients received ALVAC-HIV (vCP2438) alone at months 0 and 1 and with bivalent subtype C gp120/MF59 at months 3, 6, and 12. Antibody (IgG, IgG3 binding, and neutralizing) and CD4+ T-cell (expressing interferon-gamma, interleukin-2, and CD40 ligand) responses were evaluated at month 6.5 for all participants and at months 12, 12.5, and 18 for a randomly selected subset. The primary analysis compared IgG binding antibody (bAb) responses and CD4+ T-cell responses to 3 vaccine-matched antigens at peak (month 6.5 versus 12.5) and durability (month 12 versus 18) timepoints; IgG responses to CaseA2_gp70_V1V2.B, a primary correlate of risk in RV144, were also compared at these same timepoints. Secondary and exploratory analyses compared IgG3 bAb responses, IgG bAb breadth scores, neutralizing antibody (nAb) responses, antibody-dependent cellular phagocytosis, CD4+ polyfunctionality responses, and CD4+ memory sub-population responses at the same timepoints. Vaccines were generally safe and well tolerated. During the study, there were 2 deaths (both in the vaccine group and both unrelated to study products). Ten participants became HIV-infected during the trial, 7% (3/42) of placebo recipients and 3% (7/210) of vaccine recipients. All 8 serious adverse events were unrelated to study products. Less waning of immune responses was seen after the fifth vaccination than after the fourth, with higher antibody and cellular response rates at month 18 than at month 12: IgG bAb response rates to 1086.C V1V2, 21.0% versus 9.7% (difference = 11.3%, 95% CI = 0.6%–22.0%, P = 0.039), and ZM96.C V1V2, 21.0% versus 6.5% (difference = 14.5%, 95% CI = 4.1%–24.9%, P = 0.004). IgG bAb response rates to all 4 primary V1V2 antigens were higher 2 weeks after the fifth vaccination than 2 weeks after the fourth vaccination: 87.7% versus 75.4% (difference = 12.3%, 95% CI = 1.7%–22.9%, P = 0.022) for 1086.C V1V2, 86.0% versus 63.2% (difference = 22.8%, 95% CI = 9.1%–36.5%, P = 0.001) for TV1c8.2.C V1V2, 67.7% versus 44.6% (difference = 23.1%, 95% CI = 10.4%–35.7%, P < 0.001) for ZM96.C V1V2, and 81.5% versus 60.0% (difference = 21.5%, 95% CI = 7.6%–35.5%, P = 0.002) for CaseA2_gp70_V1V2.B. IgG bAb response rates to the 3 primary vaccine-matched gp120 antigens were all above 90% at both peak timepoints, with no significant differences seen, except a higher response rate to ZM96.C gp120 at month 18 versus month 12: 64.5% versus 1.6% (difference = 62.9%, 95% CI = 49.3%–76.5%, P < 0.001). CD4+ T-cell response rates were higher at month 18 than month 12 for all 3 primary vaccine-matched antigens: 47.3% versus 29.1% (difference = 18.2%, 95% CI = 2.9%–33.4%, P = 0.021) for 1086.C, 61.8% versus 38.2% (difference = 23.6%, 95% CI = 9.5%–37.8%, P = 0.001) for TV1.C, and 63.6% versus 41.8% (difference = 21.8%, 95% CI = 5.1%–38.5%, P = 0.007) for ZM96.C, with no significant differences seen at the peak timepoints. Limitations were that higher doses of gp120 were not evaluated, this study was not designed to investigate HIV prevention efficacy, and the clinical significance of the observed immunological effects is uncertain. Conclusions In this study, a 12-month booster of subtype C pox-protein vaccines restored immune responses, and slowed response decay compared to the 6-month vaccination. Trial registration ClinicalTrials.gov NCT02404311. South African National Clinical Trials Registry (SANCTR number: DOH--27-0215-4796)., Fatima Laher and co-authors report on safety and immune responses in a randomized trial of a candidate HIV vaccine incorporating a "booster" vaccination., Author summary Why was this study done? The RV144 vaccine trial, which tested a pox-protein regimen designed against HIV subtypes B and E, showed modest efficacy in preventing HIV acquisition. However, efficacy and vaccine-induced immune responses declined considerably after the first year. Our clinical trial, HVTN 100, investigated whether adding a booster at month 12 to a similar vaccine regimen, tailored against subtype C HIV, would prolong immune responses, and also evaluated its safety. What did the researchers do and find? We gave intramuscular injections of ALVAC-HIV (vCP2438) alone at months 0 and 1 and with bivalent subtype C gp120/MF59 at months 3, 6, and 12 to 210 vaccine recipients. We administered placebo to 42 participants. We tested antibody (IgG, IgG3 binding, antibody-dependent cellular phagocytosis, and neutralizing) and cellular (T cells expressing interferon-gamma, interleukin-2, or CD40 ligand) immune responses at month 6.5 in all participants and at months 12, 12.5, and 18 in a randomly chosen subset. We evaluated safety for 18 months. Vaccines were generally safe and well tolerated. Antibody and cellular response rates were higher after the 12-month booster than after the 6-month vaccination. What do these findings mean? Adding a booster osf subtype C pox-protein vaccines at month 12 can improve the durability of vaccine-induced immune responses. The ongoing phase 2b–3 trial HVTN 702 was designed to evaluate the efficacy of this regimen with month 12 and month 18 boosters.

Published

2020

119. Boosting with AIDSVAX B/E Enhances Env Constant Region 1 and 2 Antibody-Dependent Cellular Cytotoxicity Breadth and Potency

Author

Sanjay Phogat, Jaranit Kaewkungwal, Georgia D. Tomaras, S. Munir Alam, Brianna D. Young, Jean-Louis Excler, William D. Tolbert, Kevin O. Saunders, Merlin L. Robb, Justin Pollara, Jerome H. Kim, James Tartaglia, Punnee Pitisuttithum, Shalini Jha, Nelson L. Michael, Marzena Pazgier, Barton F. Haynes, David C. Montefiori, Kevin Wiehe, Supachai Rerks-Ngarm, Sandhya Vasan, Kan Luo, Robert J. O'Connell, Dieter Mielke, M. Anthony Moody, Guido Ferrari, Faruk Sinangil, Sorachai Nitayaphan, David Easterhoff, and Thomas B. Kepler

Subjects

HIV vaccine, medicine.drug_class, Immunology, Immunization, Secondary, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Biology, Monoclonal antibody, Microbiology, Epitope, Epitopes, 03 medical and health sciences, 0302 clinical medicine, Antibody Repertoire, Antibody Specificity, Virology, Vaccines and Antiviral Agents, medicine, Humans, 030304 developmental biology, AIDS Vaccines, Antibody-dependent cell-mediated cytotoxicity, 0303 health sciences, Antibody-Dependent Cell Cytotoxicity, Antibodies, Monoclonal, virus diseases, Vaccine efficacy, 3. Good health, Immunoglobulin G, 030220 oncology & carcinogenesis, Insect Science, AIDSVAX, Antibody Formation, HIV-1, biology.protein, Antibody, antibody function

Abstract

Over one million people become infected with HIV-1 each year, making the development of an efficacious HIV-1 vaccine an important unmet medical need. The RV144 human HIV-1 vaccine regimen is the only HIV-1 clinical trial to date to demonstrate vaccine efficacy. An area of focus has been on identifying ways by which to improve upon RV144 vaccine efficacy. The RV305 HIV-1 vaccine regimen was a follow-up boost of RV144 vaccine recipients that occurred 6 to 8 years after the conclusion of RV144. Our study focused on the effect of delayed boosting in humans on the vaccine-induced Env constant region 1 and 2 (C1C2)-specific antibody repertoire. It was found that boosting with an HIV-1 Env vaccine increased C1C2-specific antibody-dependent cellular cytotoxicity potency and breadth., Induction of protective antibodies is a critical goal of HIV-1 vaccine development. One strategy is to induce nonneutralizing antibodies (NNAbs) that kill virus-infected cells, as these antibody specificities have been implicated in slowing HIV-1 disease progression and in protection. HIV-1 Env constant region 1 and 2 (C1C2) monoclonal antibodies (MAbs) frequently mediate potent antibody-dependent cellular cytotoxicity (ADCC), making them an important vaccine target. Here, we explore the effect of delayed and repetitive boosting of RV144 vaccine recipients with AIDSVAX B/E on the C1C2-specific MAb repertoire. It was found that boosting increased clonal lineage-specific ADCC breadth and potency. A ligand crystal structure of a vaccine-induced broad and potent ADCC-mediating C1C2-specific MAb showed that it bound a highly conserved Env gp120 epitope. Thus, boosting to affinity mature these types of IgG C1C2-specific antibody responses may be one method by which to make an improved HIV vaccine with higher efficacy than that seen in the RV144 trial. IMPORTANCE Over one million people become infected with HIV-1 each year, making the development of an efficacious HIV-1 vaccine an important unmet medical need. The RV144 human HIV-1 vaccine regimen is the only HIV-1 clinical trial to date to demonstrate vaccine efficacy. An area of focus has been on identifying ways by which to improve upon RV144 vaccine efficacy. The RV305 HIV-1 vaccine regimen was a follow-up boost of RV144 vaccine recipients that occurred 6 to 8 years after the conclusion of RV144. Our study focused on the effect of delayed boosting in humans on the vaccine-induced Env constant region 1 and 2 (C1C2)-specific antibody repertoire. It was found that boosting with an HIV-1 Env vaccine increased C1C2-specific antibody-dependent cellular cytotoxicity potency and breadth.

Published

2020

120. HIV vaccine delayed boosting increases Env variable region 2–specific antibody effector functions

Author

Neelakshi Gohain, Susie Min, S Rerks-Ngarm, Benjamin M. Janus, Georgia D. Tomaras, Barton F. Haynes, Jerome H. Kim, Matthew Zirui Tay, Nelson L. Michael, Merlin L. Robb, Peng Zhang, Jaranit Kaewkungwal, Guido Ferrari, David C. Montefiori, Mangala Rao, David Easterhoff, Matina Kakalis, Jean-Louis Excler, Faruk Sinangil, Anthony Monroe, Kwan-Ki Hwang, Mattia Bonsignori, M. Gordon Joyce, James Arthos, Kevin Wiehe, Eden P. Go, Gilad Ofek, Kristina K. Peachman, Paolo Lusso, Sanjay Phogat, S Nitayaphan, LaTonya D. Williams, Sandhya Vasan, James Tartaglia, M. Anthony Moody, Misook Choe, Punnee Pitisuttithum, Kan Luo, Charles Beck, Robert J. O'Connell, Heather Desaire, Kevin O. Saunders, and Justin Pollara

Subjects

Models, Molecular, 0301 basic medicine, Protein Conformation, medicine.drug_class, Immunization, Secondary, Immunoglobulin Variable Region, Somatic hypermutation, HIV Infections, HIV Antibodies, Monoclonal antibody, Epitope, Epitopes, 03 medical and health sciences, 0302 clinical medicine, X-Ray Diffraction, medicine, Humans, HIV vaccine, Memory B cell, AIDS Vaccines, Clinical Trials as Topic, biology, Antibody-Dependent Cell Cytotoxicity, env Gene Products, Human Immunodeficiency Virus, Antibodies, Monoclonal, Viral Vaccines, General Medicine, Vaccine efficacy, Vaccination, 030104 developmental biology, 030220 oncology & carcinogenesis, Mutation, Immunology, HIV-1, biology.protein, Antibody, Research Article

Abstract

In the RV144 HIV-1 phase III trial, vaccine efficacy directly correlated with the magnitude of the variable region 2–specific (V2-specific) IgG antibody response, and in the presence of low plasma IgA levels, with the magnitude of plasma antibody-dependent cellular cytotoxicity. Reenrollment of RV144 vaccinees in the RV305 trial offered the opportunity to define the function, maturation, and persistence of vaccine-induced V2-specific and other mAb responses after boosting. We show that the RV144 vaccine regimen induced persistent V2 and other HIV-1 envelope–specific memory B cell clonal lineages that could be identified throughout the approximately 11-year vaccination period. Subsequent boosts increased somatic hypermutation, a critical requirement for antibody affinity maturation. Characterization of 22 vaccine-induced V2-specific mAbs with epitope specificities distinct from previously characterized RV144 V2-specific mAbs CH58 and CH59 found increased in vitro antibody-mediated effector functions. Thus, when inducing non-neutralizing antibodies, one method by which to improve HIV-1 vaccine efficacy may be through late boosting to diversify the V2-specific response to increase the breadth of antibody-mediated anti–HIV-1 effector functions.

