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

51. Safety and immunogenicity of a replication-defective adenovirus type 5 HIV vaccine in Ad5-seronegative persons: a randomized clinical trial (HVTN 054).

Author

Laurence Peiperl, Cecilia Morgan, Zoe Moodie, Hongli Li, Nina Russell, Barney S Graham, Georgia D Tomaras, Stephen C De Rosa, M Juliana McElrath, and NIAID HIV Vaccine Trials Network

Subjects

Medicine, Science

Abstract

Individuals without prior immunity to a vaccine vector may be more sensitive to reactions following injection, but may also show optimal immune responses to vaccine antigens. To assess safety and maximal tolerated dose of an adenoviral vaccine vector in volunteers without prior immunity, we evaluated a recombinant replication-defective adenovirus type 5 (rAd5) vaccine expressing HIV-1 Gag, Pol, and multiclade Env proteins, VRC-HIVADV014-00-VP, in a randomized, double-blind, dose-escalation, multicenter trial (HVTN study 054) in HIV-1-seronegative participants without detectable neutralizing antibodies (nAb) to the vector. As secondary outcomes, we also assessed T-cell and antibody responses.Volunteers received one dose of vaccine at either 10(10) or 10(11) adenovector particle units, or placebo. T-cell responses were measured against pools of global potential T-cell epitope peptides. HIV-1 binding and neutralizing antibodies were assessed. Systemic reactogenicity was greater at the higher dose, but the vaccine was well tolerated at both doses. Although no HIV infections occurred, commercial diagnostic assays were positive in 87% of vaccinees one year after vaccination. More than 85% of vaccinees developed HIV-1-specific T-cell responses detected by IFN-γ ELISpot and ICS assays at day 28. T-cell responses were: CD8-biased; evenly distributed across the three HIV-1 antigens; not substantially increased at the higher dose; and detected at similar frequencies one year following injection. The vaccine induced binding antibodies against at least one HIV-1 Env antigen in all recipients.This vaccine appeared safe and was highly immunogenic following a single dose in human volunteers without prior nAb against the vector.ClinicalTrials.gov NCT00119873.

Published

2010

52. Polyclonal B cell differentiation and loss of gastrointestinal tract germinal centers in the earliest stages of HIV-1 infection.

Author

Marc C Levesque, M Anthony Moody, Kwan-Ki Hwang, Dawn J Marshall, John F Whitesides, Joshua D Amos, Thaddeus C Gurley, Sallie Allgood, Benjamin B Haynes, Nathan A Vandergrift, Steven Plonk, Daniel C Parker, Myron S Cohen, Georgia D Tomaras, Paul A Goepfert, George M Shaw, Jörn E Schmitz, Joseph J Eron, Nicholas J Shaheen, Charles B Hicks, Hua-Xin Liao, Martin Markowitz, Garnett Kelsoe, David M Margolis, and Barton F Haynes

Subjects

Medicine

Abstract

The antibody response to HIV-1 does not appear in the plasma until approximately 2-5 weeks after transmission, and neutralizing antibodies to autologous HIV-1 generally do not become detectable until 12 weeks or more after transmission. Moreover, levels of HIV-1-specific antibodies decline on antiretroviral treatment. The mechanisms of this delay in the appearance of anti-HIV-1 antibodies and of their subsequent rapid decline are not known. While the effect of HIV-1 on depletion of gut CD4(+) T cells in acute HIV-1 infection is well described, we studied blood and tissue B cells soon after infection to determine the effect of early HIV-1 on these cells.In human participants, we analyzed B cells in blood as early as 17 days after HIV-1 infection, and in terminal ileum inductive and effector microenvironments beginning at 47 days after infection. We found that HIV-1 infection rapidly induced polyclonal activation and terminal differentiation of B cells in blood and in gut-associated lymphoid tissue (GALT) B cells. The specificities of antibodies produced by GALT memory B cells in acute HIV-1 infection (AHI) included not only HIV-1-specific antibodies, but also influenza-specific and autoreactive antibodies, indicating very early onset of HIV-1-induced polyclonal B cell activation. Follicular damage or germinal center loss in terminal ileum Peyer's patches was seen with 88% of follicles exhibiting B or T cell apoptosis and follicular lysis.Early induction of polyclonal B cell differentiation, coupled with follicular damage and germinal center loss soon after HIV-1 infection, may explain both the high rate of decline in HIV-1-induced antibody responses and the delay in plasma antibody responses to HIV-1. Please see later in the article for Editors' Summary.

Published

2009

53. Tat-SF1 is not required for Tat transactivation but does regulate the relative levels of unspliced and spliced HIV-1 RNAs.

Author

Heather B Miller, Kevin O Saunders, Georgia D Tomaras, and Mariano A Garcia-Blanco

Subjects

Medicine, Science

Abstract

BACKGROUND:HIV-1 relies on several host proteins for productive viral transcription. HIV-1 Tat-specific factor 1 (Tat-SF1) is among these cofactors that were identified by in vitro reconstituted transcription reactions with immunodepleted nuclear extracts. At the onset of this work, the prevailing hypothesis was that Tat-SF1 was a required cofactor for the viral regulatory protein, Tat; however, this had not previously been formally tested in vivo. METHODOLOGY/PRINCIPAL FINDINGS:To directly address the involvement of Tat-SF1 in HIV-1 gene expression, we depleted Tat-SF1 in HeLa cells by conventional expression of shRNAs and in T- Rex -293 cells containing tetracycline-inducible shRNAs targeting Tat-SF1. We achieved efficient depletion of Tat-SF1 and demonstrated that this did not affect cell viability. HIV-1 infectivity decreased in Tat-SF1-depleted cells, but only when multiple rounds of infection occurred. Neither Tat-dependent nor basal transcription from the HIV-1 LTR was affected by Tat-SF1 depletion, suggesting that the decrease in infectivity was due to a deficiency at a later step in the viral lifecycle. Finally, Tat-SF1 depletion resulted in an increase in the ratio of unspliced to spliced viral transcripts. CONCLUSIONS/SIGNIFICANCE:Tat-SF1 is not required for regulating HIV-1 transcription, but is required for maintaining the ratios of different classes of HIV-1 transcripts. These new findings highlight a novel, post-transcriptional role for Tat-SF1 in the HIV-1 life cycle.

Published

2009

54. Analysis of the HIV Vaccine Trials Network 702 Phase 2b–3 HIV-1 Vaccine Trial in South Africa Assessing RV144 Antibody and T-Cell Correlates of HIV-1 Acquisition Risk

Author

Zoe Moodie, One Dintwe, Sheetal Sawant, Doug Grove, Yunda Huang, Holly Janes, Jack Heptinstall, Faatima Laher Omar, Kristen Cohen, Stephen C De Rosa, Lu Zhang, Nicole L Yates, Marcella Sarzotti-Kelsoe, Kelly E Seaton, Fatima Laher, Linda Gail Bekker, Mookho Malahleha, Craig Innes, Sheetal Kassim, Nivashnee Naicker, Vaneshree Govender, Modulakgotla Sebe, Nishanta Singh, Philip Kotze, Erica Lazarus, Maphoshane Nchabeleng, Amy M Ward, William Brumskine, Thozama Dubula, April K Randhawa, Nicole Grunenberg, John Hural, Jia Jin Kee, David Benkeser, Yutong Jin, Lindsay N Carpp, Mary Allen, Patricia D’Souza, James Tartaglia, Carlos A DiazGranados, Marguerite Koutsoukos, Peter B Gilbert, James G Kublin, Lawrence Corey, Erica Andersen-Nissen, Glenda E Gray, Georgia D Tomaras, and M Juliana McElrath

Subjects

AIDS Vaccines, Male, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, South Africa, Infectious Diseases, Immunoglobulin G, HIV Seropositivity, Major Article, HIV-1, Humans, Immunology and Allergy, Female

Abstract

Background The ALVAC/gp120 + MF59 vaccines in the HIV Vaccine Trials Network (HVTN) 702 efficacy trial did not prevent human immunodeficiency virus-1 (HIV-1) acquisition. Vaccine-matched immunological endpoints that were correlates of HIV-1 acquisition risk in RV144 were measured in HVTN 702 and evaluated as correlates of HIV-1 acquisition. Methods Among 1893 HVTN 702 female vaccinees, 60 HIV-1–seropositive cases and 60 matched seronegative noncases were sampled. HIV-specific CD4+ T-cell and binding antibody responses were measured 2 weeks after fourth and fifth immunizations. Cox proportional hazards models assessed prespecified responses as predictors of HIV-1 acquisition. Results The HVTN 702 Env-specific CD4+ T-cell response rate was significantly higher than in RV144 (63% vs 40%, P = .03) with significantly lower IgG binding antibody response rate and magnitude to 1086.C V1V2 (67% vs 100%, P Conclusions HVTN 702 and RV144 had distinct immunogenicity profiles. However, both identified significant correlations (univariate or interaction) for IgG V1V2 and polyfunctional CD4+ T cells with HIV-1 acquisition. Clinical Trials Registration . NCT02968849.

Published

2022

55. Cholera toxin B scaffolded, focused SIV V2 epitope elicits antibodies that influence the risk of SIVmac251 acquisition in macaques

Author

Mohammad Arif Rahman, Manuel Becerra-Flores, Yury Patskovsky, Isabela Silva de Castro, Massimiliano Bissa, Shraddha Basu, Xiaoying Shen, LaTonya D. Williams, Sarkis Sarkis, Kombo F. N’guessan, Celia LaBranche, Georgia D. Tomaras, Pyone Pyone Aye, Ronald Veazey, Dominic Paquin-Proulx, Mangala Rao, Genoveffa Franchini, and Timothy Cardozo

Subjects

Immunology, Immunology and Allergy

Abstract

IntroductionAn efficacious HIV vaccine will need to elicit a complex package of innate, humoral, and cellular immune responses. This complex package of responses to vaccine candidates has been studied and yielded important results, yet it has been a recurring challenge to determine the magnitude and protective effect of specific in vivo immune responses in isolation. We therefore designed a single, viral-spike-apical, epitope-focused V2 loop immunogen to reveal individual vaccine-elicited immune factors that contribute to protection against HIV/SIV.MethodWe generated a novel vaccine by incorporating the V2 loop B-cell epitope in the cholera toxin B (CTB) scaffold and compared two new immunization regimens to a historically protective ‘standard’ vaccine regimen (SVR) consisting of 2xDNA prime boosted with 2xALVAC-SIV and 1xΔV1gp120. We immunized a cohort of macaques with 5xCTB-V2c vaccine+alum intramuscularly simultaneously with topical intrarectal vaccination of CTB-V2c vaccine without alum (5xCTB-V2/alum). In a second group, we tested a modified version of the SVR consisting of 2xDNA prime and boosted with 1xALVAC-SIV and 2xALVAC-SIV+CTB-V2/alum, (DA/CTB-V2c/alum).ResultsIn the absence of any other anti-viral antibodies, V2c epitope was highly immunogenic when incorporated in the CTB scaffold and generated highly functional anti-V2c antibodies in the vaccinated animals. 5xCTB-V2c/alum vaccination mediated non-neutralizing ADCC activity and efferocytosis, but produced low avidity, trogocytosis, and no neutralization of tier 1 virus. Furthermore, DA/CTB-V2c/alum vaccination also generated lower total ADCC activity, avidity, and neutralization compared to the SVR. These data suggest that the ΔV1gp120 boost in the SVR yielded more favorable immune responses than its CTB-V2c counterpart. Vaccination with the SVR generates CCR5- α4β7+CD4+ Th1, Th2, and Th17 cells, which are less likely to be infected by SIV/HIV and likely contributed to the protection afforded in this regimen. The 5xCTB-V2c/alum regimen likewise elicited higher circulating CCR5- α4β7+ CD4+ T cells and mucosal α4β7+ CD4+ T cells compared to the DA/CTB-V2c/alum regimen, whereas the first cell type was associated with reduced risk of viral acquisition.ConclusionTaken together, these data suggest that individual viral spike B-cell epitopes can be highly immunogenic and functional as isolated immunogens, although they might not be sufficient on their own to provide full protection against HIV/SIV infection.

Published

2023

56. Development of flow cytometry‐based assays to assess the ability of antibodies to bind to SARS‐CoV‐2‐infected and spike‐transfected cells and mediate NK cell degranulation

Author

Dieter Mielke, Sherry Stanfield‐Oakley, Shalini Jha, Taylor Keyes, Adam Zalaquett, Brooke Dunn, Nicole Rodgers, Thomas Oguin, Greg D. Sempowski, Raquel A. Binder, Gregory C. Gray, Shelly Karuna, Lawrence Corey, John Hural, Georgia D. Tomaras, Justin Pollara, and Guido Ferrari

Subjects

Histology, SARS-CoV-2, Spike Glycoprotein, Coronavirus, COVID-19, Humans, Cell Biology, Antibodies, Viral, Flow Cytometry, Cell Degranulation, Pathology and Forensic Medicine

Abstract

Since the beginning of the SARS-CoV-2 pandemic, antibody responses and antibody effector functions targeting SARS-CoV-2-infected cells have been understudied. Consequently, the role of these types of antibodies in SARS-CoV-2 disease (COVID-19) and immunity is still undetermined. To provide tools to study these responses, we used plasma from SARS-CoV-2-infected individuals (n = 50) and SARS-CoV-2 naive healthy controls (n = 20) to develop four specific and reproducible flow cytometry-based assays: (i) two assessing antibody binding to, and antibody-mediated NK cell degranulation against, SARS-CoV-2-infected cells and (ii) two assessing antibody binding to, and antibody-mediated NK cell degranulation against, SARS-CoV-2 Spike-transfected cells. All four assays demonstrated the ability to detect the presence of these functional antibody responses in a specific and reproducible manner. Interestingly, we found weak to moderate correlations between the four assays (Spearman rho ranged from 0.50 to 0.74), suggesting limited overlap in the responses captured by the individual assays. Lastly, while we initially developed each assay with multiple dilutions in an effort to capture the full relationship between antibody titers and assay outcome, we explored the relationship between fewer antibody dilutions and the full dilution series for each assay to reduce assay costs and improve assay efficiency. We found high correlations between the full dilution series and fewer or single dilutions of plasma. Use of single or fewer sample dilutions to accurately determine the response rates and magnitudes of the responses allows for high-throughput use of these assays platforms to facilitate assessment of antibody responses elicited by SARS-CoV-2 infection and vaccination in large clinical studies.

