Your search keyword '"Peter B Gilbert"' showing total 13 results

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

Author

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

Subjects

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

Abstract

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

Published

2020

2. DNA Priming Increases Frequency of T-Cell Responses to a Vesicular Stomatitis Virus HIV Vaccine with Specific Enhancement of CD8 + T-Cell Responses by Interleukin-12 Plasmid DNA

Author

Rong Xu, Kristen W. Cohen, John H. Eldridge, Nidhi Kochar, Georgia D. Tomaras, Ian Frank, Michael A. Egan, M. Juliana McElrath, Drew Hannaman, Daryl E. Morris, Christine M. Hay, Ayuko Ota-Setlik, Raphael Gottardo, Nicole Frahm, Magdalena E. Sobieszczyk, Shuying S. Li, Mary Allen, Lawrence Corey, David K. Clarke, Stephen C. De Rosa, Hong Van Tieu, Gregory J. Wilson, Greg Finak, Peter B. Gilbert, and Marnie Elizaga

Subjects

0301 basic medicine, Microbiology (medical), biology, business.industry, Electroporation, Immunogenicity, medicine.medical_treatment, Clinical Biochemistry, Immunology, Vaccine trial, biology.organism_classification, Virology, DNA vaccination, Vaccination, 03 medical and health sciences, 030104 developmental biology, Vesicular stomatitis virus, Immunology and Allergy, Medicine, HIV vaccine, business, Adjuvant

Abstract

The HIV Vaccine Trials Network (HVTN) 087 vaccine trial assessed the effect of increasing doses of pIL-12 (interleukin-12 delivered as plasmid DNA) adjuvant on the immunogenicity of an HIV-1 multiantigen (MAG) DNA vaccine delivered by electroporation and boosted with a vaccine comprising an attenuated vesicular stomatitis virus expressing HIV-1 Gag (VSV-Gag). We randomized 100 healthy adults to receive placebo or 3 mg HIV-MAG DNA vaccine (ProfectusVax HIV-1 gag / pol or ProfectusVax nef / tat / vif , env ) coadministered with pIL-12 at 0, 250, 1,000, or 1,500 μg intramuscularly by electroporation at 0, 1, and 3 months followed by intramuscular inoculation with 3.4 × 10 7 PFU VSV-Gag vaccine at 6 months. Immune responses were assessed after the prime and boost and 6 months after the last vaccination. High-dose pIL-12 increased the magnitude of CD8 + T-cell responses postboost compared to no pIL-12 ( P = 0.02), while CD4 + T-cell responses after the prime were higher in the absence of pIL-12 than with low- and medium-dose pIL-12 ( P ≤ 0.05). The VSV boost increased Gag-specific CD4 + and CD8 + T-cell responses in all groups ( P < 0.001 for CD4 + T cells), inducing a median of four Gag epitopes in responders. Six to 9 months after the boost, responses decreased in magnitude, but CD8 + T-cell response rates were maintained. The addition of a DNA prime dramatically improved responses to the VSV vaccine tested previously in the HVTN 090 trial, leading to broad epitope targeting and maintained CD8 + T-cell response rates at early memory. The addition of high-dose pIL-12 given with a DNA prime by electroporation and boosted with VSV-Gag increased the CD8 + T-cell responses but decreased the CD4 + responses. This approach may be advantageous in reshaping the T-cell responses to a variety of chronic infections or tumors. (This study has been registered at ClinicalTrials.gov under registration no. NCT01578889.)

Published

2017

3. Infectious Virion Capture by HIV-1 gp120-Specific IgG from RV144 Vaccinees

Author

Hua-Xin Liao, Guido Ferrari, Thomas N. Denny, Peter B. Gilbert, M. Anthony Moody, John C. Kappes, Barton F. Haynes, Punnee Pitisuttithum, David C. Montefiori, Pinghuang Liu, R. Glenn Overman, Christina Ochsenbauer, Nelson L. Michael, Georgia D. Tomaras, Supachai Rerks-Ngarm, Youyi Fong, Xiaoying Shen, Sorachai Nitayaphan, Jerome H. Kim, Victoria R. Polonis, Jaranit Kaewkungwal, S. Munir Alam, Mattia Bonsignori, and Nicole L. Yates