Published

2020

121. Landscapes of binding antibody and T-cell responses to pox-protein HIV vaccines in Thais and South Africans

Author

Llewellyn Fleurs, Nadine Rouphael, Nigel Garrett, Craig Innes, Lue Ping Zhao, Lawrence Corey, Nicole L. Yates, One B. Dintwe, Lindsay N. Carpp, Punnee Pitisuttithum, Kristen W. Cohen, Peter B. Gilbert, Michael Zhao, Youyi Fong, Kelly E. Seaton, Merlin L. Robb, Andrew Fiore-Gartland, Stephen C. De Rosa, Nicole Frahm, Nelson L. Michael, M. Juliana McElrath, Sorachai Nitayaphan, Zoe Moodie, Glenda Gray, Supachai Rerks-Ngarm, Ying Huang, Erica Lazarus, Holly Janes, and Georgia D. Tomaras

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Male, Physiology, HIV Antigens, MF59, Antibody Response, HIV Infections, HIV Antibodies, Biochemistry, White Blood Cells, South Africa, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine and Health Sciences, Cytotoxic T cell, Public and Occupational Health, 030212 general & internal medicine, HIV vaccine, Immune Response, AIDS Vaccines, Vaccines, Multidisciplinary, Immune System Proteins, T Cells, Thailand, Vaccination and Immunization, 3. Good health, medicine.anatomical_structure, Infectious Diseases, Medicine, Female, Antibody, Cellular Types, Research Article, Adult, Infectious Disease Control, Adolescent, T cell, Immune Cells, Science, Immunology, Cytotoxic T cells, Biology, Microbiology, Antibodies, 03 medical and health sciences, Young Adult, Immune system, Antigen, Virology, medicine, Humans, Blood Cells, Viral vaccines, HIV vaccines, Biology and Life Sciences, Proteins, Cell Biology, Antibodies, Neutralizing, Regimen, 030104 developmental biology, Antibody Formation, biology.protein, HIV-1, Preventive Medicine

Abstract

BackgroundHIV vaccine trials routinely measure multiple vaccine-elicited immune responses to compare regimens and study their potential associations with protection. Here we employ unsupervised learning tools facilitated by a bidirectional power transformation to explore the multivariate binding antibody and T-cell response patterns of immune responses elicited by two pox-protein HIV vaccine regimens. Both regimens utilized a recombinant canarypox vector (ALVAC-HIV) prime and a bivalent recombinant HIV-1 Envelope glycoprotein 120 subunit boost. We hypothesized that within each trial, there were participant subgroups sharing similar immune responses and that their frequencies differed across trials.Methods and findingsWe analyzed data from three trials-RV144 (NCT00223080), HVTN 097 (NCT02109354), and HVTN 100 (NCT02404311), the latter of which was pivotal in advancing the tested pox-protein HIV vaccine regimen to the HVTN 702 Phase 2b/3 efficacy trial. We found that bivariate CD4+ T-cell and anti-V1V2 IgG/IgG3 antibody response patterns were similar by age, sex-at-birth, and body mass index, but differed for the pox-protein clade AE/B alum-adjuvanted regimen studied in RV144 and HVTN 097 (PAE/B/alum) compared to the pox-protein clade C/C MF59-adjuvanted regimen studied in HVTN 100 (PC/MF59). Specifically, more PAE/B/alum recipients had low CD4+ T-cell and high anti-V1V2 IgG/IgG3 responses, and more PC/MF59 recipients had broad responses of both types. Analyses limited to "vaccine-matched" antigens suggested that some of the differences in responses between the regimens could have been due to antigens in the assays that did not match the vaccine immunogens. Our approach was also useful in identifying subgroups with unusually absent or high co-responses across assay types, flagging individuals for further characterization by functional assays. We also found that co-responses of anti-V1V2 IgG/IgG3 and CD4+ T cells had broad variability. As additional immune response assays are standardized and validated, we anticipate our framework will be increasingly valuable for multivariate analysis.ConclusionsOur approach can be used to advance vaccine development objectives, including the characterization and comparison of candidate vaccine multivariate immune responses and improved design of studies to identify correlates of protection. For instance, results suggested that HVTN 702 will have adequate power to interrogate immune correlates involving anti-V1V2 IgG/IgG3 and CD4+ T-cell co-readouts, but will have lower power to study anti-gp120/gp140 IgG/IgG3 due to their lower dynamic ranges. The findings also generate hypotheses for future testing in experimental and computational analyses aimed at achieving a mechanistic understanding of vaccine-elicited immune response heterogeneity.

Published

2020

122. Fc-Mediated Antibody Functions and Fc-Receptor Polymorphism

Author

Guido Ferrari, R. Keith Reeves, Gabriella Scarlatti, and Georgia D. Tomaras

Subjects

biology, Polymorphism (computer science), Chemistry, biology.protein, Fc receptor, Antibody, Molecular biology

Published

2020

123. Optimal priming of poxvirus vector (NYVAC)-based HIV vaccine regimens for T cell responses requires three DNA injections. Results of the randomized multicentre EV03/ANRS VAC20 Phase I/II Trial

Author

Jean-Daniel Lelièvre, Ralf Wagner, Hans Wolf, Pierre-Alexandre Bart, Bernd Salzberger, Nicole L. Yates, Georgia D. Tomaras, Yves Levy, Aurélie Wiedemann, Rodolphe Thiébaut, Raphael Gottardo, Wolfgang Stöhr, David M. Koelle, Sheena McCormack, Véronique Rieux, Song Ding, Giuseppe Pantaleo, Christine Lacabaratz, Kim Ellefsen-Lavoie, Odile Launay, Bryan T. Mayer, David C. Montefiori, Geneviève Chêne, Mathieu Surenaud, Jonathan Weber, DARMIGNY, SANDRINE, Vaccine Research Institute (VRI), Université Paris-Est Créteil Val-de-Marne - Paris 12 (UPEC UP12), CHU Henri Mondor, Centre Hospitalier Universitaire Vaudois [Lausanne] (CHUV), University College of London [London] (UCL), Assistance publique - Hôpitaux de Paris (AP-HP) (AP-HP), Imperial College London, University of Washington [Seattle], Universität Regensburg (UR), Duke University Medical Center, Fred Hutchinson Cancer Research Center [Seattle] (FHCRC), EuroVacc Foundation (EVF), Statistics In System biology and Translational Medicine (SISTM), Inria Bordeaux - Sud-Ouest, Institut National de Recherche en Informatique et en Automatique (Inria)-Institut National de Recherche en Informatique et en Automatique (Inria)- Bordeaux population health (BPH), Université de Bordeaux (UB)-Institut de Santé Publique, d'Épidémiologie et de Développement (ISPED)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Bordeaux (UB)-Institut de Santé Publique, d'Épidémiologie et de Développement (ISPED)-Institut National de la Santé et de la Recherche Médicale (INSERM), Bordeaux population health (BPH), Université de Bordeaux (UB)-Institut de Santé Publique, d'Épidémiologie et de Développement (ISPED)-Institut National de la Santé et de la Recherche Médicale (INSERM), and CHU Henri Mondor [Créteil]

Subjects

RNA viruses, Male, Physiology, HIV Antigens, [SDV]Life Sciences [q-bio], Antibody Response, Priming (immunology), CD8-Positive T-Lymphocytes, Pathology and Laboratory Medicine, Biochemistry, White Blood Cells, Immunodeficiency Viruses, Animal Cells, 1108 Medical Microbiology, Immune Physiology, Medicine and Health Sciences, Vaccines, DNA, Clinical endpoint, Cytotoxic T cell, Enzyme-Linked Immunoassays, HIV vaccine, Biology (General), Immune Response, ComputingMilieux_MISCELLANEOUS, AIDS Vaccines, Vaccines, Innate Immune System, 0303 health sciences, Immune System Proteins, biology, T Cells, ELISPOT, 030302 biochemistry & molecular biology, env Gene Products, Human Immunodeficiency Virus, T-Lymphocytes, Helper-Inducer, Middle Aged, 3. Good health, [SDV] Life Sciences [q-bio], Infectious Diseases, medicine.anatomical_structure, Medical Microbiology, 1107 Immunology, Viral Pathogens, Viruses, Cytokines, Female, Cellular Types, Pathogens, Antibody, Research Article, 0605 Microbiology, Adult, Infectious Disease Control, Adolescent, QH301-705.5, Immune Cells, T cell, Genetic Vectors, Immunology, Research and Analysis Methods, Microbiology, Antibodies, Interferon-gamma, 03 medical and health sciences, Virology, Retroviruses, Genetics, medicine, Humans, Immunoassays, Microbial Pathogens, Molecular Biology, 030304 developmental biology, Blood Cells, business.industry, Poxviridae, Lentivirus, Organisms, Biology and Life Sciences, Proteins, HIV, Cell Biology, Molecular Development, RC581-607, Regimen, Immune System, Immunologic Techniques, biology.protein, Parasitology, Immunologic diseases. Allergy, business, Developmental Biology

Abstract

DNA vectors have been widely used as a priming of poxvirus vaccine in prime/boost regimens. Whether the number of DNA impacts qualitatively or quantitatively the immune response is not fully explored. With the aim to reinforce T-cell responses by optimizing the prime-boost regimen, the multicentric EV03/ANRS VAC20 phase I/II trial, randomized 147 HIV-negative volunteers to either 3xDNA plus 1xNYVAC (weeks 0, 4, 8 plus 24; n = 74) or to 2xDNA plus 2xNYVAC (weeks 0, 4 plus 20, 24; n = 73) groups. T-cell responses (IFN-γ ELISPOT) to at least one peptide pool were higher in the 3xDNA than the 2xDNA groups (91% and 80% of vaccinees) (P = 0.049). In the 3xDNA arm, 26 (37%) recipients developed a broader T-cell response (Env plus at least to one of the Gag, Pol, Nef pools) than in the 2xDNA (15; 22%) arms (primary endpoint; P = 0.047) with a higher magnitude against Env (at week 26) (P, Author summary Development of a safe and effective HIV-1 vaccine would undoubtedly be the best solution for the ultimate control of the worldwide AIDS pandemic. To date, only one large phase III trial (RV144 Thai study) showed a partial and modest protection against HIV infection. This result raised hope in the field and encouraged the development of vaccines or strategies in order to improve vaccine efficacy. Several vaccine strategies designed to elicit broad HIV-specific T cells and/or neutralizing antibodies to prevent HIV-1 transmission are under evaluation. Among diverse candidate vaccines, the safety and immunogenicity of multi-gene DNA-based and Pox-virus derived vaccines have been evaluated in several clinical studies. The present study was designed to optimize the combination of these two vaccines with the aim of determining the optimal number of DNA primes for a poxvirus-based HIV vaccine regimen. We show here that the prime boost combination is highly immunogenic and that the number of DNA primes induces differentially T cell and antibody responses. A better priming of poxvirus-based vaccine regimens for T cells is obtained with 3 DNA injections. Our results contribute and extend data of several preclinical studies pointing out the potential interest of DNA as a prime capable not only of improving immune responses but also of imprinting the long-term responses to boost vaccines.

Published

2020

124. Persistence of vaccine-elicited immune response up to 14 years post-HIV gp120-NefTat/AS01(B) vaccination

Author

Doris Mesia Vela, Caroline Brackett, Nicole L. Yates, Isabel Leroux-Roels, Erik Jongert, Annelies Aerssens, François Roman, Olivier Van Der Meeren, Sheetal Sawant, Geert Leroux-Roels, Georgia D. Tomaras, Marguerite Koutsoukos, Muriel Debois, Michel Janssens, and Kelly E. Seaton

Subjects

Cellular immunity, 030231 tropical medicine, 03 medical and health sciences, 0302 clinical medicine, Immune system, Antigen, Immunity, INFECTION, BINDING, medicine, Medicine and Health Sciences, Interferon gamma, 030212 general & internal medicine, ALVAC, CD40, General Veterinary, General Immunology and Microbiology, biology, Public Health, Environmental and Occupational Health, EFFICACY, Vaccination, Infectious Diseases, AIDSVAX, Immunology, ANTIBODIES, biology.protein, Molecular Medicine, VIRUS, TRIAL, Antibody, RHESUS-MONKEYS, medicine.drug

Abstract

Background Vaccines eliciting protective and persistent immune responses against multiple human immunodeficiency virus type 1 (HIV-1) clades are needed. This study evaluated the persistence of immune responses induced by an investigational, AS01-adjuvanted HIV-1 vaccine as long as 14 years after vaccination. Methods This phase I, open-label, descriptive, mono-centric, extension study with a single group (NCT03368053) was conducted in adults who received ≥3 doses of the clade B gp120-NefTat/AS01B vaccine candidate 14 years earlier in a previous clinical trial (NCT00434512). Binding responses of serum antibodies targeting a panel of envelope glycoproteins, including gp120, gp140 and V1V2-scaffold antigens and representative of the antigenic diversity of HIV-1, were measured by binding antibody multiplex assay (BAMA). The gp120-specific CD4+/CD8+ T-cell responses were assessed by intracellular cytokine staining assay. Results At Year 14, positive IgG binding antibody responses were detected in 15 out of the 16 antigens from the BAMA V1V2 breadth panel, with positive response rates ranging from 7.1% to 60.7%. The highest response rates were observed for clade B strain V1V2 antigens, with some level of binding antibodies against clade C strains. Anti-V1V2 IgG3 response magnitude breadth, which correlated with decreased risk of infection in a previous efficacy trial, was of limited amplitude. Response rates to the antigens from the gp120 and gp140 breadth panels ranged from 7.7% to 94.1% and from 15.4% to 96.2% at Year 14, respectively. Following stimulation with gp120 peptide pool, highly polyfunctional gp120-specific CD4+ T-cells persisted up to Year 14, with high frequencies of CD40L tumor necrosis factor alpha (TNF-α), CD40L interleukin-2 (IL-2), CD40L TNF-α IL-2 and CD40L interferon gamma (IFN-γ) TNF-α IL-2 CD4+ T-cells, but no CD8+ T-cells detected. Conclusions Persistent antibodies binding to HIV-1 envelope glycoproteins, including the V1V2-scaffold, and gp120-specific cellular immunity were observed in volunteers vaccinated 14 years earlier with the gp120-NefTat/AS01B vaccine candidate.

Published

2020

125. SARS-CoV-2 antibodies specific to the mesa and inner side of spike protein receptor binding domain maintain high affinities for both D614G and b.1.351 variants

Author

Kan Li, Richard H.C. Huntwork, Gillian Q. Horn, Elizabeth Feeney, Kathryn M. Hastie, Haoyang Li, Vamseedhar Rayaprolu, Olmedillas Olmedillas, Sharon L. Schendel, Mark Heise, Ralph S. Baric, S. Munir Alam, Erica Ollmann Saphire, Georgia D. Tomaras, and S. Moses Dennison

Subjects

Biophysics

Published

2022

126. Route of immunization defines multiple mechanisms of vaccine-mediated protection against SIV

Author

Sean O’Keefe, Derrick Goodman, Nickita Mehta, Douglas A. Lauffenburger, Thomas Broge, Eric P. Brown, Jessica K. Sassic, Caitlyn Linde, Srivamshi Pittala, Magdalena Sips, Mario Roederer, Harini Natarajan, Todd J. Suscovich, Shu Lin, Georgia D. Tomaras, Joshua A. Weiner, Todd Bradley, Jishnu Das, Barton F. Haynes, Galit Alter, Margaret E. Ackerman, and Chris Bailey-Kellogg

Subjects

Primates, 0301 basic medicine, Canarypox, Simian Acquired Immunodeficiency Syndrome, Injections, Intramuscular, Article, Antibodies, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Phagocytosis, Immunity, Administration, Inhalation, Animals, Humans, AIDS Vaccines, Vaccines, Innate immune system, biology, Drug Administration Routes, Vaccine trial, General Medicine, biology.organism_classification, Immunity, Innate, Immunoglobulin Fc Fragments, Vaccination, Disease Models, Animal, 030104 developmental biology, Immunization, Immunoglobulin G, Humoral immunity, Immunology, biology.protein, Simian Immunodeficiency Virus, Antibody, 030215 immunology

Abstract

Antibodies are the primary correlate of protection for most licensed vaccines; however, their mechanisms of protection may vary, ranging from physical blockade to clearance via the recruitment of innate immunity. Here, we uncover striking functional diversity in vaccine-induced antibodies that is driven by immunization site and is associated with reduced risk of SIV infection in nonhuman primates. While equivalent levels of protection were observed following intramuscular (IM) and aerosol (AE) immunization with an otherwise identical DNA prime-Ad5 boost regimen, reduced risk of infection was associated with IgG-driven antibody-dependent monocyte-mediated phagocytosis in the IM vaccinees, but with vaccine-elicited IgA-driven neutrophil-mediated phagocytosis in AE-immunized animals. Thus, although route-independent correlates indicate a critical role for phagocytic Fc-effector activity in protection from SIV, the site of immunization may drive this Fc activity via distinct innate effector cells and antibody isotypes. Moreover, the same correlates predicted protection from SHIV infection in a second nonhuman primate vaccine trial using a disparate IM canarypox prime-protein boost strategy, analogous to that used in the first moderately protective human HIV vaccine trial. These data identify orthogonal functional humoral mechanisms, initiated by distinct vaccination routes and immunization strategies, pointing to multiple, potentially complementary correlates of immunity that may support the rational design of a protective vaccine against HIV.