Published

2022

57. Broadly binding and functional antibodies and persisting memory B cells elicited by HIV vaccine PDPHV

Author

Shixia Wang, Nicole L. Yates, Justin Pollara, Yegor Voronin, Sherry Stanfield-Oakley, Dong Han, Guangnan Hu, Wei Li, Guido Ferrari, Georgia D. Tomaras, and Shan Lu

Subjects

Pharmacology, Infectious Diseases, Immunology, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Pharmacology (medical), Immunologic diseases. Allergy, RC581-607, RC254-282

Abstract

Since publishing our original reports on the safety and immunogenicity of a polyvalent DNA prime-protein boost HIV vaccine (PDPHV) which elicited high titer antibody responses with broad specificity, neutralizing activities to multiple HIV-1 subtypes, as well as poly-functional T cell responses, accumulated findings from other HIV vaccine studies indicated the important roles of Ig isotype distribution, Fc medicated functions and the persistence of memory immune responses which were not studied in previous PDPHV related reports. The current report provides further detailed characterization of these parameters in human volunteers receiving the PDPHV regimen. Antibody responses were assessed using IgG isotype and gp70-V1V2-binding ELISAs, peptide arrays, and antibody-dependent cellular cytotoxicity (ADCC) assays. B cell ELISPOT was used to detect gp120-specific memory B cells. Our results showed that the gp120-specific antibodies were primarily of the IgG1 isotype. HIV-1 envelope protein variable regions V1 and V2 were actively targeted by the antibodies as determined by specific binding to both peptide and V1V2-carrying scaffolds. The antibodies showed potent and broad ADCC responses. Finally, the B cell ELISPOT analysis demonstrated persistence of gp120-specific memory B cells for at least 6 months after the last dose. These data indicate that broadly reactive binding Abs and ADCC responses as well as durable gp120-specific memory B cells were elicited by the polyvalent heterologous prime-boost vaccination regimens and showed great promise as a candidate HIV vaccine.

Published

2022

58. A tool for evaluating heterogeneity in avidity of polyclonal antibodies

Author

Kan Li, Michael Dodds, Rachel L. Spreng, Milite Abraha, Richard H. C. Huntwork, Lindsay C. Dahora, Tinashe Nyanhete, Sheetij Dutta, Ulrike Wille-Reece, Erik Jongert, Katie J. Ewer, Adrian V. S. Hill, Celina Jin, Jennifer Hill, Andrew J. Pollard, S. Munir Alam, Georgia D. Tomaras, and S. Moses Dennison

Subjects

Immunology, Immunology and Allergy

Abstract

Diversity in specificity of polyclonal antibody (pAb) responses is extensively investigated in vaccine efficacy or immunological evaluations, but the heterogeneity in antibody avidity is rarely probed as convenient tools are lacking. Here we have developed a polyclonal antibodies avidity resolution tool (PAART) for use with label-free techniques, such as surface plasmon resonance and biolayer interferometry, that can monitor pAb-antigen interactions in real time to measure dissociation rate constant (kd) for defining avidity. PAART utilizes a sum of exponentials model to fit the dissociation time-courses of pAb-antigens interactions and resolve multiple kd contributing to the overall dissociation. Each kd value of pAb dissociation resolved by PAART corresponds to a group of antibodies with similar avidity. PAART is designed to identify the minimum number of exponentials required to explain the dissociation course and guards against overfitting of data by parsimony selection of best model using Akaike information criterion. Validation of PAART was performed using binary mixtures of monoclonal antibodies of same specificity but differing in kd of the interaction with their epitope. We applied PAART to examine the heterogeneity in avidities of pAb from malaria and typhoid vaccinees, and individuals living with HIV-1 that naturally control the viral load. In many cases, two to three kd were dissected indicating the heterogeneity of pAb avidities. We showcase examples of affinity maturation of vaccine induced pAb responses at component level and enhanced resolution of heterogeneity in avidity when antigen-binding fragments (Fab) are used instead of polyclonal IgG antibodies. The utility of PAART can be manifold in examining circulating pAb characteristics and could inform vaccine strategies aimed to guide the host humoral immune response.

Published

2023

59. Trivalent mosaic or consensus HIV immunogens prime humoral and broader cellular immune responses in adults

Author

Kristen W. Cohen, Andrew Fiore-Gartland, Stephen R. Walsh, Karina Yusim, Nicole Frahm, Marnie L. Elizaga, Janine Maenza, Hyman Scott, Kenneth H. Mayer, Paul A. Goepfert, Srilatha Edupuganti, Giuseppe Pantaleo, Julia Hutter, Daryl E. Morris, Stephen C. De Rosa, Daniel E. Geraghty, Merlin L. Robb, Nelson L. Michael, Will Fischer, Elena E. Giorgi, Harmandeep Malhi, Michael N. Pensiero, Guido Ferrari, Georgia D. Tomaras, David C. Montefiori, Peter B. Gilbert, M. Juliana McElrath, Barton F. Haynes, Bette T. Korber, and Lindsey R. Baden

Subjects

General Medicine

Published

2023

60. Parameter estimation and identifiability analysis for a bivalent analyte model of monoclonal antibody-antigen binding

Author

Kyle Nguyen, Kan Li, Kevin Flores, Georgia D. Tomaras, S. Moses Dennison, and Janice M. McCarthy

Abstract

1AbstractDiscovery research for therapeutic antibodies and vaccine development requires an in-depth understanding of antibody-antigen interactions. Label-free techniques such as Surface Plasmon Resonance (SPR) enable the characterization of biomolecular interactions through kinetics measurements, typically by binding antigens in solution to monoclonal antibodies immobilized on a SPR chip. 1:1 Langmuir binding model is commonly used to fit the kinetics data and derive rate constants. However, in certain contexts it is necessary to immobilize the antigen to the chip and flow the antibodies in solution. One such scenario is the screening of monoclonal antibodies (mAbs) for breadth against a range of antigens, where a bivalent analyte binding model is required to adequately describe the kinetics data unless antigen immobilizaion density is optimized to eliminate avidity effects. A bivalent analyte model is offered in several existing software packages intended for standard throughput SPR instruments, but lacking for high throughput SPR instruments. Existing methods also do not explore multiple local minima and parameter identifiability, issues common in non-linear optimization. Here, we have developed a method for analyzing bivalent analyte binding kinetics directly applicable to high throughput SPR data collected in a non-regenerative fashion, and have included a grid search on initial parameter values and a profile likelihood method to determine parameter identifiability. We fit the data of a broadly neutralizing HIV-1 mAb binding to HIV-1 envelope glycoprotein gp120 to a system of ordinary differential equations modeling bivalent binding. Our identifiability analysis discovered a non-identifiable parameter when data is collected under the standard experimental design for monitoring the association and dissociation phases. We used simulations to determine an improved experimental design, which when executed, resulted in the reliable estimation of all rate constants. These methods will be valuable tools in analyzing the binding of mAbs to an array of antigens to expedite therapeutic antibody discovery research.2Author summaryWhile commercial software programs for the analysis of bivalent analyte binding kinetics are available for low-throughput instruments, they cannot be easily applied to data generated by high-throughput instruments, particularly when the chip surface is not regenerated between titration cycles. Further, existing software does not address common issues in fitting non-linear systems of ordinary differential equations (ODEs) such as optimizations getting trapped in local minima or parameters that are not identifiable. In this work, we introduce a pipeline for analysis of bivalent analyte binding kinetics that 1) allows for the use of high-throughput, non-regenerative experimental designs, 2) optimizes using several sets of initial parameter values to ensure that the algorithm is able to reach the lowest minimum error and 3) applies a profile likelihood method to explore parameter identifiability. In our experimental application of the method, we found that one of the kinetics parameters (kd2) cannot be reliably estimated with the standard length of the dissociation phase. Using simulation and identifiability analysis we determined the optimal length of dissociation so that the parameter can be reliably estimated, saving time and reagents. These methodologies offer robust determination of the kinetics parameters for high-throughput bivalent analyte SPR experiments.

Published

2022

61. Safety, pharmacokinetics and antiviral activity of PGT121, a broadly neutralizing monoclonal antibody against HIV-1: a randomized, placebo-controlled, phase 1 clinical trial

Author

Ramya Nityanandam, Sofia Lupo, Lori F. Maxfield, Georgia D. Tomaras, Alessandra Setaro, Joseph P. Nkolola, Rebecca Zash, Zhilin Chen, Stephen R. Walsh, Dan H. Barouch, Chelsey Bennett, Lisa Sunner, Tyler Cassidy, Kshitij Wagh, Charlotte-Paige Rolle, Frances Priddy, Erica N. Borducchi, Ana N. Monczor, Jinyan Liu, Roberto C. Arduino, Huub C. Gelderblom, Bryan T. Mayer, Diane G. Kanjilal, Abishek Chandrashekar, Elena E. Giorgi, Nicole L. Yates, Edwin DeJesus, Kathryn E. Stephenson, Alicia Sato, Jessica L Ansel, Michael S. Seaman, Joseph Sapiente, C Sabrina Tan, Alan S. Perelson, Bette T. Korber, Allan C. deCamp, Zijin Lin, Boris Julg, Peter Abbink, and Lauren Peter

Subjects

Adult, CD4-Positive T-Lymphocytes, Male, Phases of clinical research, HIV Infections, HIV Envelope Protein gp120, Placebo, Antiviral Agents, Article, General Biochemistry, Genetics and Molecular Biology, Virus, Placebos, Young Adult, Double-Blind Method, Antiretroviral Therapy, Highly Active, Humans, Medicine, Adverse effect, Retrovirus, biology, business.industry, Antibody titer, General Medicine, Middle Aged, Viral Load, Peptide Fragments, Tolerability, Immunology, HIV-1, biology.protein, Female, Immunotherapy, Antibody, business, Viral load, Broadly Neutralizing Antibodies

Abstract

Human immunodeficiency virus (HIV)-1-specific broadly neutralizing monoclonal antibodies are currently under development to treat and prevent HIV-1 infection. We performed a single-center, randomized, double-blind, dose-escalation, placebo-controlled trial of a single administration of the HIV-1 V3-glycan-specific antibody PGT121 at 3, 10 and 30 mg kg–1 in HIV-uninfected adults and HIV-infected adults on antiretroviral therapy (ART), as well as a multicenter, open-label trial of one infusion of PGT121 at 30 mg kg–1 in viremic HIV-infected adults not on ART (no. NCT02960581). The primary endpoints were safety and tolerability, pharmacokinetics (PK) and antiviral activity in viremic HIV-infected adults not on ART. The secondary endpoints were changes in anti-PGT121 antibody titers and CD4+ T-cell count, and development of HIV-1 sequence variations associated with PGT121 resistance. Among 48 participants enrolled, no treatment-related serious adverse events, potential immune-mediated diseases or Grade 3 or higher adverse events were reported. The most common reactions among PGT121 recipients were intravenous/injection site tenderness, pain and headache. Absolute and relative CD4+ T-cell counts did not change following PGT121 infusion in HIV-infected participants. Neutralizing anti-drug antibodies were not elicited. PGT121 reduced plasma HIV RNA levels by a median of 1.77 log in viremic participants, with a viral load nadir at a median of 8.5 days. Two individuals with low baseline viral loads experienced ART-free viral suppression for ≥168 days following antibody infusion, and rebound viruses in these individuals demonstrated full or partial PGT121 sensitivity. The trial met the prespecified endpoints. These data suggest that further investigation of the potential of antibody-based therapeutic strategies for long-term suppression of HIV is warranted, including in individuals off ART and with low viral load., A single dose of a broadly neutralizing, HIV-specific antibody transiently reduces viral load in plasma, and in some individuals is associated with durable virus suppression in the absence of antiretroviral therapy.

Published

2021

62. The transcription factor CREB1 is a mechanistic driver of immunogenicity and reduced HIV-1 acquisition following ALVAC vaccination

Author

Robert Parks, Kelly E. Seaton, Barton F. Haynes, Jim Tartaglia, Jeffrey Tomalka, Muhammad Bilal Latif, Georgia D. Tomaras, Slim Fourati, Ana María González, Adam Pelletier, Nelson L. Michael, Richard A. Koup, Rafick Pierre Sekaly, Peter Wilkinson, Genoveffa Franchini, Merlin L. Robb, Norman L. Letvin, Kathryn Furr, Sampa Santra, Michelle A. Lifton, Nicole L. Yates, Ashish Sharma, and Kevin R. Carlson

Subjects

Innate immune system, Immunogenicity, Immunology, Antigen presentation, Simian immunodeficiency virus, Biology, medicine.disease_cause, Acquired immune system, Vaccine efficacy, Vaccination, Immune system, medicine, Immunology and Allergy

Abstract

Development of effective human immunodeficiency virus 1 (HIV-1) vaccines requires synergy between innate and adaptive immune cells. Here we show that induction of the transcription factor CREB1 and its target genes by the recombinant canarypox vector ALVAC + Alum augments immunogenicity in non-human primates (NHPs) and predicts reduced HIV-1 acquisition in the RV144 trial. These target genes include those encoding cytokines/chemokines associated with heightened protection from simian immunodeficiency virus challenge in NHPs. Expression of CREB1 target genes probably results from direct cGAMP (STING agonist)-modulated p-CREB1 activity that drives the recruitment of CD4+ T cells and B cells to the site of antigen presentation. Importantly, unlike NHPs immunized with ALVAC + Alum, those immunized with ALVAC + MF59, the regimen in the HVTN702 trial that showed no protection from HIV infection, exhibited significantly reduced CREB1 target gene expression. Our integrated systems biology approach has validated CREB1 as a critical driver of vaccine efficacy and highlights that adjuvants that trigger CREB1 signaling may be critical for efficacious HIV-1 vaccines. Understanding the mechanistic basis of vaccine efficacy is crucial to the development of next-generation vaccines. Sekaly and colleagues find that activation of the transcription factor CREB1 by the RV144 HIV-1 vaccine underpins the induction of robust adaptive immunity.

Published

2021

63. Lower SARS-CoV-2–specific humoral immunity in people living with HIV-1 recovered from nonhospitalized COVID-19

Author

Daniel J. Schuster, Shelly Karuna, Caroline Brackett, Martina Wesley, Shuying S. Li, Nathan Eisel, DeAnna Tenney, Sir’Tauria Hilliard, Nicole L. Yates, Jack R. Heptinstall, LaTonya D. Williams, Xiaoying Shen, Robert Rolfe, Robinson Cabello, Lu Zhang, Sheetal Sawant, Jiani Hu, April Kaur Randhawa, Ollivier Hyrien, John A. Hural, Lawrence Corey, Ian Frank, Georgia D. Tomaras, and Kelly E. Seaton

Subjects

Adult, Cross-Sectional Studies, SARS-CoV-2, HIV-1, Humans, COVID-19, General Medicine, Antibodies, Viral, Immunity, Humoral

Abstract

People living with HIV-1 (PLWH) exhibit more rapid antibody decline following routine immunization and elevated baseline chronic inflammation than people without HIV-1 (PWOH), indicating potential for diminished humoral immunity during SARS-CoV-2 infection. Conflicting reports have emerged on the ability of PLWH to maintain humoral protection against SARS-CoV-2 coinfection during convalescence. It is unknown whether peak COVID-19 severity, along with HIV-1 infection status, associates with the quality and quantity of humoral immunity following recovery. Using a cross-sectional observational cohort from the United States and Peru, adults were enrolled 1-10 weeks after SARS-CoV-2 infection diagnosis or symptom resolution. Serum antibodies were analyzed for SARS-CoV-2-specific response rates, binding magnitudes, ACE2 receptor blocking, and antibody-dependent cellular phagocytosis. Overall, (a) PLWH exhibited a trend toward decreased magnitude of SARS-CoV-2-specific antibodies, despite modestly increased overall response rates when compared with PWOH; (b) PLWH recovered from symptomatic outpatient COVID-19 had comparatively diminished immune responses; and (c) PLWH lacked a corresponding increase in SARS-CoV-2 antibodies with increased COVID-19 severity when asymptomatic versus symptomatic outpatient disease was compared.

Published

2022

64. Mind the gap from research laboratory to clinic: Challenges and opportunities for next-generation assays in human diseases

Author

Steven H. Kleinstein, Georgia D. Tomaras, Cesar Boggiano, Jon Warren, David H. O’Connor, M. Patricia D'Souza, Amy Palin, Erin L. Milliken, Hana Golding, and Thomas Calder

Subjects

Technology, Protective immunity, 2019-20 coronavirus outbreak, Tuberculosis, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Human immunodeficiency virus (HIV), Assay, medicine.disease_cause, Medicine, Medical education, General Veterinary, General Immunology and Microbiology, SARS-CoV-2, business.industry, Public Health, Environmental and Occupational Health, HIV, Conference Report, Vaccine delivery, medicine.disease, Influenza, Infectious Diseases, Molecular Medicine, Severe acute respiratory syndrome coronavirus, business, Vaccine

Abstract

Modern vaccinology has experienced major conceptual and technological advances over the past 30 years. These include atomic-level structures driving immunogen design, new vaccine delivery methods, powerful adjuvants, and novel animal models. In addition, utilizing advanced assays to learn how the immune system senses a pathogen and orchestrates protective immunity has been critical in the design of effective vaccines and therapeutics. The National Institute of Allergy and Infectious Diseases of the National Institutes of Health convened a workshop in September 2020 focused on next generation assays for vaccine development (Table 1). The workshop focused on four critical pathogens: severe acute respiratory syndrome coronavirus type 2 (SARS-CoV-2) and human immunodeficiency virus (HIV)—which have no licensed vaccines—and tuberculosis (TB) and influenza—both of which are in critical need of improved vaccines. The goal was to share progress and lessons learned, and to identify any commonalities that can be leveraged to design vaccines and therapeutics.

Published

2021

65. Safety and immunogenicity of an HIV-1 gp120-CD4 chimeric subunit vaccine in a phase 1a randomized controlled trial

Author

Lydiah Mutumbi, Guido Ferrari, Jennifer Schwartz, Charles E. L. B. Davis, Kelli Greene, Robin Flinko, Monica W. Gerber, Jennifer Husson, Raphael Gottardo, Amy Nelson, Joel V Chua, Celia Mahoney, Bruce L. Gilliam, Ka Wing J. Lam, George K. Lewis, Robert C. Gallo, Ilia Prado, Hongmei Gao, Georgia D. Tomaras, Dan Dong, William Fulp, Timothy R. Fouts, Nicole L. Yates, Mohammad M. Sajadi, Anthony L. DeVico, Bryan T. Mayer, and David C. Montefiori

Subjects

Adult, medicine.medical_treatment, 030231 tropical medicine, HIV Infections, HIV Antibodies, HIV Envelope Protein gp120, Article, Epitope, Chimeric subunit vaccine, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, medicine, Animals, Humans, 030212 general & internal medicine, HIV vaccine, Adverse effect, AIDS Vaccines, General Veterinary, General Immunology and Microbiology, biology, business.industry, Immunogenicity, Public Health, Environmental and Occupational Health, HIV, CD4i, Vaccination, Infectious Diseases, Immunization, CD4 Antigens, Vaccines, Subunit, Immunology, HIV-1, biology.protein, Molecular Medicine, Antibody, business, Vaccine, Adjuvant, Full-length single chain (FLSC)

Abstract

A major challenge for HIV vaccine development is to raise anti-envelope antibodies capable of recognizing and neutralizing diverse strains of HIV-1. Accordingly, a full length single chain (FLSC) of gp120-CD4 chimeric vaccine construct was designed to present a highly conserved CD4-induced (CD4i) HIV-1 envelope structure that elicits cross-reactive anti-envelope humoral responses and protective immunity in animal models of HIV infection. IHV01 is the FLSC formulated in aluminum phosphate adjuvant. We enrolled 65 healthy adult volunteers in this first-in-human phase 1a randomized, double-blind, placebo-controlled study with three dose-escalating cohorts (75 µg, 150 µg, and 300 µg doses). Intramuscular injections were given on weeks 0, 4, 8, and 24. Participants were followed for an additional 24 weeks after the last immunization. The overall incidence of adverse events (AEs) was not significantly different between vaccinees and controls. The majority (89%) of vaccine-related AE were mild. The most common vaccine-related adverse event was injection site pain. There were no vaccine-related serious AE, discontinuation due to AE, intercurrent HIV infection, or significant decreases in CD4 count. By the final vaccination, all vaccine recipients developed antibodies against IHV01 and demonstrated anti-CD4i epitope antibodies. The elicited antibodies reacted with CD4 non-liganded Env antigens from diverse HIV-1 strains. Antibody-dependent cell-mediated cytotoxicity against heterologous infected cells or gp120 bound to CD4+ cells was evident in all cohorts as were anti-gp120 T-cell responses. IHV01 vaccine was safe, well tolerated, and immunogenic at all doses tested. The vaccine raised broadly reactive humoral responses against conserved CD4i epitopes on gp120 that mediates antiviral functions.

Published

2021

66. Higher antigen occupancy of high avidity CSP serum antibodies associates with protection against human malaria

Author

Kan Li, Gillian Q. Horn, Milite Abraha, Rachel L. Spreng, S. Munir Alam, Adrian V.S. Hill, Katie Ewer, Georgia D. Tomaras, and S. Moses Dennison

Subjects

Biophysics

Published

2023

67. Impact of adjuvants on the biophysical and functional characteristics of HIV vaccine-elicited antibodies in humans

Author

Shiwei Xu, Margaret C. Carpenter, Rachel L. Spreng, Scott D. Neidich, Sharanya Sarkar, DeAnna Tenney, Derrick Goodman, Sheetal Sawant, Shalini Jha, Brooke Dunn, M. Juliana McElrath, Valerie Bekker, Sarah V. Mudrak, Robin Flinko, George K. Lewis, Guido Ferrari, Georgia D. Tomaras, Xiaoying Shen, and Margaret E. Ackerman

Subjects

Pharmacology, Infectious Diseases, Immunology, Pharmacology (medical)

Abstract

Adjuvants can alter the magnitude, characteristics, and persistence of the humoral response to protein vaccination. HIV vaccination might benefit from tailored adjuvant choice as raising a durable and protective response to vaccination has been exceptionally challenging. Analysis of trials of partially effective HIV vaccines have identified features of the immune response that correlate with decreased risk, including high titers of V1V2-binding IgG and IgG3 responses with low titers of V1V2-binding IgA responses and enhanced Fc effector functions, notably antibody-dependent cellular cytotoxicity (ADCC) and antibody-dependent cellular phagocytosis (ADCP). However, there has been limited opportunity to compare the effect of different adjuvants on these activities in humans. Here, samples from the AVEG015 study, a phase 1 trial in which participants (n = 112) were immunized with gp120SF-2and one of six different adjuvants or combinations thereof were assessed for antibody titer, biophysical features, and diverse effector functions. Three adjuvants, MF59 + MTP-PE, SAF/2, and SAF/2 + MDP, increased the peak magnitude and durability of antigen-specific IgG3, IgA, FcγR-binding responses and ADCP activity, as compared to alum. While multiple adjuvants increased the titer of IgG, IgG3, and IgA responses, none consistently altered the balance of IgG to IgA or IgG3 to IgA. Linear regression analysis identified biophysical features including gp120-specific IgG and FcγR-binding responses that could predict functional activity, and network analysis identified coordinated aspects of the humoral response. These analyses reveal the ability of adjuvants to drive the character and function of the humoral response despite limitations of small sample size and immune variability in this human clinical trial.

Published

2022

68. A clade C HIV-1 vaccine protects against heterologous SHIV infection by modulating IgG glycosylation and T helper response in macaques

Author

Anusmita Sahoo, Andrew T. Jones, Narayanaiah Cheedarla, Sailaja Gangadhara, Vicky Roy, Tiffany M. Styles, Ayalnesh Shiferaw, Korey L. Walter, LaTonya D. Williams, Xiaoying Shen, Gabriel Ozorowski, Wen-Hsin Lee, Samantha Burton, Lasanajak Yi, Xuezheng Song, Zhaohui S. Qin, Cynthia A. Derdeyn, Andrew B. Ward, John D. Clements, Raghavan Varadarajan, Georgia D. Tomaras, Pamela A. Kozlowski, Galit Alter, and Rama Rao Amara

Subjects

AIDS Vaccines, Glycosylation, Tumor Necrosis Factor-alpha, Immunology, Vaccinia virus, T-Lymphocytes, Helper-Inducer, General Medicine, CD8-Positive T-Lymphocytes, Macaca mulatta, Article, Immunoglobulin G, HIV-1, Animals, Simian Immunodeficiency Virus

Abstract

The rising global HIV-1 burden urgently requires vaccines capable of providing heterologous protection. Here, we developed a clade C HIV-1 vaccine consisting of priming with modified vaccinia Ankara (MVA) and boosting with cyclically permuted trimeric gp120 (CycP-gp120) protein, delivered either orally using a needle-free injector or through parenteral injection. We tested protective efficacy of the vaccine against intrarectal challenges with a pathogenic heterologous clade C SHIV infection in rhesus macaques. Both routes of vaccination induced a strong envelope-specific IgG in serum and rectal secretions directed against V1V2 scaffolds from a global panel of viruses with polyfunctional activities. Envelope-specific IgG showed lower fucosylation compared with total IgG at baseline, and most of the vaccine-induced proliferating blood CD4 + T cells did not express CCR5 and α4β7, markers associated with HIV target cells. After SHIV challenge, both routes of vaccination conferred significant and equivalent protection, with 40% of animals remaining uninfected at the end of six weekly repeated challenges with an estimated efficacy of 68% per exposure. Induction of envelope-specific IgG correlated positively with G1FB glycosylation, and G2S2F glycosylation correlated negatively with protection. Vaccine-induced TNF-α + IFN-γ + CD8 + T cells and TNF-α + CD4 + T cells expressing low levels of CCR5 in the rectum at prechallenge were associated with decreased risk of SHIV acquisition. These results demonstrate that the clade C MVA/CycP-gp120 vaccine provides heterologous protection against a tier2 SHIV rectal challenge by inducing a polyfunctional antibody response with distinct Fc glycosylation profile, as well as cytotoxic CD8 T cell response and CCR5-negative T helper response in the rectum.

Published

2022

69. Early and Long-Term HIV-1 Immunogenicity Induced in Macaques by the Combined Administration of DNA, NYVAC and Env Protein-Based Vaccine Candidates: The AUP512 Study

Author

Beatriz Perdiguero, Benedikt Asbach, Carmen E. Gómez, Josef Köstler, Susan W. Barnett, Marguerite Koutsoukos, Deborah E. Weiss, Anthony D. Cristillo, Kathryn E. Foulds, Mario Roederer, David C. Montefiori, Nicole L. Yates, Guido Ferrari, Xiaoying Shen, Sheetal Sawant, Georgia D. Tomaras, Alicia Sato, William J. Fulp, Raphael Gottardo, Song Ding, Jonathan L. Heeney, Giuseppe Pantaleo, Mariano Esteban, Ralf Wagner, and Apollo - University of Cambridge Repository

Subjects

AIDS Vaccines, DNA and NYVAC vectors, B and T cell responses, HIV-1 vaccine, Immunology, Gene Products, env, HIV Infections, DNA, immunogenicity, HIV Antibodies, Antibodies, Neutralizing, Macaca mulatta, combined immunization regimens, recombinant gp120 protein, HIV Seropositivity, HIV-1, Animals, Immunology and Allergy, non-human primates

Abstract

To control HIV infection there is a need for vaccines to induce broad, potent and long-term B and T cell immune responses. With the objective to accelerate and maintain the induction of substantial levels of HIV-1 Env-specific antibodies and, at the same time, to enhance balanced CD4 and CD8 T cell responses, we evaluated the effect of concurrent administration of MF59-adjuvanted Env protein together with DNA or NYVAC vectors at priming to establish if early administration of Env leads to early induction of antibody responses. The primary goal was to assess the immunogenicity endpoint at week 26. Secondary endpoints were (i) to determine the quality of responses with regard to RV144 correlates of protection and (ii) to explore a potential impact of two late boosts. In this study, five different prime/boost vaccination regimens were tested in rhesus macaques. Animals received priming immunizations with either NYVAC or DNA alone or in combination with Env protein, followed by NYVAC + protein or DNA + protein boosts. All regimens induced broad, polyfunctional and well-balanced CD4 and CD8 T cell responses, with DNA-primed regimens eliciting higher response rates and magnitudes than NYVAC-primed regimens. Very high plasma binding IgG titers including V1/V2 specific antibodies, modest antibody-dependent cellular cytotoxicity (ADCC) and moderate neutralization activity were observed. Of note, early administration of the MF59-adjuvanted Env protein in parallel with DNA priming leads to more rapid elicitation of humoral responses, without negatively affecting the cellular responses, while responses were rapidly boosted after repeated immunizations, indicating the induction of a robust memory response. In conclusion, our findings support the use of the Env protein component during priming in the context of an heterologous immunization regimen with a DNA and/or NYVAC vector as an optimized immunization protocol against HIV infection.

Published

2022

70. Safety and Immunogenicity of Ad26-vectored HIV Vaccine with Mosaic Immunogens and a Novel Mosaic Envelope Protein in HIV-uninfected Adults: A Phase 1/2a Study

Author

Daniel J, Stieh, Dan H, Barouch, Christy, Comeaux, Michal, Sarnecki, Kathryn E, Stephenson, Stephen R, Walsh, Sheetal, Sawant, Jack, Heptinstall, Georgia D, Tomaras, James G, Kublin, M Juliana, McElrath, Kristen W, Cohen, Stephen C, De Rosa, Galit, Alter, Guido, Ferrari, David, Montefiori, Philipp, Mann, Steven, Nijs, Katleen, Callewaert, Paul A, Goepfert, Srilatha, Edupuganti, Etienne, Karita, Michael S, Seaman, Lawrence, Corey, Lindsey R, Baden, Maria G, Pau, Hanneke, Schuitemaker, and Frank, Tomaka

Subjects

Infectious Diseases, Immunology and Allergy

Abstract

Background Developing a cross-clade, globally effective HIV vaccine remains crucial for eliminating HIV. Methods This placebo-controlled, double-blind, phase 1/2a study enrolled healthy HIV-uninfected adults at low risk for HIV infection. They were randomized (1:4:1) to receive 4 doses of an adenovirus 26-based HIV-1 vaccine encoding 2 mosaic Gag and Pol, and 2 mosaic Env proteins plus adjuvanted clade C gp140 (referred to here as clade C regimen), bivalent protein regimen (clade C regimen plus mosaic gp140), or placebo. Primary end points were safety and antibody responses. Results In total 152/155 participants (clade C, n = 26; bivalent protein, n = 103; placebo, n = 26) received ≥1 injection. The highest adverse event (AE) severity was grade 3 (local pain/tenderness, 12%, 2%, and 0% of the respective groups; solicited systemic AEs, 19%, 15%, 0%). HIV-1 mosaic gp140-binding antibody titers were 79 595 ELISA units (EU)/mL and 137 520 EU/mL in the clade C and bivalent protein groups (P < .001) after dose 4 and 16 862 EU/mL and 25 162 EU/mL 6 months later. Antibody response breadth against clade C gp140 and clade C/non-clade C gp120 was highest in the bivalent protein group. Conclusions Adding mosaic gp140 to the clade C regimen increased and broadened the elicited immune response without compromising safety or clade C responses. Clinical Trials Registration. NCT02935686.