Published

2018

127. Safety and anti-viral activity of combination HIV-1 broadly neutralizing antibodies in viremic individuals

Author

Nico Pfeifer, Marina Caskey, Allison L. Butler, Theodora K. Karagounis, Clara Lehmann, Kanika Jain, Lilian Nogueira, Henning Gruell, Christoph Wyen, Gerd Fätkenheuer, Stefan Scholten, Maggi Witmer-Pack, Kerstin Fiddike, Joy A. Pai, Nicole L. Yates, Kelly E. Seaton, Jörg Janne Vehreschild, Till Schoofs, Juan Dizon, Roy M. Gulick, Isabelle Suárez, Thiago Y. Oliveira, Georgia D. Tomaras, Katrina G. Millard, Florian Klein, Michel C. Nussenzweig, Yotam Bar-On, Irina Shimeliovich, Michael S. Seaman, Jill Horowitz, Yehuda Z. Cohen, Lisa Handl, and Shiraz A. Belblidia

Subjects

0301 basic medicine, medicine.medical_treatment, 030106 microbiology, Viremia, HIV Infections, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Antiretroviral Therapy, Highly Active, Medicine, Humans, Dosing, Young adult, biology, business.industry, HIV, General Medicine, Immunotherapy, medicine.disease, Antiretroviral therapy, Virology, Combined Modality Therapy, 3. Good health, Clinical trial, 030104 developmental biology, biology.protein, Antibody, business, Viral load

Abstract

Monotherapy of HIV-1 infection with single antiretroviral agents is ineffective because error-prone HIV-1 replication leads to the production of drug-resistant viral variants1,2. Combinations of drugs can establish long-term control, however, antiretroviral therapy (ART) requires daily dosing, can cause side effects and does not eradicate the infection3,4. Although anti-HIV-1 antibodies constitute a potential alternative to ART5,6, treatment of viremic individuals with a single antibody also results in emergence of resistant viral variants7–9. Moreover, combinations of first-generation anti-HIV-1 broadly neutralizing antibodies (bNAbs) had little measurable effect on the infection10–12. Here we report on a phase 1b clinical trial ( NCT02825797 ) in which two potent bNAbs, 3BNC11713 and 10-107414, were administered in combination to seven HIV-1 viremic individuals. Infusions of 30 mg kg−1 of each of the antibodies were well-tolerated. In the four individuals with dual antibody-sensitive viruses, immunotherapy resulted in an average reduction in HIV-1 viral load of 2.05 log10 copies per ml that remained significantly reduced for three months following the first of up to three infusions. In addition, none of these individuals developed resistance to both antibodies. Larger studies will be necessary to confirm the efficacy of antibody combinations in reducing HIV-1 viremia and limiting the emergence of resistant viral variants. Combination of two broadly neutralizing antibodies is effective in reducing HIV-1 viremia and in limiting the emergence of resistant viral variants in individuals harboring antibody-sensitive viruses.

Published

2018

128. Combination therapy with anti-HIV-1 antibodies maintains viral suppression

Author

Theodora K. Karagounis, Christoph Wyen, Lilian Nogueira, Anthony P. West, Cecilia Unson-O’Brien, Gisela Kremer, Nico Pfeifer, Thiago Y. Oliveira, Yehuda Z. Cohen, Henning Gruell, Tim Kümmerle, Isabelle Suárez, Carola Ruping, Lisa Handl, Roshni Patel, Eleonore Thomas, Irina Shimeliovich, Roy M. Gulick, Maggi Witmer-Pack, Gerd Fätkenheuer, Ching-Lan Lu, Joy A. Pai, Michel C. Nussenzweig, Pilar Mendoza, Katrina G. Millard, Pamela J. Bjorkman, Michael S. Seaman, Clara Lehmann, Allison L. Butler, Julio C. C. Lorenzi, Georgia D. Tomaras, Kelly E. Seaton, Jill Horowitz, Maike Schlotz, Florian Klein, and Marina Caskey

Subjects

Male, 0301 basic medicine, medicine.medical_treatment, HIV Infections, Drug resistance, HIV Antibodies, HIV Envelope Protein gp160, 0302 clinical medicine, Medicine, 030212 general & internal medicine, Young adult, Infusions, Intravenous, Phylogeny, Multidisciplinary, biology, Antibodies, Monoclonal, Middle Aged, Virus Latency, 3. Good health, Drug Combinations, Carrier State, Monoclonal, Female, Antibody, Adult, Adolescent, Combination therapy, Anti-HIV Agents, medicine.drug_class, Antibodies, Monoclonal, Humanized, Monoclonal antibody, Article, Young Adult, 03 medical and health sciences, Drug Resistance, Viral, Humans, Viremia, Aged, business.industry, Historically Controlled Study, Immunotherapy, Antibodies, Neutralizing, Clinical trial, 030104 developmental biology, Immunology, HIV-1, biology.protein, Virus Activation, Binding Sites, Antibody, business, Broadly Neutralizing Antibodies

Abstract

Individuals infected with HIV-1 require lifelong antiretroviral therapy, because interruption of treatment leads to rapid rebound viraemia. Here we report on a phase 1b clinical trial in which a combination of 3BNC117 and 10-1074, two potent monoclonal anti-HIV-1 broadly neutralizing antibodies that target independent sites on the HIV-1 envelope spike, was administered during analytical treatment interruption. Participants received three infusions of 30 mg kg^(−1) of each antibody at 0, 3 and 6 weeks. Infusions of the two antibodies were generally well-tolerated. The nine enrolled individuals with antibody-sensitive latent viral reservoirs maintained suppression for between 15 and more than 30 weeks (median of 21 weeks), and none developed viruses that were resistant to both antibodies. We conclude that the combination of the anti-HIV-1 monoclonal antibodies 3BNC117 and 10-1074 can maintain long-term suppression in the absence of antiretroviral therapy in individuals with antibody-sensitive viral reservoirs.

Published

2018

129. Antibody-Dependent Cellular Cytotoxicity (ADCC)-Mediating Antibodies Constrain Neutralizing Antibody Escape Pathway

Author

Dieter Mielke, Gama Bandawe, Justin Pollara, Melissa-Rose Abrahams, Tinashe Nyanhete, Penny L. Moore, Ruwayhida Thebus, Nicole L. Yates, John C. Kappes, Christina Ochsenbauer, Nigel Garrett, Salim Abdool Karim, Georgia D. Tomaras, David Montefiori, Lynn Morris, Guido Ferrari, and Carolyn Williamson

Subjects

CD4-Positive T-Lymphocytes, lcsh:Immunologic diseases. Allergy, 0301 basic medicine, medicine.drug_class, Immunology, Epitopes, T-Lymphocyte, selection, HIV Infections, chemical and pharmacologic phenomena, HIV Antibodies, Virus Replication, Monoclonal antibody, Epitope, Virus, Cell Line, 03 medical and health sciences, 0302 clinical medicine, immune system diseases, medicine, Humans, Immunology and Allergy, skin and connective tissue diseases, Neutralizing antibody, Original Research, CD4-induced, Antibody-dependent cell-mediated cytotoxicity, biology, Antibody-Dependent Cell Cytotoxicity, neutralizing antibody, virus diseases, hemic and immune systems, Antibodies, Neutralizing, Virology, 3. Good health, 030104 developmental biology, Viral replication, Viral evolution, HIV-1, biology.protein, escape, Antibody, ADCC, lcsh:RC581-607, 030215 immunology

Abstract

Both neutralization and antibody-dependent cellular cytotoxicity (ADCC) may be required for effective protection against HIV-1 infection. While there is extensive information on the targets of early neutralizing antibody (nAb) responses, much less is known about the targets of ADCC responses, which are more difficult to characterize. In four individuals recruited during acute HIV-infection, ADCC responses were detected 3-7 weeks prior to nAb responses. To determine the relative influence of ADCC and nAb responses on virus evolution, we performed an in-depth investigation of one individual (CAP63) who showed the highest nAb and ADCC responses. Both nAbs and ADCC antibodies targeted the V4 region of the Env, although there were some differences in epitope recognition. We identified accelerated viral evolution in this region concurrent with emergence of nAb activity, but not ADCC activity. Deep sequencing demonstrated that most nAb escape mutations were strongly selected for, however one nAb escape mutation that rendered the virus highly susceptible to autologous ADCC responses, was suppressed despite not affecting viral fitness. This escape mutation also rendered the virus more sensitive to autologous responses, as well as monoclonal antibodies targeting CD4-induced epitopes, compared to the wildtype virus. In conclusion, ADCC responses and nAbs in donor CAP63 recognized overlapping but unique epitopes in the V4 region, and while ADCC activity was present prior to nAbs, it did not drive viral evolution during this time. However, ADCC responses may select against nAb escape pathways that expose other common ADCC epitopes thereby restricting viral replication and expansion.

Published

2019

130. Human gut microbiota is associated with HIV-reactive immunoglobulin at baseline and following HIV vaccination

Author

Andrew Fiore-Gartland, James G. Kublin, Giuseppe Pantaleo, Shelly Karuna, Jacob A. Cram, Sujatha Srinivasan, David N. Fredricks, and Georgia D. Tomaras

Subjects

0301 basic medicine, RNA viruses, CD4-Positive T-Lymphocytes, Male, Physiology, viruses, HIV Infections, Gut flora, HIV Antibodies, Pathology and Laboratory Medicine, Biochemistry, 0302 clinical medicine, Immunogenicity, Vaccine, Immunodeficiency Viruses, Immune Physiology, Medicine and Health Sciences, HIV vaccine, Immune Response, AIDS Vaccines, Vaccines, Multidisciplinary, Immune System Proteins, Ecology, Immunogenicity, Vaccination, env Gene Products, Human Immunodeficiency Virus, virus diseases, Genomics, Middle Aged, Combined Modality Therapy, 3. Good health, Infectious Diseases, Community Ecology, Medical Microbiology, Viral Pathogens, Viruses, Medicine, Female, Antibody, Pathogens, Research Article, Adult, Infectious Disease Control, Adolescent, Science, Immunology, Vaccinia virus, Microbial Genomics, Biology, Vaccines, Attenuated, Microbiology, Antibodies, 03 medical and health sciences, Young Adult, Immune system, Antigen, Double-Blind Method, Virology, Retroviruses, Genetics, Humans, Microbiome, Antigens, Community Structure, Microbial Pathogens, Viral vaccines, Ecology and Environmental Sciences, Lentivirus, HIV vaccines, Organisms, Biology and Life Sciences, Proteins, HIV, biology.organism_classification, Gastrointestinal Microbiome, 030104 developmental biology, biology.protein, HIV-1, 030217 neurology & neurosurgery

Abstract

Antibodies that recognize commensal microbial antigens may be cross reactive with a part of the human immunodeficiency virus (HIV) envelope glycoprotein gp41. To improve understanding of the role of the microbiota in modulating the immune response to HIV vaccines, we studied the associations of the gut microbiota composition of participants in the HIV Vaccine Trials Network 096 clinical trial with their HIV-specific immune responses in response to vaccination with a DNA-prime, pox virus boost strategy designed to recapitulate the only efficacious HIV-vaccine trial (RV144). We observed that both levels of IgG antibodies to gp41 at baseline and post-vaccination levels of IgG antibodies to the Con.6.gp120.B, ZM96.gp140 and gp70 B.CaseA V1-V2 antigens were associated with three co-occurring clusters of family level microbial taxa. One cluster contained several families positively associated with gp41-specific IgG and negatively associated with vaccine-matched gp120, gp140 and V1-V2-specific IgG responses. A second cluster contained families that negatively associated with gp41 and positively associated with gp120, gp140 and V1-V2-specific IgG responses. A third cluster contained microbial groups that did not correlate with any immune responses. Baseline and post-vaccination levels of gp41 IgG were not significantly correlated, suggesting that factors beyond the microbiome that contribute to immune response heterogeneity. Sequence variant richness was positively associated with gp41, p24, pg140 and V1-V2 specific IgG responses, gp41 and p24 IgA responses, and CD4+ T cell responses to HIV-1 proteins. Our findings provide preliminary evidence that the gut microbiota may be an important predictor of vaccine response.

Published

2019

131. ALVAC-HIV B/C candidate HIV vaccine efficacy dependent on neutralization profile of challenge virus and adjuvant dose and type

Author

Josh Kramer, Xiaoying Shen, Karin Loré, Melvin N. Doster, Sanjay Phogat, David C. Montefiori, Monica Vaccari, David Venzon, Hung V. Trinh, Luca Schifanella, Dallas R. Brown, Frank Liang, Mangala Rao, Ranajit Pal, Michelle Metrinko, Georgia D. Tomaras, Matthew Breed, Giacomo Gorini, Massimiliano Bissa, Susan W. Barnett, Veronica Galli, Galit Alter, William Magnanelli, Genoveffa Franchini, Ruth M. Ruprecht, Namal P.M. Liyanage, Celia C. LaBranche, and Robyn Washington-Parks

Subjects

medicine.medical_treatment, HIV Infections, Monkeys, Antibodies, Viral, Graduates, Pathology and Laboratory Medicine, Biochemistry, Neutralization, 0302 clinical medicine, Immunodeficiency Viruses, Medicine, Public and Occupational Health, HIV vaccine, Biology (General), Mammals, 0303 health sciences, 030302 biochemistry & molecular biology, Eukaryota, virus diseases, 3. Good health, Blood, Medical Microbiology, Viral Pathogens, Macaque, Primates, QH301-705.5, Immunology, Alumni, Microbiology, 03 medical and health sciences, Adjuvants, Immunologic, Genetics, Molecular Biology, Microbial Pathogens, Organisms, Correction, Proteins, Virology, Antibodies, Neutralizing, chemistry, Animal Studies, Parasitology, Population Groupings, Preventive Medicine, Immunologic diseases. Allergy, RNA viruses, Physiology, viruses, MF59, Simian Acquired Immunodeficiency Syndrome, chemistry.chemical_compound, Immunologic Adjuvants, Immune Physiology, Medicine and Health Sciences, 030212 general & internal medicine, Neutralizing antibody, AIDS Vaccines, Vaccines, Immune System Proteins, biology, SAIDS Vaccines, Animal Models, Vaccination and Immunization, Body Fluids, Infectious Diseases, Experimental Organism Systems, Vertebrates, Viruses, Alum Compounds, Educational Status, Female, Simian Immunodeficiency Virus, Anatomy, Pathogens, Adjuvant, Research Article, Infectious Disease Control, Research and Analysis Methods, Virus, Antibodies, Blood Plasma, Old World monkeys, Retroviruses, Animals, 030304 developmental biology, Biology and life sciences, Rhesus Monkeys, business.industry, Alum, Lentivirus, HIV, Viral Vaccines, RC581-607, Vaccine efficacy, Macaca mulatta, 13. Climate action, Amniotes, People and Places, biology.protein, business

Abstract

The ALVAC-HIV clade B/AE and equivalent SIV-based/gp120 + Alum vaccines successfully decreased the risk of virus acquisition in humans and macaques. Here, we tested the efficacy of HIV clade B/C ALVAC/gp120 vaccine candidates + MF59 or different doses of Aluminum hydroxide (Alum) against SHIV-Cs of varying neutralization sensitivity in macaques. Low doses of Alum induced higher mucosal V2-specific IgA that increased the risk of Tier 2 SHIV-C acquisition. High Alum dosage, in contrast, elicited serum IgG to V2 that correlated with a decreased risk of Tier 1 SHIV-C acquisition. MF59 induced negligible mucosal antibodies to V2 and an inflammatory profile with blood C-reactive Protein (CRP) levels correlating with neutralizing antibody titers. MF59 decreased the risk of Tier 1 SHIV-C acquisition. The relationship between vaccine efficacy and the neutralization profile of the challenge virus appear to be linked to the different immunological spaces created by MF59 and Alum via CXCL10 and IL-1β, respectively., Author summary The ALVAC-based clade C /gp120 combination is currently being tested for efficacy and licensures in South Africa in the HVTN702 HIV vaccine trial using the MF59 adjuvant rather than Alum with the intent of inducing higher neutralizing antibodies and T cell responses. Here, we present studies in 71 macaques that evaluated the relative efficacy of identical ALVAC-HIV B/C HIV vaccines with Alum or MF59 following challenge exposure to SHIV-clade C viral stocks that differed in their neutralization profiles. Our results demonstrated that use of the proprietary Novartis Alum at lower doses affects the proportion of mucosal V2-specific IgG and IgA, and that IgAs and IgGs were respectively associated with an increased or decreased risk of virus acquisition. In contrast, animals immunized with the MF59 regimen had no V2 mucosal responses, and a high level of serum neutralizing antibodies (Tier 1) to easy to neutralize viruses that were associated with a decreased risk of Tier 1 SHIV-C acquisition. In vitro studies suggest the hypothesis that the low doses of proprietary Novartis Alum used in our studies may be the underlying reason for the decreased vaccine efficacy, via lower inflammasome activation and IL-1β production.

Published

2019

132. Modification of the Association Between T-Cell Immune Responses and Human Immunodeficiency Virus Type 1 Infection Risk by Vaccine-Induced Antibody Responses in the HVTN 505 Trial

Author

Shannon Grant, Allan C. deCamp, Chenchen Yu, Susan Buchbinder, Edith Swann, Guido Ferrari, Barney S. Graham, Lindsay N. Carpp, Richard A. Koup, Shelly Karuna, Nicole Frahm, Holly Janes, Ian Frank, Mark J. Mulligan, Youyi Fong, Kelly E. Seaton, Robert T. Bailer, Xiaoying Shen, Barton F. Haynes, Georgia D. Tomaras, Magda Sobieszczyk, Richard M. Novak, M. Juliana McElrath, Vicki C Ashley, Michael C. Keefer, Spyros A. Kalams, Edwin DeJesus, David C. Montefiori, Aaron Deal, Peter B. Gilbert, Marcella Sarzotti-Kelsoe, and Scott M. Hammer

Subjects

0301 basic medicine, Immunoglobulin A, Male, CD8 T cells, HIV Infections, CD8-Positive T-Lymphocytes, HIV Antibodies, Immunoglobulin G, 03 medical and health sciences, Major Articles and Brief Reports, 0302 clinical medicine, Immune system, vaccine, antibody, human immunodeficiency virus type 1 (HIV-1), Immunology and Allergy, Medicine, Humans, 030212 general & internal medicine, HVTN 505, AIDS Vaccines, biology, business.industry, correlate of risk, Vaccine efficacy, 3. Good health, Vaccination, 030104 developmental biology, Infectious Diseases, Immunology, Antibody Formation, biology.protein, HIV-1, HIV/AIDS, Antibody, business, CD8

Abstract

Background HVTN 505 was a human immunodeficiency virus type 1 (HIV-1) preventive vaccine efficacy trial of a DNA/recombinant adenovirus serotype 5 (rAd5) vaccine regimen. We assessed antibody responses measured 1 month after final vaccination (month 7) as correlates of HIV-1 acquisition risk. Methods Binding antibody responses were quantified in serum samples from 25 primary endpoint vaccine cases (diagnosed with HIV-1 infection between month 7 and month 24) and 125 randomly sampled frequency-matched vaccine controls (HIV-1 negative at month 24). We prespecified for a primary analysis tier 6 antibody response biomarkers that measure immunoglobulin G (IgG) and immunoglobulin A (IgA) binding to Env proteins and 2 previously assessed T-cell response biomarkers. Results Envelope-specific IgG responses were significantly correlated with decreased HIV-1 risk. Moreover, the interaction of IgG responses and Env-specific CD8+ T-cell polyfunctionality score had a highly significant association with HIV-1 risk after adjustment for multiple comparisons. Conclusions Vaccinees with higher levels of Env IgG have significantly decreased HIV-1 risk when CD8+ T-cell responses are low. Moreover, vaccinees with high CD8+ T-cell responses generally have low risk, and those with low CD8+ T-cell and low Env antibody responses have high risk. These findings suggest the critical importance of inducing a robust IgG Env response when the CD8+ T-cell response is low., Vaccine-elicited antibodies and T cells correlate with decreased human immunodeficiency virus type 1 (HIV-1) risk in an HIV-1 preventative vaccine efficacy trial of a DNA/recombinant adenovirus serotype 5 (rAd5) vaccine regimen.

Published

2018

133. Structural and genetic convergence of HIV-1 neutralizing antibodies in vaccinated non-human primates

Author

M. Gordon Joyce, Xiaoying Shen, Kevin O. Saunders, Sampa Santra, M. Anthony Moody, Misook Choe, Barton F. Haynes, Wei-Hung Chen, Kshitij Wagh, Esther Lee, Amanda Eaton, Bette T. Korber, Michael S. Seaman, Mattia Bonsignori, Julia A. Jones, Weimin Wu, David C. Montefiori, Laura L. Sutherland, Giovanna Hernandez, Kevin Wiehe, Richard M. Scearce, Celia C. LaBranche, Fangping Cai, Natalia de Val, Neelakshi Gohain, Nelson R. Wu, and Georgia D. Tomaras

Subjects

RNA viruses, Glycosylation, B Cells, Physiology, Glycobiology, HIV Infections, Monkeys, HIV Antibodies, Pathology and Laboratory Medicine, Biochemistry, Macaque, Epitope, White Blood Cells, 0302 clinical medicine, Immunodeficiency Viruses, Animal Cells, Immune Physiology, Medicine and Health Sciences, Enzyme-Linked Immunoassays, Post-Translational Modification, Biology (General), Mammals, AIDS Vaccines, Vaccines, 0303 health sciences, Immune System Proteins, biology, env Gene Products, Human Immunodeficiency Virus, Eukaryota, Vaccination, Medical Microbiology, Viral Pathogens, Vertebrates, Viruses, Infectious diseases, Pathogens, Cellular Types, Antibody, Research Article, Primates, Medical conditions, QH301-705.5, medicine.drug_class, Immune Cells, Immunology, Research and Analysis Methods, Monoclonal antibody, Microbiology, Antibodies, 03 medical and health sciences, Immune system, Virology, biology.animal, Old World monkeys, Retroviruses, Infectious disease control, Genetics, medicine, Animals, Humans, Immunoassays, Antibody-Producing Cells, Microbial Pathogens, Molecular Biology, 030304 developmental biology, Blood Cells, Viral vaccines, Lentivirus, Organisms, HIV vaccines, Biology and Life Sciences, Proteins, HIV, Cell Biology, RC581-607, Antibodies, Neutralizing, Macaca mulatta, Monoclonal Antibodies, Immunization, Amniotes, HIV-1, Immunologic Techniques, biology.protein, Parasitology, Paratope, Immunologic diseases. Allergy, Zoology, 030217 neurology & neurosurgery

Abstract

A primary goal of HIV-1 vaccine development is the consistent elicitation of protective, neutralizing antibodies. While highly similar neutralizing antibodies (nAbs) have been isolated from multiple HIV-infected individuals, it is unclear whether vaccination can consistently elicit highly similar nAbs in genetically diverse primates. Here, we show in three outbred rhesus macaques that immunization with Env elicits a genotypically and phenotypically conserved nAb response. From these vaccinated macaques, we isolated four antibody lineages that had commonalities in immunoglobulin variable, diversity, and joining gene segment usage. Atomic-level structures of the antigen binding fragments of the two most similar antibodies showed nearly identical paratopes. The Env binding modes of each of the four vaccine-induced nAbs were distinct from previously known monoclonal HIV-1 neutralizing antibodies, but were nearly identical to each other. The similarities of these antibodies show that the immune system in outbred primates can respond to HIV-1 Env vaccination with a similar structural and genotypic solution for recognizing a particular neutralizing epitope. These results support rational vaccine design for HIV-1 that aims to reproducibly elicit, in genetically diverse primates, nAbs with specific paratope structures capable of binding conserved epitopes., Author summary The primate immune system generates a diverse repertoire of pathogen-binding proteins called antibodies. Primate antibody repertoires must be diverse to respond to infection by many different pathogens. In this study, we characterized the structure and genetic features of HIV-1 inhibitory antibodies from vaccinated monkeys as a model for human vaccination. We found that individual monkeys responded to HIV vaccination by generating highly similar HIV-1 neutralizing antibodies. The antibodies had nearly identical structures and genetic makeups. Thus, the immune systems of different monkeys generate a common solution for inhibiting viral protein function and infectivity. Success of vaccines in multiple recipients may be augmented by the ability of immune systems to reproducibly devise a common antibody solution to attack vulnerable sites on pathogens.

Published

2021

134. Innate transcriptional effects by adjuvants on the magnitude, quality, and durability of HIV envelope responses in NHPs

Author

Bronwyn M. Gunn, Andres M. Salazar, Robert A. Seder, Nicholas Valiante, Pampi Sarkar, Alan Aderem, Siddhartha Jain, Barbara J. Flynn, Guido Ferrari, Manmohan Singh, Georgia D. Tomaras, Padma Malyala, Joseph R. Francica, Galit Alter, Ennio De Gregorio, Munir Alam, Caitlyn Linde, Margaret E. Ackerman, Nicole L. Yates, Susan W. Barnett, Emilio Siena, Carrie Johnson, Derek T. O’Hagan, Michal Juraska, and Daniel E. Zak

Subjects

0301 basic medicine, Agonist, medicine.drug_class, medicine.medical_treatment, Antibody titer, Hematology, TLR7, HIV envelope protein, Biology, Virology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Interferon, Immunology, medicine, biology.protein, TLR4, Antibody, Adjuvant, 030215 immunology, medicine.drug

Abstract

Adjuvants have a critical role for improving vaccine efficacy against many pathogens, including HIV. Here, using transcriptional RNA profiling and systems serology, we assessed how distinct innate pathways altered HIV-specific antibody responses in nonhuman primates (NHPs) using 8 clinically based adjuvants. NHPs were immunized with a glycoprotein 140 HIV envelope protein (Env) and insoluble aluminum salts (alum), MF59, or adjuvant nanoemulsion (ANE) coformulated with or without Toll-like receptor 4 (TLR4) and 7 agonists. These were compared with Env administered with polyinosinic-polycytidylic acid:poly-L-lysine, carboxymethylcellulose (pIC:LC) or immune-stimulating complexes. Addition of the TLR4 agonist to alum enhanced upregulation of a set of inflammatory genes, whereas the TLR7 agonist suppressed expression of alum-responsive inflammatory genes and enhanced upregulation of antiviral and interferon (IFN) genes. Moreover, coformulation of the TLR4 or 7 agonists with alum boosted Env-binding titers approximately threefold to 10-fold compared with alum alone, but remarkably did not alter gene expression or enhance antibody titers when formulated with ANE. The hierarchy of adjuvant potency was established after the second of 4 immunizations. In terms of antibody durability, antibody titers decreased ∼10-fold after the final immunization and then remained stable after 65 weeks for all adjuvants. Last, Env-specific Fc-domain glycan structures and a series of antibody effector functions were assessed by systems serology. Antiviral/IFN gene signatures correlated with Fc-receptor binding across all adjuvant groups. This study defines the potency and durability of 8 different clinically based adjuvants in NHPs and shows how specific innate pathways can alter qualitative aspects of Env antibody function.