Published

2022

71. Multi-trial analysis of HIV-1 envelope gp41-reactive antibodies among global recipients of candidate HIV-1 vaccines

Author

Koshlan Mayer-Blackwell, Andrew M. Johnson, Nicole Potchen, Simon S. Minot, Jack Heptinstall, Kelly Seaton, Sheetal Sawant, Xiaoying Shen, Georgia D. Tomaras, Andrew Fiore-Gartland, and James G. Kublin

Subjects

AIDS Vaccines, Immunoglobulin G, Immunology, HIV Seropositivity, HIV-1, Immunology and Allergy, Humans, HIV Infections, HIV Antibodies

Abstract

Many participants in HIV-1 vaccine trials, who have not previously been exposed to or vaccinated against HIV-1, display serum immunoglobulin antibodies that bind the gp41 region of HIV-1 envelope prior to vaccination. Previous studies have hypothesized that these pre-existing antibodies may be cross-reactive and may skew future vaccine responses. In 12 large studies conducted by the HIV Vaccine Trial Network (HVTN) (n=1470 individuals), we find wide variation among participants in the pre-vaccine levels of gp41-reactive antibodies as measured by the binding antibody multiplex assay (BAMA). In the absence of exposure to the gp41 immunogen, anti-gp41 IgG levels were temporally stable over 26-52 weeks in repeated measures of placebo recipients. The analysis revealed that the geometric mean of pre-vaccine anti-gp41 IgG response was greater among participants in South Africa compared with participants in the United States. With gene-level metagenomic sequencing of pre-vaccination fecal samples collected from participants in one trial (HVTN 106), we detected positive associations between pre-vaccine anti-gp41 IgG and abundance of genes from multiple taxa in the Eubacteriales order. The genes most strongly associated with higher baseline anti-gp41 IgG mapped to a clade containing Blautia wexlerae and closely related strains. In trials with vaccine products containing the full or partial portion of gp41 immunogen alongside a gp120 immunogen, we did not find evidence that individuals with higher baseline anti-gp41 IgG had different levels of anti-gp120 IgG after vaccination compared to individuals with lower pre-vaccine anti-gp41 levels (pooled estimate of standardized mean difference -0.01 with a 95% CI [-0.37; 0.34]).

Published

2022

72. In vitro and in vivo inhibition of malaria parasite infection by monoclonal antibodies against Plasmodium falciparum circumsporozoite protein (CSP)

Author

S. Moses Dennison, Kun Luo, Alexis A. Bitzer, Yuanzhang Li, William Washington, Rajeshwer S. Sankhala, Misook Choe, Viseth Ngauy, Alish Giri, Xiaoyan Zou, M. Gordon Joyce, Georgia D. Tomaras, Merricka C. Livingstone, Sheetij Dutta, and Adrian H. Batchelor

Subjects

0301 basic medicine, medicine.drug_class, Science, 030231 tropical medicine, Immunology, Primary Cell Culture, Protozoan Proteins, Antibodies, Protozoan, Diseases, Monoclonal antibody, Microbiology, Epitope, Article, law.invention, Cell Line, 03 medical and health sciences, Mice, 0302 clinical medicine, Antigen, In vivo, law, Malaria Vaccines, parasitic diseases, medicine, Animals, Humans, Malaria, Falciparum, Multidisciplinary, biology, Molecular medicine, Antibodies, Monoclonal, Plasmodium falciparum, biology.organism_classification, Virology, In vitro, Circumsporozoite protein, Mice, Inbred C57BL, 030104 developmental biology, Sporozoites, Recombinant DNA, Hepatocytes, Medicine, Female, Structural biology

Abstract

Plasmodium falciparum malaria contributes to a significant global disease burden. Circumsporozoite protein (CSP), the most abundant sporozoite stage antigen, is a prime vaccine candidate. Inhibitory monoclonal antibodies (mAbs) against CSP map to either a short junctional sequence or the central (NPNA)n repeat region. We compared in vitro and in vivo activities of six CSP-specific mAbs derived from human recipients of a recombinant CSP vaccine RTS,S/AS01 (mAbs 317 and 311); an irradiated whole sporozoite vaccine PfSPZ (mAbs CIS43 and MGG4); or individuals exposed to malaria (mAbs 580 and 663). RTS,S mAb 317 that specifically binds the (NPNA)n epitope, had the highest affinity and it elicited the best sterile protection in mice. The most potent inhibitor of sporozoite invasion in vitro was mAb CIS43 which shows dual-specific binding to the junctional sequence and (NPNA)n. In vivo mouse protection was associated with the mAb reactivity to the NANPx6 peptide, the in vitro inhibition of sporozoite invasion activity, and kinetic parameters measured using intact mAbs or their Fab fragments. Buried surface area between mAb and its target epitope was also associated with in vivo protection. Association and disconnects between in vitro and in vivo readouts has important implications for the design and down-selection of the next generation of CSP based interventions.

Published

2021

73. Safety and immunogenicity of two heterologous HIV vaccine regimens in healthy, HIV-uninfected adults (TRAVERSE): a randomised, parallel-group, placebo-controlled, double-blind, phase 1/2a study

Author

Srilatha Edupuganti, Maria G. Pau, Magda Sobieszczyk, Merlin L. Robb, Johannes P. M. Langedijk, M. Juliana McElrath, Lorenz Scheppler, Michal Sarnecki, Susan Buchbinder, Dan H. Barouch, Ian Frank, Kristen W. Cohen, Joseph P. Nkolola, Stephen R. Walsh, Etienne Karita, Hong Van Tieu, Lawrence Corey, Julie A Ake, Guido Ferrari, Steven Nijs, Kenneth H. Mayer, Karen Buleza, Lindsey R. Baden, Katleen Callewaert, Nadine Rouphael, Galit Alter, Georgia D. Tomaras, Paul A. Goepfert, Dimitri Goedhart, Frank Wegmann, Colleen Kelly, James G. Kublin, Lauren Peter, Trevor A Crowell, David C. Montefiori, Frank Tomaka, Philipp Mann, Michael C. Keefer, Daniel J. Stieh, Zelda Euler, and Hanneke Schuitemaker

Subjects

Adult, Male, 0301 basic medicine, medicine.medical_specialty, Epidemiology, Vaccination schedule, Immunology, HIV Infections, HIV Antibodies, Placebo, Young Adult, 03 medical and health sciences, Immunogenicity, Vaccine, 0302 clinical medicine, Virology, Internal medicine, Humans, Medicine, 030212 general & internal medicine, HIV vaccine, Immunization Schedule, AIDS Vaccines, Reactogenicity, business.industry, Vaccination, Articles, Middle Aged, 030112 virology, Healthy Volunteers, Regimen, Treatment Outcome, Infectious Diseases, Tolerability, HIV-1, Female, business, Intramuscular injection

Abstract

Summary Background Bioinformatically designed mosaic antigens increase the breadth of HIV vaccine-elicited immunity. This study compared the safety, tolerability, and immunogenicity of a newly developed, tetravalent Ad26 vaccine with the previously tested trivalent formulation. Methods This randomised, parallel-group, placebo-controlled, double-blind, phase 1/2a study (TRAVERSE) was done at 11 centres in the USA and one centre in Rwanda. Eligible participants were adults aged 18 to 50 years, who were HIV-uninfected, healthy at screening based on their medical history and a physical examination including laboratory assessment and vital sign measurements, and at low risk of HIV infection in the opinion of study staff, who applied a uniform definition of low-risk guidelines that was aligned across sites. Enrolled participants were randomly assigned at a 2:1 ratio to tetravalent and trivalent groups. Participants in tetravalent and trivalent groups were then further randomly assigned at a 5:1 ratio to adenovirus 26 (Ad26)-vectored vaccine and placebo subgroups. Randomisation was stratified by region (USA and Rwanda) and based on a computer-generated schedule using randomly permuted blocks prepared under the sponsor's supervision. We masked participants and investigators to treatment allocation throughout the study. On day 0, participants received a first injection of tetravalent vaccine (Ad26.Mos4.HIV or placebo) or trivalent vaccine (Ad26.Mos.HIV or placebo), and those injections were repeated 12 weeks later. At week 24, vaccine groups received a third dose of tetravalent or trivalent together with clade C gp140, and this was repeated at week 48, with placebos again administered to the placebo group. All study vaccines and placebo were administered by intramuscular injection in the deltoid muscle. We assessed adverse events in all participants who received at least one study injection (full analysis set) and Env-specific binding antibodies in all participants who received at least the first three vaccinations according to the protocol-specified vaccination schedule, had at least one measured post-dose blood sample collected, and were not diagnosed with HIV during the study (per-protocol set). This study is registered with Clinicaltrials.gov , NCT02788045 . Findings Of 201 participants who were enrolled and randomly assigned, 198 received the first vaccination: 110 were in the tetravalent group, 55 in the trivalent group, and 33 in the placebo group. Overall, 185 (93%) completed two scheduled vaccinations per protocol, 180 (91%) completed three, and 164 (83%) completed four. Solicited, self-limiting local, systemic reactogenicity and unsolicited adverse events were similar in vaccine groups and higher than in placebo groups. All participants in the per-protocol set developed clade C Env binding antibodies after the second vaccination, with higher total IgG titres after the tetravalent vaccine than after the trivalent vaccine (10 413 EU/mL, 95% CI 7284–14 886 in the tetravalent group compared with 5494 EU/mL, 3759–8029 in the trivalent group). Titres further increased after the third and fourth vaccinations, persisting at least through week 72. Other immune responses were also higher with the tetravalent vaccine, including the magnitude and breadth of binding antibodies against a cross-clade panel of Env antigens, and the magnitude of IFNγ ELISPOT responses (median 521 SFU/106 peripheral blood mononuclear cells [PBMCs] in the tetravalent group and median 282 SFU/106 PBMCs in the trivalent group after the fourth vaccination) and Env-specific CD4+ T-cell response rates after the third and fourth vaccinations. No interference by pre-existing Ad26 immunity was identified. Interpretation The tetravalent vaccine regimen was generally safe, well-tolerated, and found to elicit higher immune responses than the trivalent regimen. Regimens that use this tetravalent vaccine component are being advanced into field trials to assess efficacy against HIV-1 infection. Funding National Institutes of Health, Henry M Jackson Foundation for Advancement of Military Medicine and the US Department of Defense, Ragon Institute of MGH, MIT, & Harvard, Bill & Melinda Gates Foundation, and Janssen Vaccines & Prevention.

Published

2020

74. Neonatal Rhesus Macaques Have Distinct Immune Cell Transcriptional Profiles following HIV Envelope Immunization

Author

Barton F. Haynes, Olaf Mueller, Robert Parks, Nathan Vandergrift, Sallie R. Permar, Steven G. Reed, David C. Montefiori, Christopher B. Fox, Sampa Santra, Guido Ferrari, Regina W. Edwards, Todd Bradley, Wilton B. Williams, Wes Rountree, Derek W. Cain, M. Anthony Moody, Xiaoying Shen, Koen K. A. Van Rompay, Laura L. Sutherland, Yunfei Wang, Kevin O. Saunders, Kevin Wiehe, Qifeng Han, Georgia D. Tomaras, and Mark G. Lewis

Subjects

Transcription, Genetic, medicine.medical_treatment, HIV Infections, Lymphocyte Activation, Monocytes, Article, General Biochemistry, Genetics and Molecular Biology, Interleukin 10 receptor, alpha subunit, Transcriptome, Feces, Immune system, Viral Envelope Proteins, medicine, Animals, RNA, Messenger, Receptor, lcsh:QH301-705.5, AIDS Vaccines, biology, Microbiota, virus diseases, Immunosuppression, T-Lymphocytes, Helper-Inducer, Antibodies, Neutralizing, Macaca mulatta, Lymphocyte Subsets, Up-Regulation, Vaccination, Animals, Newborn, Immunization, lcsh:Biology (General), Antibody Formation, Immunology, HIV-1, biology.protein, Antibody

Abstract

SUMMARY HIV-1-infected infants develop broadly neutralizing antibodies (bnAbs) more rapidly than adults, suggesting differences in the neonatal versus adult responses to the HIV-1 envelope (Env). Here, trimeric forms of HIV-1 Env immunogens elicit increased gp120-and gp41-specific antibodies more rapidly in neonatal macaques than adult macaques. Transcriptome analyses of neonatal versus adult immune cells after Env vaccination reveal that neonatal macaques have higher levels of the apoptosis regulator BCL2 in T cells and lower levels of the immunosuppressive interleukin-10 (IL-10) receptor alpha (IL10RA) mRNA transcripts in T cells, B cells, natural killer (NK) cells, and monocytes. In addition, immunized neonatal macaques exhibit increased frequencies of activated blood T follicular helper-like (Tfh) cells compared to adults. Thus, neonatal macaques have transcriptome signatures of decreased immunosuppression and apoptosis compared with adult macaques, providing an immune landscape conducive to early-life immunization prior to sexual debut., In Brief Han et al. demonstrate that infant macaques are capable of responding to HIV vaccines currently studied in human clinical trials. The nature of the neonatal immune system following immunization also suggests a state permissive for generating HIV-1 antibodies. Thus, infant HIV-1 immunization remains a viable strategy to end this pandemic., Graphical abstract

Published

2020

75. Framework Mutations of the 10-1074 bnAb Increase Conformational Stability, Manufacturability, and Stability While Preserving Full Neutralization Activity

Author

Chelsey Bennett, Mcclure Megan J, Georgia D. Tomaras, Michael S. Seaman, Clark Rutilio H, Randal R. Ketchem, J. Alaina Floyd, Kelly E. Seaton, Christine C. Siska, Yan Brodsky, Jeremy M. Shaver, Bryan T. Mayer, Nicole L. Yates, Bruce A. Kerwin, and Alison J. Gillespie

Subjects

analytical biochemistry, HP-SEC, High performance size exclusion chromatography, Protein Conformation, Pharmaceutical Science, CDR, Complementary determining region, 02 engineering and technology, Protein aggregation, HIV Antibodies, 030226 pharmacology & pharmacy, Neutralization, Protein Structure, Secondary, high throughput technology(s), PK, Pharmacokinetic, chemistry.chemical_compound, HC, Heavy chain, Mice, 0302 clinical medicine, Protein structure, protein folding, antibody(s), Gdn-HCl, Guanidine hydrochloride, Chemistry, Protein Stability, fluorescence spectroscopy, 021001 nanoscience & nanotechnology, stabilization, bnAbs, broadly neutralizing antibodies, Monomer, PEG, Polyethylene glycol, DSF, Differential scanning fluorimetry, CDCA, Stability design by covariance analysis, HIV/AIDS, Protein folding, 0210 nano-technology, pharmacokinetics, COGs, Cost of goods, PBS, Phosphate buffered saline, HMW, High molecular weight, Article, physical stability, protein aggregation, 03 medical and health sciences, Residue (chemistry), LC, Light chain, developability, Molecule, Animals, Humans, protein structure, mAb, monoclonal antibody, biopharmaceutical characterization, stability, HEK293 Cells, Mutation, Biophysics, Salt bridge, Broadly Neutralizing Antibodies

Abstract

The broadly neutralizing anti-HIV antibody, 10-1074, is a highly somatically hypermutated IgG1 being developed for prophylaxis in sub-Saharan Africa. A series of algorithms were applied to identify potentially destabilizing residues in the framework of the Fv region. Of 17 residues defined, a variant was identified encompassing 1 light and 3 heavy chain residues, with significantly increased conformational stability while maintaining full neutralization activity. Central to the stabilization was the replacement of the heavy chain residue T108 with R108 at the base of the CDR3 loop which allowed for the formation of a nascent salt bridge with heavy chain residue D137. Three additional mutations were necessary to confer increased conformational stability as evidenced by differential scanning fluorimetry and isothermal chemical unfolding. In addition, we observed increased stability during low pH incubation in which 40% of the parental monomer aggregated while the combinatorial variant showed no increase in aggregation. Incubation of the variant at 100 mg/mL for 6 weeks at 40°C showed a 9-fold decrease in subvisible particles ≥2 μm relative to the parental molecule. Stability-based designs have also translated to improved pharmacokinetics. Together, these data show that increasing conformational stability of the Fab can have profound effects on the manufacturability and long-term stability of a monoclonal antibody.

Published

2020

76. Selection of HIV Envelope Strains for Standardized Assessments of Vaccine-Elicited Antibody-Dependent Cellular Cytotoxicity-Mediating Antibodies

Author

Guido Ferrari, Leigh H. Fisher, Allan C. deCamp, Sherry Stanfield-Oakley, Carolyn Williamson, Georgia D. Tomaras, Barton F. Haynes, Christina Ochsenbauer, Bhavesh Borate, Katelyn Faircloth, Kelli Greene, Dieter Mielke, Hongmei Gao, Marina Tuyishime, David C. Montefiori, Lynn Morris, and Justin Pollara

Subjects

Immunology, HIV Infections, HIV Antibodies, Microbiology, Virus, Neutralization, law.invention, Neutralization Tests, law, Virology, Humans, Phylogeny, AIDS Vaccines, Infectivity, Antibody-dependent cell-mediated cytotoxicity, biology, Antibody-Dependent Cell Cytotoxicity, env Gene Products, Human Immunodeficiency Virus, Genetic Variation, virus diseases, Antibodies, Neutralizing, Clinical trial, Insect Science, HIV-1, Recombinant DNA, biology.protein, Antibody, Hiv envelope

Abstract

Antibody-dependent cellular cytotoxicity (ADCC) has been correlated with reduced risk of HIV-1 infection in several preclinical vaccine trials and the RV144 clinical trial, indicating this is a relevant antibody function to study. Given the diversity of HIV-1, the breadth of vaccine-induced antibody responses is a critical parameter to understand if a universal vaccine is to be realised. Moreover, breadth of ADCC responses can be influenced by different vaccine strategies and regimens, including adjuvants. Therefore, to accurately evaluate ADCC and to compare vaccine regimens, it is important to understand the range of HIV Envelope susceptibility to these responses. These evaluations have been limited because of the complexity of the assay and the lack of a comprehensive panel of viruses for the assessment of these humoral responses. Here, we used twenty-nine HIV-1 infectious molecular clones (IMCs) representing different Envelope subtypes and circulating recombinant forms to characterise susceptibility to ADCC from antibodies in plasma from infected individuals, including thirteen viraemic individuals, ten controllers and six with broadly neutralizing antibody responses. We found in our panel that ADCC susceptibility of the IMCs in our panel did not cluster by subtype, infectivity, level of CD4 downregulation, level of shedding, or neutralization sensitivity. Using partition-around-medoids (PAM) clustering to distinguish smaller groups of IMCs with similar ADCC susceptibility, we identified nested panels of four to eight IMCs that broadly represent the ADCC susceptibility of the entire 29 IMC panel. These panels, together with reagents developed to specifically accommodate circulating viruses at the geographical sites of vaccine trials, will provide a powerful tool to harmonise ADCC data generated across different studies, and detect common themes of ADCC responses elicited by various vaccines. IMPORTANCE Antibody-dependent cellular cytotoxicity (ADCC) responses were found to correlate with reduced risk of infection in the RV144 trial, the only human HIV-1 vaccine to show any efficacy to date. However, reagents to understand the breadth and magnitude of these responses across preclinical and clinical vaccine trials remain underdeveloped. In this study, we characterise HIV-1 infectious molecular clones encoding 29 distinct envelope strains (Env-IMCs) to understand factors which impact virus susceptibility to ADCC and use statistical methods to identify smaller nested panels of four to eight Env-IMCs which accurately represent the full set. These reagents can be used as standardized reagents across studies to fully understand how ADCC may affect efficacy of future vaccine studies, and how studies differed in the breadth of responses developed.

Published

2022

77. Structure and Fc-Effector Function of Rhesusized Variants of Human Anti-HIV-1 IgG1s

Author

William D. Tolbert, Dung N. Nguyen, Marina Tuyishime, Andrew R. Crowley, Yaozong Chen, Shalini Jha, Derrick Goodman, Valerie Bekker, Sarah V. Mudrak, Anthony L. DeVico, George K. Lewis, James F. Theis, Abraham Pinter, M. Anthony Moody, David Easterhoff, Kevin Wiehe, Justin Pollara, Kevin O. Saunders, Georgia D. Tomaras, Margaret Ackerman, Guido Ferrari, and Marzena Pazgier

Subjects

antibody engineering, Immunology, Fc-effector function, HIV, Antibodies, Monoclonal, rhesusization, RC581-607, HIV Antibodies, Immunoglobulin G, HIV-1, Immunology and Allergy, Humans, Immunologic diseases. Allergy, non-human primates, Original Research

Abstract

Passive transfer of monoclonal antibodies (mAbs) of human origin into Non-Human Primates (NHPs), especially those which function predominantly by a Fc-effector mechanism, requires an a priori preparation step, in which the human mAb is reengineered to an equivalent NHP IgG subclass. This can be achieved by changing both the Fc and Fab sequence while simultaneously maintaining the epitope specificity of the parent antibody. This Ab reengineering process, referred to as rhesusization, can be challenging because the simple grafting of the complementarity determining regions (CDRs) into an NHP IgG subclass may impact the functionality of the mAb. Here we describe the successful rhesusization of a set of human mAbs targeting HIV-1 envelope (Env) epitopes involved in potent Fc-effector function against the virus. This set includes a mAb targeting a linear gp120 V1V2 epitope isolated from a RV144 vaccinee, a gp120 conformational epitope within the Cluster A region isolated from a RV305 vaccinated individual, and a linear gp41 epitope within the immunodominant Cys-loop region commonly targeted by most HIV-1 infected individuals. Structural analyses confirm that the rhesusized variants bind their respective Env antigens with almost identical specificity preserving epitope footprints and most antigen-Fab atomic contacts with constant regions folded as in control RM IgG1s. In addition, functional analyses confirm preservation of the Fc effector function of the rhesusized mAbs including the ability to mediate Antibody Dependent Cell-mediated Cytotoxicity (ADCC) and antibody dependent cellular phagocytosis by monocytes (ADCP) and neutrophils (ADNP) with potencies comparable to native macaque antibodies of similar specificity. While the antibodies chosen here are relevant for the examination of the correlates of protection in HIV-1 vaccine trials, the methods used are generally applicable to antibodies for other purposes.

Published

2022

78. Lower SARS-CoV-2-Specific Humoral Immunity in People Living With HIV-1 Recovered From Symptomatic Non-Hospitalized COVID-19

Author

Daniel J. Schuster, Shelly T. Karuna, Caroline Brackett, Martina Wesley, Shuying S. Li, Nathan Eisel, DeAnna Tenney, Sir'Tauria Hilliard, Nicole L. Yates, Jack Heptinstall, LaTonya Williams, Xiaoying Shen, Robert Rolfe, Robinson Cabello, Lu Zhang, Sheetal Sawant, Jiani Hu, April Randhawa, Ollivier Hyrien, John Hural, Lawrence Corey, Ian Frank, Georgia D. Tomaras, and Kelly E. Seaton

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

79. Pharmacokinetic Serum Concentrations of VRC01 Correlate with Prevention of HIV-1 Acquisition

Author

Kelly E. Seaton, Yunda Huang, Shelly T. Karuna, Jack Heptinstall, Caroline Brackett, Kelvin Chiong, Yuanyuan Zhang, Nicole L. Yates, Mark Sampson, Erika Rudnicki, Michal Juraska, Allan C. deCamp, Paul T. Edlefsen, James I. Mullins, Carolyn Williamson, Raabya Rossenkhan, Elena E. Giorgi, Avi Kenny, Heather Angier, April Randhawa, Michelle Rojas, Macella Sarzotti-Kelsoe, Lu Zhang, Sheetal Sawant, Adrian McDermont, John R. Mascola, John Hural, Juliana McElrath, Philip Andrew, Jose A. Hidalgo, Jesse Clark, Fatima Laher, Catherine Orrell, Ian Frank, Pedro Gonzales, Srilatha Edupuganti, Nyaradzo Mgodi, Lawrence Corey, Lynn Morris, David C. Montefiori, Myron Cohen, Peter B. Gilbert, and Georgia D. Tomaras

Subjects

History, Polymers and Plastics, Business and International Management, Industrial and Manufacturing Engineering

Published

2022

80. Recombinant Simian Varicella Virus-Simian Immunodeficiency Virus Vaccine Induces T and B Cell Functions and Provides Partial Protection against Repeated Mucosal SIV Challenges in Rhesus Macaques

Author

Bapi Pahar, Wayne Gray, Marissa Fahlberg, Brooke Grasperge, Meredith Hunter, Arpita Das, Christopher Mabee, Pyone Pyone Aye, Faith Schiro, Krystle Hensley, Aneeka Ratnayake, Kelly Goff, Celia LaBranche, Xiaoying Shen, Georgia D. Tomaras, C. Todd DeMarco, David Montefiori, Patricia Kissinger, Preston A. Marx, and Vicki Traina-Dorge

Subjects

Vaccines, Synthetic, Simian Acquired Immunodeficiency Syndrome, SAIDS Vaccines, Antibodies, Viral, Macaca mulatta, Antibodies, Neutralizing, rhesus macaque, vaccine, varicella virus-vector, SIV, protection, Chickenpox, Infectious Diseases, Virology, Animals, Cytokines, Female, Simian Immunodeficiency Virus

Abstract

HIV vaccine mediated efficacy, using an expanded live attenuated recombinant varicella virus-vectored SIV rSVV-SIVgag/env vaccine prime with adjuvanted SIV-Env and SIV-Gag protein boosts, was evaluated in a female rhesus macaques (RM) model against repeated intravaginal SIV challenges. Vaccination induced anti-SIV IgG responses and neutralizing antibodies were found in all vaccinated RMs. Three of the eight vaccinated RM remained uninfected (vaccinated and protected, VP) after 13 repeated challenges with the pathogenic SIVmac251-CX-1. The remaining five vaccinated and infected (VI) macaques had significantly reduced plasma viral loads compared with the infected controls (IC). A significant increase in systemic central memory CD4+ T cells and mucosal CD8+ effector memory T-cell responses was detected in vaccinated RMs compared to controls. Variability in lymph node SIV-Gag and Env specific CD4+ and CD8+ T cell cytokine responses were detected in the VI RMs while all three VP RMs had more durable cytokine responses following vaccination and prior to challenge. VI RMs demonstrated predominately SIV-specific monofunctional cytokine responses while the VP RMs generated polyfunctional cytokine responses. This study demonstrates that varicella virus-vectored SIV vaccination with protein boosts induces a 37.5% efficacy rate against pathogenic SIV challenge by generating mucosal memory, virus specific neutralizing antibodies, binding antibodies, and polyfunctional T-cell responses.

Published

2022

81. Neutralization titer biomarker for antibody-mediated prevention of HIV-1 acquisition

Author

Peter B. Gilbert, Yunda Huang, Allan C. deCamp, Shelly Karuna, Yuanyuan Zhang, Craig A. Magaret, Elena E. Giorgi, Bette Korber, Paul T. Edlefsen, Raabya Rossenkhan, Michal Juraska, Erika Rudnicki, Nidhi Kochar, Ying Huang, Lindsay N. Carpp, Dan H. Barouch, Nonhlanhla N. Mkhize, Tandile Hermanus, Prudence Kgagudi, Valerie Bekker, Haajira Kaldine, Rutendo E. Mapengo, Amanda Eaton, Elize Domin, Carley West, Wenhong Feng, Haili Tang, Kelly E. Seaton, Jack Heptinstall, Caroline Brackett, Kelvin Chiong, Georgia D. Tomaras, Philip Andrew, Bryan T. Mayer, Daniel B. Reeves, Magdalena E. Sobieszczyk, Nigel Garrett, Jorge Sanchez, Cynthia Gay, Joseph Makhema, Carolyn Williamson, James I. Mullins, John Hural, Myron S. Cohen, Lawrence Corey, David C. Montefiori, and Lynn Morris

Subjects

HIV-1, Animals, Humans, HIV Infections, General Medicine, HIV Antibodies, Antibodies, Neutralizing, General Biochemistry, Genetics and Molecular Biology, Adenosine Monophosphate, Biomarkers, Broadly Neutralizing Antibodies

Abstract

The Antibody Mediated Prevention trials showed that the broadly neutralizing antibody (bnAb) VRC01 prevented acquisition of human immunodeficiency virus-1 (HIV-1) sensitive to VRC01. Using AMP trial data, here we show that the predicted serum neutralization 80% inhibitory dilution titer (PT80) biomarker—which quantifies the neutralization potency of antibodies in an individual’s serum against an HIV-1 isolate—can be used to predict HIV-1 prevention efficacy. Similar to the results of nonhuman primate studies, an average PT80 of 200 (meaning a bnAb concentration 200-fold higher than that required to reduce infection by 80% in vitro) against a population of probable exposing viruses was estimated to be required for 90% prevention efficacy against acquisition of these viruses. Based on this result, we suggest that the goal of sustained PT80 >200 against 90% of circulating viruses can be achieved by promising bnAb regimens engineered for long half-lives. We propose the PT80 biomarker as a surrogate endpoint for evaluation of bnAb regimens, and as a tool for benchmarking candidate bnAb-inducing vaccines.