Published

2017

135. Vaccination establishes clonal relatives of germinal center T cells in the blood of humans

Author

Paul Spearman, Britta Flach, M. Juliana McElrath, Harlan Robins, Sarah E. Gerdts, Miranda S Moore, Stephen C. De Rosa, Georgia D. Tomaras, Frank Schmitz, Alan Aderem, Antje Heit, and Jonathan A. Perkins

Subjects

CD4-Positive T-Lymphocytes, Receptors, CXCR5, 0301 basic medicine, Adolescent, T cell, Palatine Tonsil, Programmed Cell Death 1 Receptor, Immunology, Receptors, Antigen, T-Cell, Article, Immunophenotyping, 03 medical and health sciences, 0302 clinical medicine, Antigen, medicine, Humans, Immunology and Allergy, Child, Research Articles, B cell, AIDS Vaccines, biology, Reverse Transcriptase Polymerase Chain Reaction, Vaccination, T-cell receptor, Germinal center, T-Lymphocytes, Helper-Inducer, Flow Cytometry, Germinal Center, Clone Cells, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Child, Preschool, biology.protein, Antibody, Immunologic Memory, Memory T cell, 030215 immunology

Abstract

Heit et al. describe that in humans, circulating memory T follicular helper cells (cTfh) have a clonal relationship to germinal center Tfh (GCTfh) cells. Upon vaccination, such memory cTfh respond with clonal expansion, activation, and simultaneous expression of a GCTfh-like phenotype., Germinal center T follicular helper cells (GCTfh) in lymphatic tissue are critical for B cell differentiation and protective antibody induction, but whether GCTfh establish clonal derivatives as circulating memory T cells is less understood. Here, we used markers expressed on GCTfh, CXCR5, PD1, and ICOS, to identify potential circulating CXCR5+CD4+ Tfh-like cells (cTfh) in humans, and investigated their functional phenotypes, diversity, and ontogeny in paired donor blood and tonsils, and in blood after vaccination. Based on T cell receptor repertoire analysis, we found that PD-1–expressing cTfh and tonsillar GCTfh cells were clonally related. Furthermore, an activated, antigen-specific PD1+ICOS+ cTfh subset clonally expanded after booster immunization whose frequencies correlated with vaccine-specific serum IgG; these phenotypically resembled GCTfh, and were clonally related to a resting PD1+ICOS− CD4+ memory T cell subset. Thus, we postulate that vaccination establishes clonal relatives of GCTfh within the circulating memory CD4+CXCR5+PD1+ T cell pool that expand upon reencounter of their cognate antigen.

Published

2017

136. Pentavalent HIV-1 vaccine protects against simian-human immunodeficiency virus challenge

Author

Linh Mach, Bette T. Korber, Robert Parks, Hua-Xin Liao, Steven G. Reed, Barton F. Haynes, Amanda Eaton, Georgia D. Tomaras, Richard M. Scearce, Nelson L. Michael, Xiaoying Shen, James F. Theis, Galit Alter, M. Anthony Moody, Kristina K. Peachman, Srivamshi Pittala, Shiu Lok Hu, Guido Ferrari, David C. Montefiori, Harikrishnan Balachandran, Mangala Rao, Sanjay Phogat, Derrick Goodman, Thomas B. Kepler, Laura L. Sutherland, Margaret E. Ackerman, Todd Bradley, Joshua A. Weiner, Kevin O. Saunders, Justin Pollara, Sampa Santra, Jim Tartaglia, Nathan Vandergrift, Abraham Pinter, Todd J. Suscovich, and Chris Bailey-Kellogg

Subjects

0301 basic medicine, Male, Immunogen, viruses, General Physics and Astronomy, HIV Antibodies, HIV Envelope Protein gp120, Serology, law.invention, Epitopes, 0302 clinical medicine, law, Medicine, Phylogeny, Antibody-dependent cell-mediated cytotoxicity, AIDS Vaccines, Multidisciplinary, biology, virus diseases, Recombinant Proteins, 3. Good health, Killer Cells, Natural, 030220 oncology & carcinogenesis, Recombinant DNA, Regression Analysis, Female, Simian Immunodeficiency Virus, Antibody, Protein Binding, Science, General Biochemistry, Genetics and Molecular Biology, Article, Pentavalent vaccine, 03 medical and health sciences, Phagocytosis, Neutralization Tests, Predictive Value of Tests, Animals, Humans, business.industry, General Chemistry, Complement System Proteins, Vaccine efficacy, Virology, Macaca mulatta, 030104 developmental biology, Immunization, Immunology, Mutation, biology.protein, HIV-1, Leukocytes, Mononuclear, business

Abstract

The RV144 Thai trial HIV-1 vaccine of recombinant poxvirus (ALVAC) and recombinant HIV-1 gp120 subtype B/subtype E (B/E) proteins demonstrated 31% vaccine efficacy. Here we design an ALVAC/Pentavalent B/E/E/E/E vaccine to increase the diversity of gp120 motifs in the immunogen to elicit a broader antibody response and enhance protection. We find that immunization of rhesus macaques with the pentavalent vaccine results in protection of 55% of pentavalent-vaccine-immunized macaques from simian–human immunodeficiency virus (SHIV) challenge. Systems serology of the antibody responses identifies plasma antibody binding to HIV-infected cells, peak ADCC antibody titres, NK cell-mediated ADCC and antibody-mediated activation of MIP-1β in NK cells as the four immunological parameters that best predict decreased infection risk that are improved by the pentavalent vaccine. Thus inclusion of additional gp120 immunogens to a pox-prime/protein boost regimen can augment antibody responses and enhance protection from a SHIV challenge in rhesus macaques., A previous human HIV-1 vaccine clinical trial, boosting with HIV envelope protein from two strains, demonstrated moderate vaccine efficacy. Here, Bradley et al. show that a pentavalent HIV envelope protein boost improves protection from viral challenge in non-human primates and they identify immune correlates of protection.

Published

2017

137. Humoral and Innate Antiviral Immunity as Tools to Clear Persistent HIV Infection

Author

Justin Pollara, Guido Ferrari, Barton F. Haynes, and Georgia D. Tomaras

Subjects

0301 basic medicine, Cell, HIV Infections, Adaptive Immunity, HIV Antibodies, Biology, Antibodies, 03 medical and health sciences, 0302 clinical medicine, Immune system, medicine, Humans, cure, Immunology and Allergy, Cytotoxic T cell, innate immunity, latency, Antibody-dependent cell-mediated cytotoxicity, Immunity, Cellular, Innate immune system, Effector, virus diseases, Provirus, Virology, Immunity, Innate, Virus Latency, 3. Good health, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, HIV-1, biology.protein, Supplement Article, Immunotherapy, bispecific antibodies, Antibody, ADCC

Abstract

Human immunodeficiency virus (HIV) type 1 uses the CD4 molecule as its principal receptor to infect T cells. HIV-1 integrates its viral genome into the host cell, leading to persistent infection wherein HIV-1 can remain transcriptionally silent in latently infected CD4+ T cells. On reactivation of replication-competent provirus, HIV-1 envelope glycoproteins (Env) are expressed and accumulate on the cell surface, allowing infected cells to be detected and targeted by endogenous immune responses or immune interventions. HIV-1 Env-specific antibodies have the potential to bind HIV-1 cell surface Env and promote elimination of infected CD4+ T cells by recruiting cytotoxic effector cells, such as natural killer cells, monocytes, and polymorphonuclear cells. Harnessing humoral and innate cellular responses has become one focus of research to develop innovative strategies to recruit and redirect cytotoxic effector cells to eliminate the HIV-1 latently infected CD4+ T-cell reservoir.

Published

2017

138. Randomized, Double-Blind Evaluation of Late Boost Strategies for HIV-Uninfected Vaccine Recipients in the RV144 HIV Vaccine Efficacy Trial

Author

Jaranit Kaewkungwal, Saintedym Wills, Carlos A. DiazGranados, Merlin L. Robb, Poonam Pegu, James Tartaglia, Rv Study Team, Allan C. deCamp, Nakorn Premsri, Alexandra Schuetz, Sanjay Garunathan, Michael A. Eller, Robert J. O'Connell, Nicos Karasavvas, Nathan Vandergrift, Sorachai Nitayaphan, Faruk Sinangil, Jean-Louis Excler, Punnee Pitisuttithum, Chitraporn Karnasuta, Nelson L. Michael, Silvia Ratto-Kim, Georgia D. Tomaras, Sanjay Phogat, Jerome H. Kim, Supachai Rerks-Ngarm, Sheetal Sawant, David C. Montefiori, Prayura Kunasol, Viseth Ngauy, Sandhya Vasan, and Peter Dawson

Subjects

Adult, Male, 0301 basic medicine, Immunization, Secondary, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Placebo, Immunoglobulin G, 03 medical and health sciences, 0302 clinical medicine, Double-Blind Method, Major Article, Humans, Immunology and Allergy, Medicine, 030212 general & internal medicine, HIV vaccine, Neutralizing antibody, AIDS Vaccines, biology, business.industry, Immunogenicity, Thailand, Antibodies, Neutralizing, Healthy Volunteers, Immunity, Humoral, Immunoglobulin A, Vaccination, 030104 developmental biology, Infectious Diseases, AIDSVAX, Immunology, HIV-1, biology.protein, Cytokines, Female, Antibody, business

Abstract

Background The RV144 ALVAC-HIV prime, AIDSVAX B/E boost afforded 60% efficacy against human immunodeficiency virus (HIV) acquisition at 1 year, waning to 31.2% after 3.5 years. We hypothesized that additional vaccinations might augment immune correlates of protection. Methods In a randomized placebo-controlled double-blind study of 162 HIV-negative RV144 vaccine recipients, we evaluated 2 additional boosts, given 6-8 years since RV144 vaccination, for safety and immunogenicity, at weeks 0 and 24. Study groups 1-3 received ALVAC-HIV+AIDSVAX B/E, AIDSVAX B/E, and ALVAC-HIV, respectively, or placebo. Results Vaccines were well tolerated. For groups 1 and 2, plasma immunoglobulin (Ig) G, IgA, and neutralizing antibody responses at week 2 were all significantly higher than 2 weeks after the last RV144 vaccination. IgG titers against glycoprotein (gp) 70V1V2 92TH023 increased 14-fold compared with 2 weeks after the last RV144 vaccination (14069 vs 999; P < .001). Groups 1 and 2 did not differ significantly from each other, whereas group 3 was similar to placebo recipients. Responses in groups 1 and 2 declined by week 24 but were boosted by the second vaccination, albeit at lower magnitude than for week 2. Conclusions In RV144 vaccinees, AIDSVAX B/E with or without ALVAC-HIV 6-8 years after initial vaccination generated higher humoral responses than after RV144, but these responses were short-lived, and their magnitude did not increase with subsequent boost. Clinical Trials Registration NCT01435135.

Published

2017

139. Immunodominance of Antibody Recognition of the HIV Envelope V2 Region in Ig-Humanized Mice

Author

Macdonald Lynn, Kara Anasti, Barton F. Haynes, Ryan Duffy, S. Munir Alam, M. Anthony Moody, Christos A. Kyratsous, Andrew J. Murphy, Krissey E. Lloyd, Cindy M. Bowman, Shi-Mao Xia, Nathan I. Nicely, Richard M. Scearce, Robert Parks, Masayuki Kuraoka, Christina Stolarchuk, Laurent Verkoczy, Garnett Kelsoe, Kevin Wiehe, Xiaoying Shen, Bradley Lockwood, Georgia D. Tomaras, and Sabrina Arora

Subjects

0301 basic medicine, Subdominant, Amino Acid Motifs, Immunology, Immunodominance, HIV Antibodies, HIV Envelope Protein gp120, Biology, Article, Epitope, Epitopes, Mice, 03 medical and health sciences, Immunoglobulin lambda-Chains, Aspartic acid, Animals, Humans, Immunology and Allergy, AIDS Vaccines, 030102 biochemistry & molecular biology, Linear epitope, Glutamic acid, Antibodies, Neutralizing, Virology, 030104 developmental biology, HIV-1, biology.protein, Immunoglobulin heavy chain, Antibody, Immunoglobulin Heavy Chains

Abstract

In the RV144 gp120 HIV vaccine trial, decreased transmission risk was correlated with Abs that reacted with a linear epitope at a lysine residue at position 169 (K169) in the HIV-1 envelope (Env) V2 region. The K169 V2 response was restricted to Abs bearing Vλ rearrangements that expressed aspartic acid/glutamic acid in CDR L2. The AE.A244 gp120 in AIDSVAX B/E also bound to the unmutated ancestor of a V2-glycan broadly neutralizing Ab, but this Ab type was not induced in the RV144 trial. In this study, we sought to determine whether immunodominance of the V2 linear epitope could be overcome in the absence of human Vλ rearrangements. We immunized IgH- and Igκ-humanized mice with the AE.A244 gp120 Env. In these mice, the V2 Ab response was focused on a linear epitope that did not include K169. V2 Abs were isolated that used the same human VH gene segment as an RV144 V2 Ab but paired with a mouse λ L chain. Structural characterization of one of these V2 Abs revealed how the linear V2 epitope could be engaged, despite the lack of aspartic acid/glutamic acid encoded in the mouse repertoire. Thus, despite the absence of the human Vλ locus in these humanized mice, the dominance of Vλ pairing with human VH for HIV-1 Env V2 recognition resulted in human VH pairing with mouse λ L chains instead of allowing otherwise subdominant V2-glycan broadly neutralizing Abs to develop.

Published

2017

140. Complex immune correlates of protection in HIV-1 vaccine efficacy trials

Author

Georgia D. Tomaras and Stanley A. Plotkin

Subjects

Risk, 0301 basic medicine, Immunology, HIV Infections, Human pathogen, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Animals, Humans, Immunology and Allergy, 030212 general & internal medicine, AIDS Vaccines, Clinical Trials as Topic, biology, Transmission (medicine), Vaccination, Disease Models, Animal, 030104 developmental biology, Immune correlates, HIV-1, biology.protein, Antibody

Abstract

Development of an efficacious HIV-1 vaccine is a major priority for improving human health worldwide. Vaccine-mediated protection against human pathogens can be achieved through elicitation of protective innate, humoral, and cellular responses. Identification of specific immune responses responsible for pathogen protection enables vaccine development and provides insights into host defenses against pathogens and the immunological mechanisms that most effectively fight infection. Defining immunological correlates of transmission risk in preclinical and clinical HIV-1 vaccine trials has moved the HIV-1 vaccine development field forward and directed new candidate vaccine development. Immune correlate studies are providing novel hypotheses about immunological mechanisms that may be responsible for preventing HIV-1 acquisition. Recent results from HIV-1 immune correlates work has demonstrated that there are multiple types of immune responses that together, comprise an immune correlate-thus implicating polyfunctional immune control of HIV-1 transmission. An in depth understanding of these complex immunological mechanisms of protection against HIV-1 will accelerate the development of an efficacious HIV-1 vaccine.

Published

2017

141. Vaccine Elicitation of High Mannose-Dependent Neutralizing Antibodies against the V3-Glycan Broadly Neutralizing Epitope in Nonhuman Primates

Author

Robert Parks, Nelson R. Wu, Thomas B. Kepler, Fangping Cai, Tarra Von Holle, Yusuf Vohra, Bette T. Korber, Georgia D. Tomaras, Mattia Bonsignori, Barton F. Haynes, Samuel J. Danishefsky, M. Anthony Moody, Richard M. Scearce, Amanda Eaton, Eden P. Go, Ruijun Zhang, Hua-Xin Liao, Peter K. Park, Sampa Santra, Dan H. Barouch, Nathan I. Nicely, Heather Desaire, Kevin O. Saunders, R. Ryan Meyerhoff, David C. Montefiori, William E. Walkowicz, Kevin Wiehe, Rogier W. Sanders, Kara Anasti, Gary J. Nabel, R. Glenn Overman, Baptiste Aussedat, S. Munir Alam, Norman L. Letvin, Laura L. Sutherland, AII - Infectious diseases, and Medical Microbiology and Infection Prevention

Subjects

Primates, 0301 basic medicine, Glycan, medicine.drug_class, Mannose, HIV Infections, HIV Antibodies, Monoclonal antibody, Article, General Biochemistry, Genetics and Molecular Biology, Epitope, law.invention, Epitopes, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Polysaccharides, law, medicine, Animals, Binding site, lcsh:QH301-705.5, Vaccines, Binding Sites, biology, env Gene Products, Human Immunodeficiency Virus, Antibodies, Monoclonal, virus diseases, Antibodies, Neutralizing, Macaca mulatta, Virology, 3. Good health, carbohydrates (lipids), 030104 developmental biology, chemistry, Immunization, lcsh:Biology (General), HIV-1, Recombinant DNA, biology.protein, Antibody, 030217 neurology & neurosurgery

Abstract

Summary: Induction of broadly neutralizing antibodies (bnAbs) that target HIV-1 envelope (Env) is a goal of HIV-1 vaccine development. A bnAb target is the Env third variable loop (V3)-glycan site. To determine whether immunization could induce antibodies to the V3-glycan bnAb binding site, we repetitively immunized macaques over a 4-year period with an Env expressing V3-high mannose glycans. Env immunizations elicited plasma antibodies that neutralized HIV-1 expressing only high-mannose glycans—a characteristic shared by early bnAb B cell lineage members. A rhesus recombinant monoclonal antibody from a vaccinated macaque bound to the V3-glycan site at the same amino acids as broadly neutralizing antibodies. A structure of the antibody bound to glycan revealed that the three variable heavy-chain complementarity-determining regions formed a cavity into which glycan could insert and neutralized multiple HIV-1 isolates with high-mannose glycans. Thus, HIV-1 Env vaccination induced mannose-dependent antibodies with characteristics of V3-glycan bnAb precursors. : Most bnAb epitopes on HIV-1 Envelope include host glycans, but previous Env vaccines have not induced glycan-dependent antibodies. Saunders et al. describe here the ontogeny, crystal structure with glycan, and virion Man9GlcNAc2-dependent neutralization for glycan-reactive antibodies induced by envelope vaccination. Keywords: HIV, V3 glycan, vaccination, glycan, long-term immunization

Published

2017

142. Unique cellular and humoral immunogenicity profiles generated by aerosol, intranasal, or parenteral vaccination in rhesus macaques

Author

Mario Roederer, Srinivas S. Rao, Diane L. Bolton, Kaimei Song, and Georgia D. Tomaras

Subjects

CD4-Positive T-Lymphocytes, 0301 basic medicine, CD8-Positive T-Lymphocytes, Biology, complex mixtures, Article, Injections, 03 medical and health sciences, 0302 clinical medicine, Immune system, Administration, Inhalation, medicine, Animals, Respiratory system, Administration, Intranasal, Immunity, Cellular, Vaccines, General Veterinary, General Immunology and Microbiology, medicine.diagnostic_test, Immunogenicity, Public Health, Environmental and Occupational Health, respiratory system, Macaca mulatta, Immunity, Humoral, Vaccination, 030104 developmental biology, Infectious Diseases, Bronchoalveolar lavage, medicine.anatomical_structure, Immunization, Immunology, Molecular Medicine, Female, Nasal administration, Bronchoalveolar Lavage Fluid, 030215 immunology, Respiratory tract

Abstract

Respiratory mucosa immunization is capable of eliciting both local and distal mucosal immune responses; it is a potentially powerful yet largely unused modality for vaccination against respiratory diseases. Targeting the lower versus upper airways by aerosol delivery alters the immunogenicity profile of a vaccine, although the full extent of this impact is not well characterized. We set out to define the cellular and humoral response profiles elicited by immunization via intranasal, small aerosol droplets, and large aerosol droplets. We compared responses following adenovirus-vectored vaccination by these routes in macaques, either for the generation of primary immune responses or for the boosting of previously primed systemic responses. Aerosol delivery (4 or 10 μm diameter droplets, addressing lower or upper airways, respectively) generated the highest magnitude lung CD4 and CD8 T-cell responses, reaching 10–30% vaccine-specific levels in bronchoalveolar lavage cells. In contrast, intranasal delivery was less immunogenic with >10-fold lower peak lung T-cell responses. Systemic (blood) T-cell responses were only observed following 4 μm aerosol (and parenteral) immunization, while all delivery routes elicited similar humoral responses. These data demonstrate distinct immune response profiles with each respiratory tract vaccination modality and suggest that small droplet aerosol offers several immunological advantages over other respiratory routes.

Published

2017

143. Neutralization Takes Precedence Over IgG or IgA Isotype-related Functions in Mucosal HIV-1 Antibody-mediated Protection

Author

Hua-Xin Liao, Guido Ferrari, Punnee Pitisuttithum, Thomas N. Denny, Justin Pollara, Nicole L. Yates, Georgia D. Tomaras, Florian Hladik, George M. Shaw, Barton F. Haynes, M. Juliana McElrath, Georgeanna Morton, Katharine Westerberg, Tiffany Hensley-McBain, Shi-Mao Xia, Linh Mach, Sampa Santra, Benjamin Mildenberg, Gregory J. Mize, Ranjit Warrier, Rena D. Astronomo, Jaranit Kaewkungwal, Christina Ochsenbauer, Sorachai Nitayapan, Supachai Rerks-Ngarm, Lamar Ballweber-Fleming, Laura L. Sutherland, and David C. Montefiori

Subjects

0301 basic medicine, Immunoglobulin A, Non-human primate rectal challenge model, Vaginal explants, Simian Acquired Immunodeficiency Syndrome, pIgR, Polymeric IgA receptor, GI, Gastrointestinal, HIV Infections, ADCC, Antibody-dependent cell-mediated cytotoxicity, HIV Antibodies, Immunoglobulin G, sIgA, Secretory IgA, Leukocytes, T/F, Transmitted/founder, CD4bs, CD4 binding site, Antibody-dependent cell-mediated cytotoxicity, biology, General Medicine, Isotype, 3. Good health, mIgA, Monomeric IgA, dIgA, Dimeric IgA, Vagina, Mucosal immunology, Female, Simian Immunodeficiency Virus, Antibody, MPER, Membrane-proximal external region, IDV, Indinivir, IgA, Research Paper, AZT, Zidovudine, ARV, Anti-retroviral, IgG, nnAb, Non-neutralizing antibody, 030106 microbiology, LED, Lowest effective dose, Neutralizing antibodies, General Biochemistry, Genetics and Molecular Biology, snLuc, Secreted nanoluciferase, Antibodies, Immunophenotyping, GalCer, Galactosyl ceramide, 03 medical and health sciences, Neutralization Tests, SC, Secretory component, Animals, Humans, FcRn, Neonatal Fc receptor, Immunity, Mucosal, IMC, Infectious molecular clone, bnAb, Broadly neutralizing antibody, Mucous Membrane, Virology, Antibodies, Neutralizing, Macaca mulatta, Disease Models, Animal, 030104 developmental biology, Immunoglobulin class switching, Immunology, biology.protein, HIV-1, mAb, Monoclonal antibody, GU, Genitourinary, Ex vivo, Biomarkers

Abstract

HIV-1 infection occurs primarily through mucosal transmission. Application of biologically relevant mucosal models can advance understanding of the functional properties of antibodies that mediate HIV protection, thereby guiding antibody-based vaccine development. Here, we employed a human ex vivo vaginal HIV-1 infection model and a rhesus macaque in vivo intrarectal SHIV challenge model to probe the protective capacity of monoclonal broadly-neutralizing (bnAb) and non-neutralizing Abs (nnAbs) that were functionally modified by isotype switching. For human vaginal explants, we developed a replication-competent, secreted NanoLuc reporter virus system and showed that CD4 binding site bnAbs b12 IgG1 and CH31 IgG1 and IgA2 isoforms potently blocked HIV-1JR-CSF and HIV-1Bal26 infection. However, IgG1 and IgA nnAbs, either alone or together, did not inhibit infection despite the presence of FcR-expressing effector cells in the tissue. In macaques, the CH31 IgG1 and IgA2 isoforms infused before high-dose SHIV challenge were completely to partially protective, respectively, while nnAbs (CH54 IgG1 and CH38 mIgA2) were non-protective. Importantly, in both mucosal models IgG1 isotype bnAbs were more protective than the IgA2 isotypes, attributable in part to greater neutralization activity of the IgG1 variants. These findings underscore the importance of potent bnAb induction as a primary goal of HIV-1 vaccine development., Highlights • Only broadly-neutralizing IgG and IgA Abs were protective in two relevant mucosal models of HIV-1 infection. • IgG isotype variants were typically more protective than the IgA isotype variants against vaginal or rectal challenge. • Neutralization rather than IgA-specific functions may afford better protection against mucosal HIV-1 infection. Antibodies are likely to play a key role in preventing HIV-1 infection following mucosal exposure. We used two mucosal models, in conjunction with IgG and IgA versions of the same antibodies, to identify protective antibody properties relevant to vaginal and rectal transmission. Antibodies that can potently neutralize most HIV-1 strains were protective against viral challenge, but those without this capability were non-protective. The IgA antibodies were no more protective than their IgG counterparts even though IgA antibody forms are more abundant in the mucosa. These findings can help prioritize vaccine designs to those that induce potent broadly neutralizing IgG antibodies.

Published

2016

144. Antibody and cellular responses to HIV vaccine regimens with DNA plasmid as compared with ALVAC priming: An analysis of two randomized controlled trials

Author

Allan C. deCamp, Mary Allen, James G. Kublin, M. Juliana McElrath, Mina C. Hosseinipour, Craig Innes, Zoe Moodie, Giuseppe Pantaleo, Jack Heptinstall, Chenchen Yu, Nonhlanhla N. Mkhize, Nicole Frahm, Peter B. Gilbert, Erica Andersen-Nissen, Maurine D. Miner, Linda-Gail Bekker, Fatima Laher, Sarita Naidoo, Glenda Gray, Kristen W. Cohen, Julia Hutter, Hvtn trial teams, Philipp Mann, Lucas Maganga, David C. Montefiori, Lynn Morris, Ralf Wagner, One Dintwe, Georgia D. Tomaras, Nicole L. Yates, Nicole Grunenberg, Stephen R. Walsh, and Michael E Herce

Subjects

Male, HIV Antigens, Physiology, Molecular biology, medicine.medical_treatment, MF59, Antibody Response, HIV Infections, 030204 cardiovascular system & hematology, HIV Antibodies, Gastroenterology, Biochemistry, White Blood Cells, 0302 clinical medicine, Animal Cells, Immune Physiology, Medicine and Health Sciences, 030212 general & internal medicine, HIV vaccine, Immune Response, AIDS Vaccines, Vaccines, Immune System Proteins, T Cells, Immunogenicity, Vaccination, General Medicine, Infectious Diseases, Medicine, Female, Cellular Types, Adjuvant, Plasmids, Research Article, Adult, medicine.medical_specialty, Infectious Disease Control, Immune Cells, Genetic Vectors, Immunology, DNA construction, Microbiology, Antibodies, 03 medical and health sciences, Young Adult, Antigen, Double-Blind Method, Internal medicine, Virology, medicine, Humans, Antigens, Blood Cells, business.industry, Viral vaccines, HIV vaccines, Biology and Life Sciences, Proteins, DNA, Cell Biology, Antibodies, Neutralizing, Research and analysis methods, Regimen, Molecular biology techniques, Antibody Formation, Plasmid Construction, HIV-1, business