Published

2021

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

Author

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

Subjects

Pharmacology, Messenger RNA, Vaccines, Protein vaccines, biology, Chemistry, Immunology, Human immunodeficiency virus (HIV), Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC581-607, medicine.disease_cause, Virology, Antibodies, Infectious Diseases, RNA vaccines, medicine, biology.protein, Pharmacology (medical), Antibody, Immunologic diseases. Allergy, Author Correction, Nucleoside, RC254-282

Abstract

The 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 show that mRNA-LNP immunization compared to protein immunization elicits either the same or superior magnitude and breadth of HIV-1 Env-specific polyfunctional antibodies. Immunization with mRNA-LNP encoding Zika premembrane and envelope or HIV-1 Env gp160 induces durable neutralizing antibodies for at least 41 weeks. Doses of mRNA-LNP as low as 5 μg are 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

2021

83. Salmonella Typhi Vi capsule prime-boost vaccination induces convergent and functional antibody responses

Author

S. Munir Alam, Lisa Stockdale, Jennifer Hill, S. Moses Dennison, M K Verheul, Celina Jin, Sjoerd Rijpkema, Guy Cavet, Yvonne Leung, Katherine L. Williams, Leonard D. Spicer, Lindsay C. Dahora, Eldar Giladi, Georgia D. Tomaras, Benjamin G. Bobay, Sheetal Sawant, Dongkyoon Kim, and Andrew J. Pollard

Subjects

biology, Immunology, Toxoid, General Medicine, Salmonella typhi, complex mixtures, Virology, Article, Epitope, Affinity maturation, Immunization, Antibody Repertoire, biology.protein, Avidity, Antibody

Abstract

Vaccine development to prevent Salmonella Typhi infections has accelerated over the past decade, resulting in licensure of new vaccines, which use the Vi polysaccharide (Vi PS) of the bacterium conjugated to an unrelated carrier protein as the active component. Antibodies elicited by these vaccines are important for mediating protection against typhoid fever. However, the characteristics of protective and functional Vi antibodies are unknown. In this study, we investigated the human antibody repertoire, avidity maturation, epitope specificity, and function after immunization with a single dose of Vi-tetanus toxoid conjugate vaccine (Vi-TT) and after a booster with plain Vi PS (Vi-PS). The Vi-TT prime induced an IgG1-dominant response, whereas the Vi-TT prime followed by the Vi-PS boost induced IgG1 and IgG2 antibody production. B cells from recipients who received both prime and boost showed evidence of convergence, with shared V gene usage and CDR3 characteristics. The detected Vi antibodies showed heterogeneous avidity ranging from 10 μM to 500 pM, with no evidence of affinity maturation after the boost. Vi-specific antibodies mediated Fc effector functions, which correlated with antibody dissociation kinetics but not with association kinetics. We identified antibodies induced by prime and boost vaccines that recognized subdominant epitopes, indicated by binding to the de–O-acetylated Vi backbone. These antibodies also mediated Fc-dependent functions, such as complement deposition and monocyte phagocytosis. Defining strategies on how to broaden epitope targeting for S. Typhi Vi and enriching for antibody Fc functions that protect against typhoid fever will advance the design of high-efficacy Vi vaccines for protection across diverse populations.

Published

2021

84. Defining variant-resistant epitopes targeted by SARS-CoV-2 antibodies: A global consortium study

Author

Yanan Lu, Timothy C. Germann, Adrian Enriquez, Ruben Diaz Avalos, Marit J. van Gils, Ana G. Lujan Hernandez, Yoann Aldon, Guojun Lang, Mohammad M. Sajadi, Elizabeth Feeney, John Ingraham, Georgia D. Tomaras, Milite Abraha, Junli Liu, Jacob Glanville, S. Moses Dennison, Minsoo Kim, Erica Ollmann Saphire, Sawsan Youssef, Ross S. Federman, Gillian Q. Horn, Bingqing Shen, Sean Hui, Anne L. Palser, Joseph M. Fernandez, Gevorg Grigoryan, Vamseedhar Rayaprolu, David D. Ho, Jieyun Yin, Sharon L. Schendel, Jian Yu, Haoyang Li, Shelly J. Krebs, Qian Zhang, Ronald R. Cobb, Colin Mann, Eduardo Olmedillas, Rogier W. Sanders, Robin Green, Hyeong Mi Kim, Tierra Buck, Dawid Zyla, Hanif Ali, Paul Kellam, Terence H. Rabbitts, Diptiben V. Parekh, Anna J. MacCamy, Cheolmin Kim, Kuan-Ying A. Huang, Milan T. Tomic, Andrew T. McGuire, Tom Z. Yuan, Chitra Hariharan, Zahra Rikhtegaran Tehrani, Bjoern Peters, Xiaoying Yu, Sooyoung Lee, CoVIC-DB team, Kan Li, Leonidas Stamatatos, Cheuk Lun Leung, Chao Kong, Michelle Zandonatti, Fei Lan, Yongcong Tan, Aaron K. Sato, Kathryn M. Hastie, Liang Schweizer, Sanja Aracic, Jonne L. Snitselaar, Weidong Jiang, Kelly Shaffer, Jimin Seo, Daniel Bedinger, Medical Microbiology and Infection Prevention, and AII - Infectious diseases

Subjects

2019-20 coronavirus outbreak, Multidisciplinary, Coronavirus disease 2019 (COVID-19), biology, Immunodominant Epitopes, SARS-CoV-2, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Protein domain, COVID-19, Antibodies, Viral, Virology, Antibodies, Neutralizing, Epitope, Article, Epitope mapping, Protein Domains, Spike Glycoprotein, Coronavirus, biology.protein, Humans, Antibody, Antigens, Viral, Epitope Mapping, Protein Binding

Abstract

Antibody-based therapeutics and vaccines are essential to combat COVID-19 morbidity and mortality after severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Multiple mutations in SARS-CoV-2 that could impair antibody defenses propagated in human-to-human transmission and spillover or spillback events between humans and animals. To develop prevention and therapeutic strategies, we formed an international consortium to map the epitope landscape on the SARS-CoV-2 spike protein, defining and structurally illustrating seven receptor binding domain (RBD)–directed antibody communities with distinct footprints and competition profiles. Pseudovirion-based neutralization assays reveal spike mutations, individually and clustered together in variants, that affect antibody function among the communities. Key classes of RBD-targeted antibodies maintain neutralization activity against these emerging SARS-CoV-2 variants. These results provide a framework for selecting antibody treatment cocktails and understanding how viral variants might affect antibody therapeutic efficacy.

Published

2021

85. Safety and antiviral activity of triple combination broadly neutralizing monoclonal antibody therapy against HIV-1: a phase 1 clinical trial

Author

Boris Julg, Kathryn E. Stephenson, Kshitij Wagh, Sabrina C. Tan, Rebecca Zash, Stephen Walsh, Jessica Ansel, Diane Kanjilal, Joseph Nkolola, Victoria E. K. Walker-Sperling, Jasper Ophel, Katherine Yanosick, Erica N. Borducchi, Lori Maxfield, Peter Abbink, Lauren Peter, Nicole L. Yates, Martina S. Wesley, Tom Hassell, Huub C. Gelderblom, Allen deCamp, Bryan T. Mayer, Alicia Sato, Monica W. Gerber, Elena E. Giorgi, Lucio Gama, Richard A. Koup, John R. Mascola, Ana Monczor, Sofia Lupo, Charlotte-Paige Rolle, Roberto Arduino, Edwin DeJesus, Georgia D. Tomaras, Michael S. Seaman, Bette Korber, and Dan H. Barouch

Subjects

Adult, HIV Seropositivity, HIV-1, Antibodies, Monoclonal, Humans, HIV Infections, General Medicine, Viremia, HIV Antibodies, Antibodies, Neutralizing, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Broadly Neutralizing Antibodies

Abstract

HIV-1 therapy with single or dual broadly neutralizing antibodies (bNAbs) has shown viral escape, indicating that at least a triple bNAb therapy may be needed for robust suppression of viremia. We performed a two-part study consisting of a single-center, randomized, double-blind, dose-escalation, placebo-controlled first-in-human trial of the HIV-1 V2-glycan-specific antibody PGDM1400 alone or in combination with the V3-glycan-specific antibody PGT121 in 24 adults without HIV in part 1, as well as a multi-center, open-label trial of the combination of PGDM1400, PGT121 and the CD4-binding-site antibody VRC07-523LS in five viremic adults living with HIV not on antiretroviral therapy (ART) in part 2 (NCT03205917). The primary endpoints were safety, tolerability and pharmacokinetics for both parts and antiviral activity among viremic adults living with HIV and not on ART for part 2 of the study. The secondary endpoints were changes in CD4+ T cell counts and development of HIV-1 sequence variations associated with PGDM1400, PGT121 and VRC07-523LS resistance in part 2. Intravenously administered PGDM1400 was safe and well-tolerated at doses up to 30 mg kg−1 and when given in combination with PGT121 and VRC07-523LS. A single intravenous infusion of 20 mg kg−1 of each of the three antibodies reduced plasma HIV RNA levels in viremic individuals by a maximum mean of 2.04 log10 copies per ml; however, viral rebound occurred in all participants within a median of 20 days after nadir. Rebound viruses demonstrated partial to complete resistance to PGDM1400 and PGT121 in vitro, whereas susceptibility to VRC07-523LS was preserved. Viral rebound occurred despite mean VRC07-523LS serum concentrations of 93 µg ml−1. The trial met the pre-specified endpoints. Our data suggest that future bNAb combinations likely need to achieve broad antiviral activity, while also maintaining high serum concentrations, to mediate viral control.

Published

2021

86. Author response: Monocyte-derived transcriptome signature indicates antibody-dependent cellular phagocytosis as a potential mechanism of vaccine-induced protection against HIV-1

Author

Kelly May, Suwat Chariyalertsak, Shida Shangguan, Peter B. Gilbert, Georgia D. Tomaras, Supachai Rerks-Ngarm, Krystelle Nganou-Makamdop, Eric Lewitus, Slim Fourati, Sheetal Sawant, Nelson L. Michael, LaTonya D. Williams, Aviva Geretz, Rasmi Thomas, Lauren Yum, Philip K. Ehrenberg, Sorachai Nitayaphan, Punnee Pitisuttithum, Gautam Kundu, Daniel C. Douek, Morgane Rolland, and Sandhya Vasan

Subjects

Transcriptome, Monocyte derived, Human immunodeficiency virus (HIV), medicine, Biology, medicine.disease_cause, Potential mechanism, Antibody dependent phagocytosis, Cell biology

Published

2021

87. Monocyte-derived transcriptome signature indicates antibody-dependent cellular phagocytosis as a potential mechanism of vaccine-induced protection against HIV-1

Author

Rasmi Thomas, Daniel C. Douek, Krystelle Nganou-Makamdop, Philip K. Ehrenberg, Peter B. Gilbert, Aviva Geretz, Eric Lewitus, Slim Fourati, Lauren Yum, Punnee Pitisuttithum, Sheetal Sawant, Sandhya Vasan, LaTonya D. Williams, Nelson L. Michael, Supachai Rerks-Ngarm, Sorachai Nitayaphan, Gautam Kundu, Suwat Chariyalertsak, Kelly May, Morgane Rolland, Shida Shangguan, and Georgia D. Tomaras

Subjects

Time Factors, HIV vaccine, HIV Infections, HIV Antibodies, medicine.disease_cause, Monocytes, Transcriptome, transcriptomics, Immunogenicity, Vaccine, Rhesus macaque, Databases, Genetic, Vaccines, DNA, RNA-Seq, Biology (General), Oligonucleotide Array Sequence Analysis, AIDS Vaccines, Microbiology and Infectious Disease, Clinical Trials as Topic, Effector, General Neuroscience, Vaccination, ADCP, General Medicine, vaccine efficacy, single cell, Treatment Outcome, Host-Pathogen Interactions, Medicine, Single-Cell Analysis, Research Article, Human, QH301-705.5, Science, Biology, General Biochemistry, Genetics and Molecular Biology, Phagocytosis, medicine, Humans, Gene, General Immunology and Microbiology, Gene Expression Profiling, Vaccine trial, Simian immunodeficiency virus, Gene signature, Vaccine efficacy, Virology, CITE-seq, HIV-1

Abstract

A gene signature was previously found to be correlated with mosaic adenovirus 26 vaccine protection in simian immunodeficiency virus and simian-human immunodeficiency virus challenge models in non-human primates. In this report, we investigated the presence of this signature as a correlate of reduced risk in human clinical trials and potential mechanisms of protection. The absence of this gene signature in the DNA/rAd5 human vaccine trial, which did not show efficacy, strengthens our hypothesis that this signature is only enriched in studies that demonstrated protection. This gene signature was enriched in the partially effective RV144 human trial that administered the ALVAC/protein vaccine, and we find that the signature associates with both decreased risk of HIV-1 acquisition and increased vaccine efficacy (VE). Total RNA-seq in a clinical trial that used the same vaccine regimen as the RV144 HIV vaccine implicated antibody-dependent cellular phagocytosis (ADCP) as a potential mechanism of vaccine protection. CITE-seq profiling of 53 surface markers and transcriptomes of 53,777 single cells from the same trial showed that genes in this signature were primarily expressed in cells belonging to the myeloid lineage, including monocytes, which are major effector cells for ADCP. The consistent association of this transcriptome signature with VE represents a tool both to identify potential mechanisms, as with ADCP here, and to screen novel approaches to accelerate the development of new vaccine candidates.

Published

2021

88. Validation of a Triplex Pharmacokinetic Assay for Simultaneous Quantitation of HIV-1 Broadly Neutralizing Antibodies PGT121, PGDM1400, and VRC07-523-LS

Author

Martina S. Wesley, Kelvin T. Chiong, Kelly E. Seaton, Christine A. Arocena, Sheetal Sawant, Jonathan Hare, Kasey Hernandez, Michelle Rojas, Jack Heptinstall, David Beaumont, Katherine Crisafi, Joseph Nkolola, Dan H. Barouch, Marcella Sarzotti-Kelsoe, Georgia D. Tomaras, and Nicole L. Yates

Subjects

Glycan, Immunology, HIV - human immunodeficiency virus, Human immunodeficiency virus (HIV), immunoprophilaxis, HIV Antibodies, medicine.disease_cause, Neutralization, Microsphere, Pharmacokinetics, Limit of Detection, In vivo, antibody, Methods, medicine, Humans, Immunology and Allergy, Potency, validation, biology, Chemistry, broadly neutralizing antibodies, Reproducibility of Results, RC581-607, Virology, Microspheres, HIV-1, biology.protein, Antibody, Immunologic diseases. Allergy, pharmacokinetics

Abstract

The outcome of the recent Antibody Mediated Prevention (AMP) trials that tested infusion of the broadly neutralizing antibody (bnAb) VRC01 provides proof of concept for blocking infection from sensitive HIV-1 strains. These results also open up the possibility that triple combinations of bnAbs such as PGT121, PGDM1400, as well as long-lasting LS variants such as VRC07-523 LS, have immunoprophylactic potential. PGT121 and PGDM1400 target the HIV-1 V3 and V2 glycan regions of the gp120 envelope protein, respectively, while VRC07-523LS targets the HIV-1 CD4 binding site. These bnAbs demonstrate neutralization potency and complementary breadth of HIV-1 strain coverage. An important clinical trial outcome is the accurate measurement of in vivo concentrations of passively infused bnAbs to determine effective doses for therapy and/or prevention. Standardization and validation of this testing method is a key element for clinical studies as is the ability to simultaneously detect multiple bnAbs in a specific manner. Here we report the development of a sensitive, specific, accurate, and precise multiplexed microsphere-based assay that simultaneously quantifies the respective physiological concentrations of passively infused bnAbs in human serum to ultimately define the threshold needed for protection from HIV-1 infection.

Published

2021

89. Changes at V2 apex of HIV-1 Clade C trimer enhance elicitation of autologous neutralizing and broad V1V2-scaffold antibodies

Author

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

Subjects

Specific antibody, Immunization, Human trial, biology.protein, Human immunodeficiency virus (HIV), medicine, Trimer, Biology, Antibody, Clade, medicine.disease_cause, Virology, Epitope

Abstract

SummaryHIV-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 introduced structure-guided changes followed by consensus-C sequence-guided optimizations at the V2-region to generate UFO-v2-RQH173 trimer. This improved the abundance of native-like trimers and carried an intrinsic dynamic V2-loop. Following immunization of rabbits, the wild-type protein failed to elicit any autologous neutralizing antibodies but UFO-v2-RQH173 elicited both autologous neutralizing and broad V1V2-scaffold antibodies. The variant with 173Y modification in V2-region, most prevalent among HIV-1 sequences, showed decreased ability in displaying native-like V1V2 epitope with time in-vitro and elicited antibodies with lower neutralizing and higher V1V2-scaffold activities. Our results identify a clade C C.1086-UFO-v2-RQH173 trimer capable of eliciting improved neutralizing and V1V2-scaffold antibodies, and reveal the importance of V2-region in tuning this.