Abstract

Background DNA plasmids promise a pragmatic alternative to viral vectors for prime-boost HIV-1 vaccines. We evaluated DNA plasmid versus canarypox virus (ALVAC) primes in 2 randomized, double-blind, placebo-controlled trials in southern Africa with harmonized trial designs. HIV Vaccine Trials Network (HVTN) 111 tested DNA plasmid prime by needle or needleless injection device (Biojector) and DNA plasmid plus gp120 protein plus MF59 adjuvant boost. HVTN 100 tested ALVAC prime and ALVAC plus gp120 protein plus MF59 adjuvant boost (same protein/adjuvant as HVTN 111) by needle. Methods and findings The primary endpoints for this analysis were binding antibody (bAb) responses to HIV antigens (gp120 from strains ZM96, 1086, and TV1; variable 1 and 2 [V1V2] regions of gp120 from strains TV1, 1086, and B.CaseA, as 1086 V1V2 and B.CaseA were correlates of risk in the RV144 efficacy trial), neutralizing antibody (nAb) responses to pseudoviruses TV1c8.2 and MW925.26, and cellular responses to vaccine-matched antigens (envelope [Env] from strains ZM96, 1086, and TV1; and Gag from strains LAI and ZM96) at month 6.5, two weeks after the fourth vaccination. Per-protocol cohorts included vaccine recipients from HVTN 100 (n = 186, 60% male, median age 23 years) enrolled between February 9, 2015, and May 26, 2015 and from HVTN 111 (n = 56, 48% male, median age 24 years) enrolled between June 21, 2016, and July 13, 2017. IgG bAb response rates were 100% to 3 Env gp120 antigens in both trials. Response rates to V1V2 were lower and similar in both trials except to vaccine-matched 1086 V1V2, with rates significantly higher for the DNA-primed regimen than the ALVAC-primed regimen: 96.6% versus 72.7% (difference = 23.9%, 95% CI 15.6%–32.2%, p < 0.001). Among positive responders, bAb net mean fluorescence intensity (MFI) was significantly higher with the DNA-primed regimen than ALVAC-primed for 1086 V1V2 (geometric mean [GM] 2,833.3 versus 1,200.9; ratio = 2.36, 95% CI 1.42–3.92, p < 0.001) and B.CaseA V1V2 (GM 2314.0 versus 744.6, ratio = 3.11, 95% CI 1.51–6.38, p = 0.002). nAb response rates were >98% in both trials, with significantly higher 50% inhibitory dilution (ID50) among DNA-primed positive responders (n = 53) versus ALVAC-primed (n = 182) to tier 1A MW965.26 (GM 577.7 versus 265.7, ratio = 2.17, 95% CI 1.67–2.83, p < 0.001) and to TV1c8.2 (GM 187.3 versus 100.4, ratio = 1.87, 95% CI 1.48–2.35, p < 0.001). CD4+ T-cell response rates were significantly higher with DNA plasmid prime via Biojector than ALVAC prime (91.4% versus 52.8%, difference = 38.6%, 95% CI 20.5%–56.6%, p < 0.001 for ZM96.C; 88.0% versus 43.1%, difference = 44.9%, 95% CI 26.7%–63.1%, p < 0.001 for 1086.C; 55.5% versus 2.2%, difference = 53.3%, 95% CI 23.9%–82.7%, p < 0.001 for Gag LAI/ZM96). The study’s main limitations include the nonrandomized comparison of vaccines from 2 different trials, the lack of data on immune responses to other non–vaccine-matched antigens, and the uncertain clinical significance of the observed immunological effects. Conclusions In this study, we found that further investigation of DNA/protein regimens is warranted given enhanced immunogenicity to the V1V2 correlates of decreased HIV-1 acquisition risk identified in RV144, the only HIV vaccine trial to date to show any efficacy., Zoe Moodie and co-workers study immunological responses with DNA priming in trials of a candidate HIV vaccine., Author summary Why was this study done? HIV remains a major global health problem, especially in sub-Saharan Africa. Developing an efficacious HIV vaccine for subtype C infections, which predominate in southern Africa, is a high priority. Comparing immune responses after DNA plasmid versus viral vector priming in 2 similar subtype C HIV vaccine regimens could help inform the choice of priming strategy to use moving forward. DNA plasmid vaccines are cost-effective, easy to manufacture, and tolerable. What did the researchers do and find? We compared antibody and cellular immune responses to two phase I/II HIV-1 vaccines that differed in their priming mechanism (canarypox virus [ALVAC] vector versus DNA) but were matched in their protein boost and adjuvant. Specifically, we measured T-cell and binding and neutralizing antibody (nAb) responses to the vaccine-matched antigens from the HIV Vaccine Trials Network (HVTN) 100 and HVTN 111 trials. The vaccine regimens with DNA plasmid priming in general stimulated higher binding antibody (bAb) response magnitudes to the variable 1 and 2 (V1V2) correlates of decreased risk in RV144 and higher neutralizing responses to tier 1 viruses than the vaccine regimen with ALVAC priming. Both regimens stimulated high binding and neutralizing response rates, while DNA plasmid priming with MF59 adjuvanted protein boost induced significantly higher CD4+ T-cell response rates than ALVAC priming with MF59 adjuvanted protein boost. What do these findings mean? Our results suggest that DNA plasmid is a superior priming method for stimulating vaccine-matched humoral and cellular responses for HIV vaccine trials using this prime/boost approach. Additional investigations are warranted to optimize DNA plasmid delivery methods, such as electroporation for priming of DNA–protein combinations.

Published

2019

145. Structural Basis for Broad HIV-1 Neutralization by the MPER-Specific Human Broadly Neutralizing Antibody LN01

Author

Christophe Chipot, Timothée Bruel, Georgia D. Tomaras, Antonio Lanzavecchia, Dora Pinto, David C. Montefiori, Giuseppe Pantaleo, Winfried Weissenhorn, Sonia Barbieri, Agostino Riva, Craig Fenwick, Davide Corti, Maciej Tarkowski, Christophe Caillat, Olivier Schwartz, David Jarrossay, Andrea Minola, Michael S. Seaman, Jérémy Dufloo, Chiara Silacci, François Dehez, Serafima Guseva, Xiaoying Shen, Institute for Research in Biomedicine [Ticono, Suisse], Université de Lausanne = University of Lausanne (UNIL), Institut de biologie structurale (IBS - UMR 5075 ), Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), Laboratoire de Physique et Chimie Théoriques (LPCT), Institut de Chimie du CNRS (INC)-Université de Lorraine (UL)-Centre National de la Recherche Scientifique (CNRS), Department of Physics [Illinois at Urbana-Champaign, USA], University of Illinois at Urbana-Champaign [Urbana], University of Illinois System-University of Illinois System, Institute for Biomedicine [Bolzano, Italy] (Eurac Research), Affiliated Institute of the University of Lübeck, Humabs BioMed SA, Duke Human Vaccine Institute [Durham, North Carolina, USA], Université Paris Diderot - Paris 7 (UPD7), Luigi Sacco University Hospital [Milan], Rheumatology Unit, Milano (ASST Fatebenefratelli-Sacco), Virus et Immunité - Virus and immunity, Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), Vaccine Research Institute (VRI), Université Paris-Est Créteil Val-de-Marne - Paris 12 (UPEC UP12), Université Sorbonne Paris Cité (USPC), Beth Israel Deaconess Medical Center, Beth Israel Deaconess Medical Center [Boston] (BIDMC), Harvard Medical School [Boston] (HMS)-Harvard Medical School [Boston] (HMS), Duke University Medical Center, Institute for Research in Biomedicine, ANR-10-INBS-0005,FRISBI,Infrastructure Française pour la Biologie Structurale Intégrée(2010), ANR-17-EURE-0003,CBH-EUR-GS,CBH-EUR-GS(2017), European Project: 681137,H2020,H2020-PHC-2015-single-stage_RTD,EAVI2020(2015), Université de Lausanne (UNIL), Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS), Duke Human Vaccine Institute, and Duke School of Medicine

Subjects

Env, education, Mice, Transgenic, HIV Antibodies, Gp41, Microbiology, Neutralization, Epitope, Article, Cell Line, broadly neutralizing antibody, 03 medical and health sciences, Mice, 0302 clinical medicine, 10E8, Protein Domains, 4E10, Virology, Animals, Humans, membrane interaction, Amino Acid Sequence, 030304 developmental biology, AIDS Vaccines, 0303 health sciences, biology, Germinal center, Fusion protein, Antibodies, Neutralizing, gp41, Transmembrane protein, HIV Envelope Protein gp41, 3. Good health, Cell biology, MPER, [SDV.BBM.BP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biophysics, Disease Models, Animal, HEK293 Cells, [SDV.MP.VIR]Life Sciences [q-bio]/Microbiology and Parasitology/Virology, biology.protein, HIV-1, [SDV.IMM]Life Sciences [q-bio]/Immunology, Parasitology, Paratope, Female, LN01, Antibody, 030217 neurology & neurosurgery

Abstract

Summary Potent and broadly neutralizing antibodies (bnAbs) are the hallmark of HIV-1 protection by vaccination. The membrane-proximal external region (MPER) of the HIV-1 gp41 fusion protein is targeted by the most broadly reactive HIV-1 neutralizing antibodies. Here, we examine the structural and molecular mechansims of neutralization by anti-MPER bnAb, LN01, which was isolated from lymph-node-derived germinal center B cells of an elite controller and exhibits broad neutralization breadth. LN01 engages both MPER and the transmembrane (TM) region, which together form a continuous helix in complex with LN01. The tilted TM orientation allows LN01 to interact simultaneously with the peptidic component of the MPER epitope and membrane via two specific lipid binding sites of the antibody paratope. Although LN01 carries a high load of somatic mutations, most key residues interacting with the MPER epitope and lipids are germline encoded, lending support for the LN01 epitope as a candidate for lineage-based vaccine development., Graphical Abstract, Highlights • bNAb LN01 neutralizes 92% of a 118-strain virus panel • LN01 targets the HIV-1 gp41 MPER, the TM region, and lipids • LN01-complexed MPER forms a continuous helix with TM • Most LN01 paratope residues interacting with MPER-TM and lipids are germline encoded, The gp41 membrane-proximal external region (MPER) is a highly conserved region of HIV-1 Env. Pinto et al. characterize the broadly neutralizing anti-MPER mAb LN01, which shows low autoreactivity. LN01 interacts with a complex epitope comprising MPER, the transmembrane region, and lipids, providing insights for vaccine design.

Published

2019

146. Structural Basis for Broad HIV-1 Neutralization by a Novel MPER-Specific Human Broadly Neutralizing Antibody

Author

Christophe Chipot, Winfried Weissenhorn, Antonio Lanzavecchia, Georgia D. Tomaras, Craig Fenwick, Serafima Guseva, Maciej Tarkowski, Dora Pinto, Chiara Silacci, Christophe Caillat, Sonia Barbieri, David C. Montefiori, Andrea Minola, Agostino Riva, Timothée Bruel, Jérémy Dufloo, Xiaoying Shen, Giuseppe Pantaleo, Olivier Schwartz, David Jarrossay, Michael S. Seaman, François Dehez, Davide Corti, Institute for Research in Biomedicine [Ticino, Switzerland], Università della Svizzera italiana = University of Italian Switzerland (USI), Service of Immunology and Allergy, Department of Medicine, Lausanne University Hospital, Laboratoire d'Enzymologie et Biochimie Structurales (LEBS), Centre National de la Recherche Scientifique (CNRS), International Center for Infectiology Research, Laboratoire de Physique et Chimie Théoriques (LPCT), Institut de Chimie du CNRS (INC)-Université de Lorraine (UL)-Centre National de la Recherche Scientifique (CNRS), Humabs BioMed SA, Duke Human Vaccine Institute [Durham, North Carolina, USA], Department of Cytomorphology, Università degli Studi di Cagliari = University of Cagliari (UniCa)-School of Medicine, Università degli Studi di Milano = University of Milan (UNIMI), Virus et Immunité - Virus and immunity (CNRS-UMR3569), Institut Pasteur [Paris] (IP)-Centre National de la Recherche Scientifique (CNRS), Vaccine Research Institute [Créteil, France] (VRI), Université Paris-Est Créteil Val-de-Marne - Paris 12 (UPEC UP12), Université Paris Diderot, Sorbonne Paris Cité, Paris, France, Université Paris Diderot - Paris 7 (UPD7), Beth Israel Deaconess Medical Center, Beth Israel Deaconess Medical Center [Boston] (BIDMC), Harvard Medical School [Boston] (HMS)-Harvard Medical School [Boston] (HMS), Duke University Medical Center, Institute for Research in Biomedicine, ISMN, CNR, Roma, Institut de biologie structurale (IBS - UMR 5075 ), Centre National de la Recherche Scientifique (CNRS)-Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Direction de Recherche Fondamentale (CEA) (DRF (CEA)), Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA), This work was supported by Collaboration for AIDS Vaccine Discovery grants from the Bill and Melinda Gates Foundation (OPP1114725 to G.P. and A.L. and OPP1032144 to D.C.M.). Part of the project (W.W.) has received funding from the European Union’s Horizon 2020 research and innovation program under grant agreement no. 681137. W.W. acknowledges the Institute Universitaire de France (IUF) and the platforms of the Grenoble Instruct-ERIC center (ISBG, UMS 3518 CNRS-CEA-UGA-EMBL) within the Grenoble Partnership for Structural Biology (PSB). Platform access was supported by FRISBI (ANR-10-INBS-05-02) and GRAL, a project of the University Grenoble Alpes graduate school (Ecoles Universitaires de Recherche) CBH-EUR-GS (ANR-17-EURE-0003). O.S. acknowledges funding from the Institut Pasteur, the ANRS, the Vaccine Research Institute and the Gilead HIV cure program., ANR-10-INBS-0005,FRISBI,Infrastructure Française pour la Biologie Structurale Intégrée(2010), ANR-17-EURE-0003,CBH-EUR-GS,CBH-EUR-GS(2017), European Project: 681137,H2020,H2020-PHC-2015-single-stage_RTD,EAVI2020(2015), Virus et Immunité - Virus and immunity, Institut Pasteur [Paris]-Centre National de la Recherche Scientifique (CNRS), Vaccine Research Institute (VRI), Institute for Biomedicine [Bolzano, Italy] (Eurac Research), Affiliated Institute of the University of Lübeck, Duke Human Vaccine Institute, Duke School of Medicine, School of Medicine-University of Cagliar, Université Grenoble Alpes [2016-2019] (UGA [2016-2019])-Institut de Recherche Interdisciplinaire de Grenoble (IRIG), and Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Commissariat à l'énergie atomique et aux énergies alternatives (CEA)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Env, Gp41, Epitope, Neutralization, broadly neutralizing antibody, 10E8, 4E10, 0502 economics and business, membrane interaction, 050207 economics, 050208 finance, biology, 05 social sciences, Germinal center, Fusion protein, gp41, Transmembrane protein, 3. Good health, Cell biology, MPER, [SDV.BBM.BP]Life Sciences [q-bio]/Biochemistry, Molecular Biology/Biophysics, biology.protein, HIV-1, Paratope, LN01, Antibody

Abstract

International audience; Potent and broadly neutralizing antibodies (bnAbs) are the hallmark of HIV-1 protection by vaccination. The membrane-proximal external region (MPER) of the HIV-1 gp41 fusion protein is targeted by the most broadly reactive HIV-1 neutralizing antibodies. Here, we examine the structural and molecular mechansims of neutralization by anti-MPER bnAb, LN01, which was isolated from lymph-node-derived germinal center B cells of an elite controller and exhibits broad neutralization breadth. LN01 engages both MPER and the transmembrane (TM) region, which together form a continuous helix in complex with LN01. The tilted TM orientation allows LN01 to interact simultaneously with the peptidic component of the MPER epitope and membrane via two specific lipid binding sites of the antibody paratope. Although LN01 carries a high load of somatic mutations, most key residues interacting with the MPER epitope and lipids are germline encoded, lending support for the LN01 epitope as a candidate for lineage-based vaccine development.