Published

2021

90. Four-Parameter Paired Response Curve for Serial Dilution Assays

Author

Georgia D. Tomaras, Youyi Fong, and Sallie R. Permar

Subjects

Pharmacology, Statistics and Probability, Immunoassay, Likelihood Functions, medicine.diagnostic_test, Serial dilution, Sample (material), Article, medicine, Humans, Pharmacology (medical), Biological Assay, Two sample, Biological system, Mathematics

Abstract

Newer immunoassay platforms offer improved signal-to-noise ratio, but are more expensive. Thus, it is more cost-efficient to perform these assays at a few selected, rather than a full series of, sample dilutions. We propose a new four-parameter paired response curve to model the relationship between assay outcomes from two sample dilutions and study likelihood-based inference. Given a fitted paired response curve, we can predict assay outcomes for de novo dilutions of samples, which enables cross-protocol comparison of immune response biomarkers even when different protocols use different sample dilutions. Numerical studies on both simulated and real data are presented.

Published

2021

91. Comprehensive Data Integration Approach to Assess Immune Responses and Correlates of RTS,S/AS01-Mediated Protection From Malaria Infection in Controlled Human Malaria Infection Trials

Author

William Chad Young, Lindsay N. Carpp, Sidhartha Chaudhury, Jason A. Regules, Elke S. Bergmann-Leitner, Christian Ockenhouse, Ulrike Wille-Reece, Allan C. deCamp, Ellis Hughes, Celia Mahoney, Suresh Pallikkuth, Savita Pahwa, S. Moses Dennison, Sarah V. Mudrak, S. Munir Alam, Kelly E. Seaton, Rachel L. Spreng, Jon Fallon, Ashlin Michell, Fernando Ulloa-Montoya, Margherita Coccia, Erik Jongert, Galit Alter, Georgia D. Tomaras, and Raphael Gottardo

Subjects

Big Data, 0301 basic medicine, correlates of protection, malaria, Parasitemia, Information technology, immune response, 03 medical and health sciences, 0302 clinical medicine, Artificial Intelligence, vaccine, parasitic diseases, Computer Science (miscellaneous), medicine, Original Research, biology, Malaria vaccine, business.industry, Immunogenicity, RTS,S, medicine.disease, Vaccine efficacy, T58.5-58.64, Clinical trial, 030104 developmental biology, machine learning, 030220 oncology & carcinogenesis, Immunology, biology.protein, Antibody, business, Malaria, Information Systems

Abstract

RTS,S/AS01 (GSK) is the world’s first malaria vaccine. However, despite initial efficacy of almost 70% over the first 6 months of follow-up, efficacy waned over time. A deeper understanding of the immune features that contribute to RTS,S/AS01-mediated protection could be beneficial for further vaccine development. In two recent controlled human malaria infection (CHMI) trials of the RTS,S/AS01 vaccine in malaria-naïve adults, MAL068 and MAL071, vaccine efficacy against patent parasitemia ranged from 44% to 87% across studies and arms (each study included a standard RTS,S/AS01 arm with three vaccine doses delivered in four-week-intervals, as well as an alternative arm with a modified version of this regimen). In each trial, RTS,S/AS01 immunogenicity was interrogated using a broad range of immunological assays, assessing cellular and humoral immune parameters as well as gene expression. Here, we used a predictive modeling framework to identify immune biomarkers measured at day-of-challenge that could predict sterile protection against malaria infection. Using cross-validation on MAL068 data (either the standard RTS,S/AS01 arm alone, or across both the standard RTS,S/AS01 arm and the alternative arm), top-performing univariate models identified variables related to Fc effector functions and titer of antibodies that bind to the central repeat region (NANP6) of CSP as the most predictive variables; all NANP6-related variables consistently associated with protection. In cross-study prediction analyses of MAL071 outcomes (the standard RTS,S/AS01 arm), top-performing univariate models again identified variables related to Fc effector functions of NANP6-targeting antibodies as highly predictive. We found little benefit–with this dataset–in terms of improved prediction accuracy in bivariate models vs. univariate models. These findings await validation in children living in malaria-endemic regions, and in vaccinees administered a fourth RTS,S/AS01 dose. Our findings support a “quality as well as quantity” hypothesis for RTS,S/AS01-elicited antibodies against NANP6, implying that malaria vaccine clinical trials should assess both titer and Fc effector functions of anti-NANP6 antibodies.

Published

2021

92. Repeated semen exposure decreases cervicovaginal SIVmac251 infection in rhesus macaques

Author

Shaheed A. Abdulhaqq, Luis J. Montaner, Qingsheng Li, Stephanie M. Nichols, Guobin Kang, Melween I. Martínez, David B. Weiner, Xiangfan Yin, Livio Azzoni, Jan Münch, Megan C. Wise, Jocelin Joseph, Georgia D. Tomaras, Frank Kirchhoff, Andrea S. Foulkes, Preston A. Marx, Edmundo Kraiselburd, Qin Liu, Idia V. Rodríguez, David Beaumont, Carlos A. Sariol, and Christos Coutifaris

Subjects

CD4-Positive T-Lymphocytes, Myxovirus Resistance Proteins, 0301 basic medicine, Simian Acquired Immunodeficiency Syndrome, General Physics and Astronomy, Viral transmission, HIV Infections, Cervix Uteri, 02 engineering and technology, Interferon, Rhesus macaque, Medicine, lcsh:Science, Infectivity, Multidisciplinary, biology, Transmission (medicine), FOXP3, virus diseases, Forkhead Transcription Factors, 021001 nanoscience & nanotechnology, 3. Good health, Vagina, Mucosal immunology, Cytokines, Female, Simian Immunodeficiency Virus, 0210 nano-technology, medicine.drug, endocrine system, Receptors, CCR5, Science, Semen, Article, General Biochemistry, Genetics and Molecular Biology, Andrology, 03 medical and health sciences, In vivo, Animals, Humans, Mucous Membrane, business.industry, General Chemistry, biology.organism_classification, Macaca mulatta, Disease Models, Animal, 030104 developmental biology, lcsh:Q, business

Abstract

Semen is the vehicle for virion dissemination in the female reproductive tract (FRT) in male-to-female HIV transmission. Recent data suggests that higher frequency semen exposure is associated with activation of anti-HIV mechanisms in HIV negative sex workers. Here, we use a non-human primate (NHP) model to show that repeated vaginal exposure to semen significantly reduces subsequent infection by repeated low-dose vaginal SIVmac251 challenge. Repeated semen exposures result in lower CCR5 expression in circulating CD4+ T-cells, as well as higher expression of Mx1 (in correlation with IFNε expression) and FoxP3 in the cervicovaginal mucosa, and increased infiltration of CD4+ T-cells. Establishing in vivo evidence of competing effects of semen on transmission impacts our basic understanding of what factors may determine HIV infectivity in humans. Our results clearly indicate that repeated semen exposure can profoundly modulate the FRT microenvironment, paradoxically promoting host resistance against HIV acquisition., High frequency semen exposure has been associated with activation of anti-HIV mechanisms in HIV negative sex workers. Here, Abdulhaqq et al. show that repeated vaginal exposure to semen reduces vaginal infection by SIV in non-human primates, and is associated with lower CCR5 expression in CD4 T-cells and a local type-I interferon response.

Published

2019

93. Difficult-to-neutralize global HIV-1 isolates are neutralized by antibodies targeting open envelope conformations

Author

Robert J. Edwards, Kevin O. Saunders, Bette Korber, Ashley M. Trama, David C. Montefiori, John R. Mascola, Seaman, R.K. Reed, Julia A. Jones, Nathan I. Nicely, Barton F. Haynes, S.M. Alam, Mark K. Louder, Katayoun Mansouri, Xiaoying Shen, Mattia Bonsignori, Qifeng Han, and Georgia D. Tomaras

Subjects

0301 basic medicine, Glycosylation, Protein Conformation, Science, viruses, Amino Acid Motifs, Adaptive immunity, General Physics and Astronomy, HIV Infections, 02 engineering and technology, HIV Antibodies, V3 loop, Article, General Biochemistry, Genetics and Molecular Biology, Neutralization, Virus, 03 medical and health sciences, chemistry.chemical_compound, Protein structure, Antigen, Neutralization Tests, Animals, Humans, lcsh:Science, chemistry.chemical_classification, Vaccines, Multidisciplinary, biology, fungi, env Gene Products, Human Immunodeficiency Virus, virus diseases, food and beverages, General Chemistry, 021001 nanoscience & nanotechnology, Antibodies, Neutralizing, Macaca mulatta, Virology, 3. Good health, Amino acid, 030104 developmental biology, chemistry, HIV-1, biology.protein, lcsh:Q, Antibody, 0210 nano-technology

Abstract

The HIV-1 envelope (Env) is the target for neutralizing antibodies and exists on the surface of virions in open or closed conformations. Difficult-to-neutralize viruses (tier 2) express Env in a closed conformation antigenic for broadly neutralizing antibodies (bnAbs) but not for third variable region (V3) antibodies. Here we show that select V3 macaque antibodies elicited by Env vaccination can neutralize 26% of otherwise tier 2 HIV-1 isolates in standardized virus panels. The V3 antibodies only bound to Env in its open conformation. Thus, Envs on tier 2 viruses sample a state where the V3 loop is not in its closed conformation position. Envelope second variable region length, glycosylation sites and V3 amino acids were signatures of neutralization sensitivity. This study determined that open conformations of Env with V3 exposed are present on a subset of otherwise neutralization-resistant virions, therefore neutralization of tier 2 HIV-1 does not always indicate bnAb induction., Here, the authors report that specific monoclonal antibodies isolated from vaccinated rhesus macaques can neutralize a subset of Tier 2 difficult-to-neutralize HIV-1 that express Env in an open conformation, suggesting that V3 loop-specific targeting can bias the estimation of vaccine-induced bnAbs.

Published

2019

94. HLA class II-Restricted CD8+ T cells in HIV-1 Virus Controllers

Author

Stephanie A. Freel, Kent J. Weinhold, Kevin Wiehe, M. Anthony Moody, Tamika L. Payne, Qi-Jing Li, Tinashe Nyanhete, Georgia D. Tomaras, Todd Bradley, Guido Ferrari, Elizabeth Robins, Alyse Frisbee, Sheetal Sawant, William J. Faison, and Barton F. Haynes

Subjects

0301 basic medicine, Adult, CD4-Positive T-Lymphocytes, Male, T cell, lcsh:Medicine, HIV Infections, CD8-Positive T-Lymphocytes, Virus Replication, Virus, Article, 03 medical and health sciences, 0302 clinical medicine, MHC class I, HIV Seropositivity, medicine, Cytotoxic T cell, HLA-DQ beta-Chains, Humans, Antigen presentation, lcsh:Science, Gene, Lymphocyte activation, Multidisciplinary, biology, lcsh:R, Histocompatibility Antigens Class II, Viral Load, Virology, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Viral replication, biology.protein, HIV-1, Female, lcsh:Q, Infection, Viral load, 030217 neurology & neurosurgery, CD8, HLA-DRB1 Chains

Abstract

A paradigm shifting study demonstrated that induction of MHC class E and II-restricted CD8+ T cells was associated with the clearance of SIV infection in rhesus macaques. Another recent study highlighted the presence of HIV-1-specific class II-restricted CD8+ T cells in HIV-1 patients who naturally control infection (virus controllers; VCs). However, questions regarding class II-restricted CD8+ T cells ontogeny, distribution across different HIV-1 disease states and their role in viral control remain unclear. In this study, we investigated the distribution and anti-viral properties of HLA-DRB1*0701 and DQB1*0501 class II-restricted CD8+ T cells in different HIV-1 patient cohorts; and whether class II-restricted CD8+ T cells represent a unique T cell subset. We show that memory class II-restricted CD8+ T cell responses were more often detectable in VCs than in chronically infected patients, but not in healthy seronegative donors. We also demonstrate that VC CD8+ T cells inhibit virus replication in both a class I- and class II-dependent manner, and that in two VC patients the class II-restricted CD8+ T cells with an anti-viral gene signature expressed both CD4+ and CD8+ T cell lineage-specific genes. These data demonstrated that anti-viral memory class II-restricted CD8+ T cells with hybrid CD4+ and CD8+ features are present during natural HIV-1 infection.

Published

2019

95. Functional Homology for Antibody-Dependent Phagocytosis Across Humans and Rhesus Macaques

Author

Justin Pollara, Matthew Zirui Tay, R. Whitney Edwards, Derrick Goodman, Andrew R. Crowley, Robert J. Edwards, David Easterhoff, Haleigh E. Conley, Taylor Hoxie, Thaddeus Gurley, Caroline Jones, Emily Machiele, Marina Tuyishime, Elizabeth Donahue, Shalini Jha, Rachel L. Spreng, Thomas J. Hope, Kevin Wiehe, Max M. He, M. Anthony Moody, Kevin O. Saunders, Margaret E. Ackerman, Guido Ferrari, and Georgia D. Tomaras

Subjects

Neutrophils, medicine.drug_class, Phagocytosis, Immunology, Simian Acquired Immunodeficiency Syndrome, Fc receptor, HIV Infections, Fc Receptor, Monoclonal antibody, Macaque, Virus, rhesus macaques, Species Specificity, biology.animal, medicine, Animals, Humans, Immunology and Allergy, Amino Acid Sequence, Original Research, Phagocytes, biology, Monocyte, Receptors, IgG, Antibody-Dependent Cell Cytotoxicity, IgG3, phagocytosis, RC581-607, biology.organism_classification, Macaca mulatta, Immunoglobulin Isotypes, Rhesus macaque, medicine.anatomical_structure, Immunoglobulin G, Leukocytes, Mononuclear, biology.protein, Immunologic diseases. Allergy, Antibody, antibody function, Biomarkers

Abstract

Analyses of human clinical HIV-1 vaccine trials and preclinical vaccine studies performed in rhesus macaque (RM) models have identified associations between non-neutralizing Fc Receptor (FcR)-dependent antibody effector functions and reduced risk of infection. Specifically, antibody-dependent phagocytosis (ADP) has emerged as a common correlate of reduced infection risk in multiple RM studies and the human HVTN505 trial. This recurrent finding suggests that antibody responses with the capability to mediate ADP are most likely a desirable component of vaccine responses aimed at protecting against HIV-1 acquisition. As use of RM models is essential for development of the next generation of candidate HIV-1 vaccines, there is a need to determine how effectively ADP activity observed in RMs translates to activity in humans. In this study we compared ADP activity of human and RM monocytes and polymorphonuclear leukocytes (PMN) to bridge this gap in knowledge. We observed considerable variability in the magnitude of monocyte and PMN ADP activity across individual humans and RM that was not dependent on FcR alleles, and only modestly impacted by cell-surface levels of FcRs. Importantly, we found that for both human and RM phagocytes, ADP activity of antibodies targeting the CD4 binding site was greatest when mediated by human IgG3, followed by RM and human IgG1. These results demonstrate that there is functional homology between antibody and FcRs from these two species for ADP. We also used novel RM IgG1 monoclonal antibodies engineered with elongated hinge regions to show that hinge elongation augments RM ADP activity. The RM IgGs with engineered hinge regions can achieve ADP activity comparable to that observed with human IgG3. These novel modified antibodies will have utility in passive immunization studies aimed at defining the role of IgG3 and ADP in protection from virus challenge or control of disease in RM models. Our results contribute to a better translation of human and macaque antibody and FcR biology, and may help to improve testing accuracy and evaluations of future active and passive prevention strategies.