Published

2019

147. Correction for Kibler et al., 'Replication-Competent NYVAC-KC Yields Improved Immunogenicity to HIV-1 Antigens in Rhesus Macaques Compared to Nonreplicating NYVAC'

Author

Sanjay Phogat, Song Ding, Robert Parks, Raphael Gottardo, Lindsey Galmin, Kathryn E. Foulds, Guido Ferrari, Karen V. Kibler, Steve Self, Beatriz Perdiguero, Sherry Stanfield-Oakley, Nicole L. Yates, Deborah T. Weiss, Jonathan L. Heeney, Mariano Esteban, David C. Montefiori, Michael S. Seaman, Benedikt Asbach, Giuseppe Pantaleo, Donald N. Forthal, Bertram L. Jacobs, Mario Roederer, Georgia D. Tomaras, James Tartaglia, Juan García-Arriaza, Anthony D. Cristillo, Ralf Wagner, and Susan W. Barnett

Subjects

Virology, Insect Science, Published Erratum, Immunology, Human immunodeficiency virus (HIV), medicine, Creative commons, Biology, medicine.disease_cause, Microbiology, Humanities

Abstract

Author(s): Kibler, Karen V; Asbach, Benedikt; Perdiguero, Beatriz; Garcia-Arriaza, Juan; Yates, Nicole L; Parks, Robert; Stanfield-Oakley, Sherry; Ferrari, Guido; Montefiori, David C; Tomaras, Georgia D; Roederer, Mario; Foulds, Kathryn E; Forthal, Donald N; Seaman, Michael S; Self, Steve; Gottardo, Raphael; Phogat, Sanjay; Tartaglia, James; Barnett, Susan; Cristillo, Anthony D; Weiss, Deborah; Galmin, Lindsey; Ding, Song; Heeney, Jonathan L; Esteban, Mariano; Wagner, Ralf; Pantaleo, Giuseppe; Jacobs, Bertram L | Abstract: Volume 93, no. 3, e01513-18, 2019, https://doi.org/10.1128/JVI.01513-18. The article was originally published on 17 January 2019 with a standard copyright line (“© 2019 American Society for Microbiology. All Rights Reserved.”). We elected to pay for open access for the article after publication, necessitating replacement of the original copyright line with “© 2019 Kibler et al. This is an open-access article distributed under the terms of the Creative Commons Attribution 4.0 International license.” This change was made to the online version of the article on 21 August 2019.

Published

2019

148. Impact of T

Author

Anil, Verma, Brian A, Schmidt, Sonny R, Elizaldi, Nancy K, Nguyen, Korey A, Walter, Zoltan, Beck, Hung V, Trinh, Ashok R, Dinasarapu, Yashavanth Shaan, Lakshmanappa, Niharika N, Rane, Gary R, Matyas, Mangala, Rao, Xiaoying, Shen, Georgia D, Tomaras, Celia C, LaBranche, Keith A, Reimann, David H, Foehl, Johannes S, Gach, Donald N, Forthal, Pamela A, Kozlowski, Rama R, Amara, and Smita S, Iyer

Subjects

AIDS Vaccines, B-Lymphocytes, Immunization, Secondary, virus diseases, Tfh, HIV Antibodies, Saponins, Th1 Cells, Germinal Center, Macaca mulatta, CD4, Lipid A, Adjuvants, Immunologic, adjuvant, Immunoglobulin G, antibody, vaccine, Vaccines and Antiviral Agents, HIV-1, Animals, Humans, Female

Abstract

The results of the RV144 trial demonstrated that vaccination could prevent HIV transmission in humans and that longevity of anti-Env antibodies may be key to this protection. Efforts to improve upon the prime-boost vaccine regimen used in RV144 have indicated that booster immunizations can increase serum anti-Env antibody titers but only transiently. Poor antibody durability hampers efforts to develop an effective HIV-1 vaccine. This study was designed to identify the specific elements involved in the immunological mechanism necessary to produce robust HIV-1-specific antibodies in rhesus macaques. By clearly defining immune-mediated pathways that improve the magnitude and functionality of the anti-HIV-1 antibody response, we will have the foundation necessary for the rational development of an HIV-1 vaccine., Generating durable humoral immunity through vaccination depends upon effective interactions of follicular helper T (Tfh) cells with germinal center (GC) B cells. Th1 polarization of Tfh cells is an important process shaping the success of Tfh-GC B cell interactions by influencing costimulatory and cytokine-dependent Tfh help to B cells. However, the question remains as to whether adjuvant-dependent modulation of Tfh cells enhances HIV-1 vaccine-induced antienvelope (anti-Env) antibody responses. We investigated whether an HIV-1 vaccine platform designed to increase the number of Th1-polarized Tfh cells enhances the magnitude and quality of anti-Env antibodies. Utilizing a novel interferon-induced protein 10 (IP-10)-adjuvanted HIV-1 DNA prime followed by a monophosphoryl lipid A and QS-21 (MPLA+QS-21)-adjuvanted Env protein boost (DIP-10 PALFQ) in macaques, we observed higher anti-Env serum IgG titers with greater cross-clade reactivity, specificity for V1V2, and effector functions than in macaques primed with DNA lacking IP-10 and boosted with MPLA-plus-alum-adjuvanted Env protein (DPALFA) The DIP-10 PALFQ vaccine regimen elicited higher anti-Env IgG1 and lower IgG4 antibody levels in serum, showing for the first time that adjuvants can dramatically impact the IgG subclass profile in macaques. The DIP-10 PALFQ regimen also increased vaginal and rectal IgA antibodies to a greater extent. Within lymph nodes, we observed augmented GC B cell responses and the promotion of Th1 gene expression profiles in GC Tfh cells. The frequency of GC Tfh cells correlated with both the magnitude and avidity of anti-Env serum IgG. Together, these data suggest that adjuvant-induced stimulation of Th1-Tfh cells is an effective strategy for enhancing the magnitude and quality of anti-Env antibody responses. IMPORTANCE The results of the RV144 trial demonstrated that vaccination could prevent HIV transmission in humans and that longevity of anti-Env antibodies may be key to this protection. Efforts to improve upon the prime-boost vaccine regimen used in RV144 have indicated that booster immunizations can increase serum anti-Env antibody titers but only transiently. Poor antibody durability hampers efforts to develop an effective HIV-1 vaccine. This study was designed to identify the specific elements involved in the immunological mechanism necessary to produce robust HIV-1-specific antibodies in rhesus macaques. By clearly defining immune-mediated pathways that improve the magnitude and functionality of the anti-HIV-1 antibody response, we will have the foundation necessary for the rational development of an HIV-1 vaccine.

Published

2019

149. Phase 1 Human Immunodeficiency Virus (HIV) Vaccine Trial to Evaluate the Safety and Immunogenicity of HIV Subtype C DNA and MF59-Adjuvanted Subtype C Envelope Protein

Author

Mina C, Hosseinipour, Craig, Innes, Sarita, Naidoo, Philipp, Mann, Julia, Hutter, Gita, Ramjee, Modulakgotla, Sebe, Lucas, Maganga, Michael E, Herce, Allan C, deCamp, Kyle, Marshall, One, Dintwe, Erica, Andersen-Nissen, Georgia D, Tomaras, Nonhlanhla, Mkhize, Lynn, Morris, Ryan, Jensen, Maurine D, Miner, Giuseppe, Pantaleo, Song, Ding, Olivier, Van Der Meeren, Susan W, Barnett, M Juliana, McElrath, Lawrence, Corey, James G, Kublin, and Daryl, Morris

Subjects

0301 basic medicine, Microbiology (medical), Adult, Squalene, HIV vaccine, MF59, C-DNA, Immunization, Secondary, Polysorbates, Zambia, HIV Infections, HIV Antibodies, Tanzania, 03 medical and health sciences, South Africa, 0302 clinical medicine, Immunogenicity, Vaccine, Medicine, Humans, 030212 general & internal medicine, Articles and Commentaries, AIDS Vaccines, business.industry, Immunogenicity, Biojector, HIV envelope protein, DNA, Virology, Clinical trial, Vaccination, Regimen, 030104 developmental biology, Infectious Diseases, AcademicSubjects/MED00290, DNA prime/protein boost, HIV-1, subtype C, business

Abstract

Background The Pox-Protein Public-Private Partnership is performing a suite of trials to evaluate the bivalent subtype C envelope protein (TV1.C and 1086.C glycoprotein 120) vaccine in the context of different adjuvants and priming agents for human immunodeficiency virus (HIV) type 1 (HIV-1) prevention. Methods In the HIV Vaccine Trials Network 111 trial, we compared the safety and immunogenicity of DNA prime followed by DNA/protein boost with DNA/protein coadministration injected intramuscularly via either needle/syringe or a needle-free injection device (Biojector). One hundred thirty-two healthy, HIV-1–uninfected adults were enrolled from Zambia, South Africa, and Tanzania and were randomized to 1 of 6 arms: DNA prime, protein boost by needle/syringe; DNA and protein coadministration by needle/syringe; placebo by needle/syringe; DNA prime, protein boost with DNA given by Biojector; DNA and protein coadministration with DNA given by Biojector; and placebo by Biojector. Results All vaccinations were safe and well tolerated. DNA and protein coadministration was associated with increased HIV-1 V1/V2 antibody response rate, a known correlate of decreased HIV-1 infection risk. DNA administration by Biojector elicited significantly higher CD4+ T-cell response rates to HIV envelope protein than administration by needle/syringe in the prime/boost regimen (85.7% vs 55.6%; P = .02), but not in the coadministration regimen (43.3% vs 48.3%; P = .61). Conclusions Both the prime/boost and coadministration regimens are safe and may be promising for advancement into efficacy trials depending on whether cellular or humoral responses are desired. Clinical Trials Registration South African National Clinical Trials Registry (application 3947; Department of Health [DoH] no. DOH-27–0715–4917) and ClinicalTrials.gov (NCT02997969)., DNA and protein coadministration was associated with increased human immunodeficiency virus (HIV) type 1 V1/V2 antibody response. Biojector DNA administration elicited significantly greater CD4+ T-cell responses to HIV envelope protein than needle/syringe in the prime/boost but not the coadministration regimen.

Published

2019

150. Immune correlates of the Thai RV144 HIV vaccine regimen in South Africa

Author

Erica Andersen-Nissen, Nicole L. Yates, Erica Lazarus, Surita Roux, Peter B. Gilbert, Xiaoying Shen, John Hural, Linda-Gail Bekker, Craig Innes, Carlos A. DiazGranados, Nonhlanhla N. Mkhize, Fatima Laher, Nelson L. Michael, Edith Swann, M. Juliana McElrath, Georgia D. Tomaras, Abby Isaacs, Stephen C. De Rosa, Carter Lee, Ying Huang, Nicole Grunenberg, Lawrence Corey, Sanjay Phogat, Britta Flach, Glenda Gray, Lynn Morris, Guido Ferrari, Ryan L. Jensen, Faruk Sinangil, Sheetal Sawant, David C. Montefiori, James G. Kublin, April K. Randhawa, and Merlin L. Robb

Subjects

Adult, Male, 0301 basic medicine, HIV Antigens, T-Lymphocytes, T cell, CD40 Ligand, HIV Antibodies, Article, Immunoglobulin G, Placebos, Interferon-gamma, South Africa, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Immune system, Phagocytosis, Antigen, Neutralization Tests, medicine, Humans, 030212 general & internal medicine, HIV vaccine, AIDS Vaccines, Antibody-dependent cell-mediated cytotoxicity, Principal Component Analysis, biology, business.industry, Immunogenicity, Vaccination, Antibody-Dependent Cell Cytotoxicity, virus diseases, General Medicine, Thailand, Immunity, Humoral, 030104 developmental biology, medicine.anatomical_structure, Antibody Formation, Immunology, biology.protein, Interleukin-2, Female, business

Abstract

One of the most successful HIV vaccines to date, the RV144 vaccine tested in Thailand, demonstrated correlates of protection including cross-clade V1V2 immunoglobulin G (IgG) breadth, Env-specific CD4+ T cell polyfunctionality, and antibody-dependent cellular cytotoxicity (ADCC) in vaccinees with low IgA binding. The HIV Vaccine Trials Network (HVTN) 097 trial evaluated this vaccine regimen in South Africa, where clade C HIV-1 predominates. We compared cellular and humoral responses at peak and durability immunogenicity time points in HVTN 097 and RV144 vaccinee samples, and evaluated vaccine-matched and cross-clade immune responses. At peak immunogenicity, HVTN 097 vaccinees exhibited significantly higher cellular and humoral immune responses than RV144 vaccinees. CD4+ T cell responses were more frequent in HVTN 097 irrespective of age and sex, and CD4+ T cell Env-specific functionality scores were higher in HVTN 097. Env-specific CD40L+ CD4+ T cells were more common in HVTN 097, with individuals having this pattern of expression demonstrating higher median antibody responses to HIV-1 Env. IgG and IgG3 binding antibody rates and response magnitude to gp120 vaccine- and V1V2 vaccine-matched antigens were higher or comparable in HVTN 097 than in RV144 ADCC, and ADCP functional antibody responses were elicited in HVTN 097. Env-specific IgG and CD4+ Env responses declined significantly over time in both trials. Overall, cross-clade immune responses associated with protection were better than expected in South Africa, suggesting wider applicability of this regimen.

Published

2019