Published

2021

96. Monocyte-derived transcriptome signature indicates antibody-dependent cellular phagocytosis as the primary mechanism of vaccine-induced protection against HIV-1

Author

Georgia D. Tomaras, Sorachai Nitayaphan, Daniel C. Douek, Gautam Kundu, Sheetal Sawant, Rasmi Thomas, Punnee Pitisuttithum, Sandhya Vasan, Peter B. Gilbert, Shida Shangguan, Eric Lewitus, Slim Fourati, Philip K. Ehrenberg, Supachai Rerks-Ngarm, Lauren Yum, Nelson L. Michael, Krystelle Nganou-Makamdop, LaTonya D. Williams, Aviva Geretz, Suwat Chariyalertsak, Kelly May, and Morgane Rolland

Subjects

Transcriptome, biology, medicine, Vaccine trial, biology.protein, Simian immunodeficiency virus, Gene signature, Antibody, HIV vaccine, medicine.disease_cause, Vaccine efficacy, Gene, Virology

Abstract

A gene signature previously correlated with mosaic adenovirus 26 vaccine protection in simian immunodeficiency virus (SIV) and SHIV challenge models in non-human primates (NHP). In this report we investigated presence of this signature as a correlate of reduced risk in human clinical trials and potential mechanism for protection. The absence of this gene signature in the DNA/rAd5 human vaccine trial which did not show efficacy, strengthens our hypothesis that this signature is only enriched in studies that demonstrated protection. This gene signature was enriched in the partially effective RV144 human trial that administered the ALVAC/protein vaccine, and we find that the signature associates with both decreased risk of HIV-1 acquisition and increased vaccine efficacy. Total RNA-seq in a clinical trial that used the same vaccine regimen as the RV144 HIV vaccine implicated antibody-dependent cellular phagocytosis (ADCP) as a potential mechanism of vaccine protection. CITE-seq profiling of 53 surface markers and transcriptomes of 53,777 single cells from the same trial, showed that genes in this signature were primarily expressed in cells belonging to the myeloid lineage including monocytes, which are major effector cells for ADCP. The consistent association of this transcriptome signature with vaccine efficacy represents a tool both to identify potential mechanisms, as with ADCP here, and to screen novel approaches to accelerate development of new vaccine candidates.

Published

2021

97. Meta-analysis of HIV-1 vaccine elicited mucosal antibodies in humans

Author

M. Juliana McElrath, Jack Heptinstall, Xiaoying Shen, Cecilia Morgan, Shuying S. Li, Harriet L. Robinson, Giuseppe Pantaleo, Shelly Karuna, Nicole L. Yates, Shannon Grant, Nicole Grunenberg, Glenda Gray, Peter B. Gilbert, Ashley Clayton, Laura Polakowski, April K. Randhawa, Sheetal Sawant, Mary Allen, Xue Han, Ying Huang, Janine Maenza, Kelly E. Seaton, Paul Spearman, Ann Duerr, Yunda Huang, Aaron Deal, Gavin J. Churchyard, Georgia D. Tomaras, and Paul A. Goepfert

Subjects

0301 basic medicine, Protein vaccines, Saliva, Immunogen, Immunology, Gp41, Article, DNA vaccines, 03 medical and health sciences, 0302 clinical medicine, Medicine, Pharmacology (medical), Vector (molecular biology), RC254-282, Pharmacology, Vaccines, biology, business.industry, virus diseases, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC581-607, Vaccination, 030104 developmental biology, Infectious Diseases, Immunization, 030220 oncology & carcinogenesis, Meta-analysis, biology.protein, Immunologic diseases. Allergy, Antibody, business

Abstract

We studied mucosal immune responses in six HIV-1 vaccine trials investigating different envelope (Env)-containing immunogens. Regimens were classified into four categories: DNA/vector, DNA/vector plus protein, protein alone, and vector alone. We measured HIV-1-specific IgG and IgA in secretions from cervical (n = 111) and rectal swabs (n = 154), saliva (n = 141), and seminal plasma (n = 124) and compared to corresponding blood levels. Protein-containing regimens had up to 100% response rates and the highest Env-specific IgG response rates. DNA/vector groups elicited mucosal Env-specific IgG response rates of up to 67% that varied across specimen types. Little to no mucosal IgA responses were observed. Overall, gp41- and gp140-specific antibodies dominated gp120 mucosal responses. In one trial, prior vaccination with a protein-containing immunogen maintained durability of cervical and rectal IgG for up to 17 years. Mucosal IgG responses were boosted after revaccination. These findings highlight a role for protein immunization in eliciting HIV-1-specific mucosal antibodies and the ability of HIV-1 vaccines to elicit durable HIV-1-specific mucosal IgG.

Published

2021

98. A yeast expressed RBD-based SARS-CoV-2 vaccine formulated with 3M-052-alum adjuvant promotes protective efficacy in non-human primates

Author

Guido Ferrari, Neeta Shenvi, Thomas H. Vanderford, Susan Pereira Ribeiro, Wen-Hsiang Chen, David C. Montefiori, Talha Abid, Alessandro Sette, Daniela Weiskopf, Debashis Dutta, Katharine Floyd, Shelly Wang, Dieter Mielke, Sudhir Pai Kasturi, Georgia D. Tomaras, Pamela A. Kozlowski, Celia C. LaBranche, Maria Pino, Jungsoon Lee, Sherrie Jean, Venkata Viswanadh Edara, Xiaoying Shen, Justin Pollara, Justin C Smith, Mirko Paiardini, Rafick Pierre Sekaly, Fawn Connor-Stroud, Joyce Cohen, Gabriela Pacheco-Sanchez, Hongmei Gao, Zhuyun Liu, Christopher B. Fox, Sanjeev Gumber, Junfei Wei, Nathan Eisel, Maria Elena Bottazzi, Rachelle L. Stammen, Jennifer S. Wood, Shannon Kirejczyk, Bin Zhan, Muhammad Bilal Latif, Peter J. Hotez, Kirk Easley, Ulrich Strych, Jeroen Pollet, Mehul S. Suthar, and Mark A. Tomai

Subjects

0301 basic medicine, CD4-Positive T-Lymphocytes, Male, Immunogen, COVID-19 Vaccines, T cell, Immunology, Biology, CD8-Positive T-Lymphocytes, Antibodies, Viral, Immunoglobulin G, Cell Line, 03 medical and health sciences, 0302 clinical medicine, Immune system, Adjuvants, Immunologic, Protein Domains, Administration, Inhalation, medicine, Animals, Humans, Alum adjuvant, Lung, Administration, Intranasal, SARS-CoV-2, COVID-19, General Medicine, Viral Load, Antibodies, Neutralizing, Macaca mulatta, 030104 developmental biology, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Saccharomycetales, Spike Glycoprotein, Coronavirus, biology.protein, Alum Compounds, Cytokines, Nasal administration, Antibody, Viral load, Protein Binding

Abstract

Ongoing SARS-CoV-2 vaccine development is focused on identifying stable, cost-effective, and accessible candidates for global use, specifically in low and middle-income countries. Here, we report the efficacy of a rapidly scalable, novel yeast expressed SARS-CoV-2 specific receptor-binding domain (RBD) based vaccine in rhesus macaques. We formulated the RBD immunogen in alum, a licensed and an emerging alum adsorbed TLR-7/8 targeted, 3M-052-alum adjuvants. The RBD+3M-052-alum adjuvanted vaccine promoted better RBD binding and effector antibodies, higher CoV-2 neutralizing antibodies, improved Th1 biased CD4+T cell reactions, and increased CD8+ T cell responses when compared to the alum-alone adjuvanted vaccine. RBD+3M-052-alum induced a significant reduction of SARS-CoV-2 virus in respiratory tract upon challenge, accompanied by reduced lung inflammation when compared with unvaccinated controls. Anti-RBD antibody responses in vaccinated animals inversely correlated with viral load in nasal secretions and BAL. RBD+3M-052-alum blocked a post SARS-CoV-2 challenge increase in CD14+CD16++ intermediate blood monocytes, and Fractalkine, MCP-1, and TRAIL in the plasma. Decreased plasma analytes and intermediate monocyte frequencies correlated with reduced nasal and BAL viral loads. Lastly, RBD-specific plasma cells accumulated in the draining lymph nodes and not in the bone marrow, contrary to previous findings. Together, these data show that a yeast expressed, RBD-based vaccine+3M-052-alum provides robust immune responses and protection against SARS-CoV-2, making it a strong and scalable vaccine candidate.

Published

2021

99. Systematic Assessment of Antiviral Potency, Breadth, and Synergy of Triple Broadly Neutralizing Antibody Combinations against Simian-Human Immunodeficiency Viruses

Author

Veronica Obregon-Perko, Katharine J. Bar, Genevieve G. Fouda, Stella J. Berendam, Rama Rao Amara, Sallie R. Permar, DeAnna Tenney, Amit Kumar, Kevin O. Saunders, Georgia D. Tomaras, Tiffany M. Styles, Sampa Santra, Kristina De Paris, Papa K Morgan-Asiedu, and Ann Chahroudi

Subjects

Immunology, Simian Acquired Immunodeficiency Syndrome, Human immunodeficiency virus (HIV), HIV Antibodies, Simian, medicine.disease_cause, Microbiology, Neutralization, 03 medical and health sciences, 0302 clinical medicine, Virology, Vaccines and Antiviral Agents, medicine, Animals, Humans, Potency, 030212 general & internal medicine, Immunodeficiency, 030304 developmental biology, Antibody-dependent cell-mediated cytotoxicity, 0303 health sciences, biology, Antibody-Dependent Cell Cytotoxicity, Immunization, Passive, env Gene Products, Human Immunodeficiency Virus, Antibodies, Monoclonal, medicine.disease, biology.organism_classification, Immunization, Insect Science, Mutation, biology.protein, Simian Immunodeficiency Virus, Antibody, Broadly Neutralizing Antibodies

Abstract

Daily burden and clinical toxicities associated with antiretroviral therapy (ART) emphasize the need for alternative strategies to induce long-term human immunodeficiency virus (HIV) remission upon ART cessation. Broadly neutralizing antibodies (bNAbs) can both neutralize free virions and mediate effector functions against infected cells and therefore represent a leading immunotherapeutic approach. To increase potency and breadth, as well as to limit the development of resistant virus strains, it is likely that bNAbs will need to be administered in combination. It is therefore critical to identify bNAb combinations that can achieve robust polyfunctional antiviral activity against a high number of HIV strains. In this study, we systematically assessed the abilities of single bNAbs and triple bNAb combinations to mediate robust polyfunctional antiviral activity against a large panel of cross-clade simian-human immunodeficiency viruses (SHIVs), which are commonly used as tools for validation of therapeutic strategies targeting the HIV envelope in nonhuman primate models. We demonstrate that most bNAbs are capable of mediating both neutralizing and nonneutralizing effector functions against cross-clade SHIVs, although the susceptibility to V3 glycan-specific bNAbs is highly strain dependent. Moreover, we observe a strong correlation between the neutralization potencies and nonneutralizing effector functions of bNAbs against the transmitted/founder SHIV CH505. Finally, we identify several triple bNAb combinations comprising of CD4 binding site-, V2-glycan-, and gp120-gp41 interface-targeting bNAbs that are capable of mediating synergistic polyfunctional antiviral activities against multiple clade A, B, C, and D SHIVs. IMPORTANCE Optimal bNAb immunotherapeutics will need to mediate multiple antiviral functions against a broad range of HIV strains. Our systematic assessment of triple bNAb combinations against SHIVs will identify bNAbs with synergistic, polyfunctional antiviral activity that will inform the selection of candidate bNAbs for optimal combination designs. The identified combinations can be validated in vivo in future passive immunization studies using the SHIV challenge model.

Published

2021

100. AIDSVAX protein boost improves breadth and magnitude of vaccine-induced HIV-1 envelope-specific responses after a 7-year rest period

Author

Maurine D. Miner, Lindsey R. Baden, Colleen F. Kelley, M. Juliana McElrath, Martin Casapia, Kelly E. Seaton, Georgia D. Tomaras, Paul A. Goepfert, Susan Buchbinder, Janine Maenza, Michael C. Keefer, Magdalena E. Sobieszczyk, Javier R. Lama, Stephen C. De Rosa, Faruk Sinangil, Carter Lee, Harriet L. Robinson, David C. Montefiori, Vineeta Gulati, Marnie Elizaga, Carmen Paez, Chenchen Yu, Kristen W. Cohen, Laura Polakowski, and Yunda Huang

Subjects

Modified vaccinia Ankara, viruses, Immunization, Secondary, HIV Infections, HIV Antibodies, complex mixtures, Article, DNA vaccination, Vaccines, DNA, Medicine, Humans, HIV vaccine, AIDS Vaccines, General Veterinary, General Immunology and Microbiology, business.industry, Immunogenicity, Public Health, Environmental and Occupational Health, Vaccine trial, Virology, Vaccination, Regimen, Infectious Diseases, AIDSVAX, HIV-1, Molecular Medicine, business

Abstract

Background Eliciting durable humoral immunity with sufficient breadth and magnitude is important for HIV-1 vaccine design. The HVTN 114 vaccine trial evaluated different boost regimens administered after a 7-year rest period in participants previously enrolled in HVTN 205, who received either three MVA/HIV62B (MMM) or two DNA and two MVA/HIV62B (DDMM) injections; both vaccines expressed multiple HIV-1 antigens in non-infectious virus-like-particles. The primary objective of HVTN 114 was to assess the impact of a heterologous gp120 protein AIDSVAX B/E boost on the magnitude, breadth and durability of vaccine-induced immune responses. Methods We enrolled 27 participants from HVTN 205 into five groups. Eight participants who previously received MMM were randomized and boosted with either MVA/HIV62B alone (T1; n = 4) or MVA/HIV62B and AIDSVAX B/E (T2; n = 4). Nineteen participants who received DDMM were randomized and boosted with MVA/HIV62B alone (T3; n = 6), MVA/HIV62B and AIDSVAX B/E (T4; n = 6), or AIDSVAX B/E alone (T5; n = 7). Boosts were at months 0 and 4. Participants were followed for safety and immunogenicity for 10 months and were pooled for analysis based on the regimen: MVA-only (T1 + T3), MVA + AIDSVAX (T2 + T4), and AIDSVAX-only (T5). Results All regimens were safe and well-tolerated. Prior to the boost vaccination, binding antibody and CD4+T-cell responses were observed 7 years after HVTN 205 vaccinations. Late boosting with AIDSVAX, with or without MVA, resulted in high binding antibody responses to gp120 and V1V2 epitopes, with increased magnitude and breadth compared to those observed in HVTN 205. Late boosting with MVA, with or without AIDSVAX, resulted in increased gp140 and gp41 antibody responses and higher CD4+T-cell responses to Env and Gag. Conclusions Late boosting with AIDSVAX, alone or in combination with MVA, can broaden binding antibody responses and increase T-cell responses even years following the original MVA/HIV62B with or without DNA-priming vaccine.

Published

2021