Subjects

viruses, Immunology, Pilot Projects, HIV Envelope Protein gp120, Antibodies, Viral, Microbiology, Immunoglobulin G, Virus, Immune system, Antibody Repertoire, Antibody Specificity, Virology, Vaccines and Antiviral Agents, Humans, AIDS Vaccines, biology, Viral Vaccine, Virion, virus diseases, Viral Vaccines, Antibodies, Neutralizing, Vaccination, IgG binding, Insect Science, HIV-1, biology.protein, Antibody

Abstract

The detailed examination of the antibody repertoire from RV144 provides a unique template for understanding potentially protective antibody functions. Some potential immune correlates of protection were untested in the correlates analyses due to inherent assay limitations, as well as the need to keep the correlates analysis focused on a limited number of endpoints to achieve statistical power. In an RV144 pilot study, we determined that RV144 vaccination elicited antibodies that could bind infectious virions (including the vaccine strains HIV-1 CM244 and HIV-1 MN and an HIV-1 strain expressing transmitted/founder Env, B.WITO.c). Among vaccinees with the highest IgG binding antibody profile, the majority (78%) captured the infectious vaccine strain virus (CM244), while a smaller proportion of vaccinees (26%) captured HIV-1 transmitted/founder Env virus. We demonstrated that vaccine-elicited HIV-1 gp120 antibodies of multiple specificities (V3, V2, conformational C1, and gp120 conformational) mediated capture of infectious virions. Although capture of infectious HIV-1 correlated with other humoral immune responses, the extent of variation between these humoral responses and virion capture indicates that virion capture antibodies occupy unique immunological space.

Published

2013

4. Antibody-Dependent Cellular Cytotoxicity-Mediating Antibodies from an HIV-1 Vaccine Efficacy Trial Target Multiple Epitopes and Preferentially Use the VH1 Gene Family

Author

Jerome H. Kim, Chun-Yen Tsao, David C. Montefiori, Michael D. Alpert, Peter B. Gilbert, Kwan-Ki Hwang, Anthony L. DeVico, Mattia Bonsignori, Ying Huang, Sorachai Nitayaphan, Georgia D. Tomaras, George K. Lewis, Guido Ferrari, M. Anthony Moody, Nelson L. Michael, Supachai Rerks-Ngarm, John F. Whitesides, Barton F. Haynes, Xi Chen, Thaddeus C. Gurley, Hua-Xin Liao, Dawn J. Marshall, Daniel M. Kozink, Justin Pollara, David T. Evans, Punnee Pitisuttithum, and Jaranit Kaewkungwal

Subjects

Male, Genes, Immunoglobulin Heavy Chain, Immunology, HIV Antibodies, Microbiology, Epitope, Virology, Vaccines and Antiviral Agents, Humans, Mutation frequency, AIDS Vaccines, Antibody-dependent cell-mediated cytotoxicity, biology, Antibody-Dependent Cell Cytotoxicity, Vaccine trial, Primary and secondary antibodies, Human Experimentation, Cell killing, Insect Science, HIV-1, biology.protein, Female, Antibody, Conformational epitope

Abstract

The ALVAC-HIV/AIDSVAX-B/E RV144 vaccine trial showed an estimated efficacy of 31%. RV144 secondary immune correlate analysis demonstrated that the combination of low plasma anti-HIV-1 Env IgA antibodies and high levels of antibody-dependent cellular cytotoxicity (ADCC) inversely correlate with infection risk. One hypothesis is that the observed protection in RV144 is partially due to ADCC-mediating antibodies. We found that the majority (73 to 90%) of a representative group of vaccinees displayed plasma ADCC activity, usually (96.2%) blocked by competition with the C1 region-specific A32 Fab fragment. Using memory B-cell cultures and antigen-specific B-cell sorting, we isolated 23 ADCC-mediating nonclonally related antibodies from 6 vaccine recipients. These antibodies targeted A32-blockable conformational epitopes ( n = 19), a non-A32-blockable conformational epitope ( n = 1), and the gp120 Env variable loops ( n = 3). Fourteen antibodies mediated cross-clade target cell killing. ADCC-mediating antibodies displayed modest levels of V-heavy (VH) chain somatic mutation (0.5 to 1.5%) and also displayed a disproportionate usage of VH1 family genes (74%), a phenomenon recently described for CD4-binding site broadly neutralizing antibodies (bNAbs). Maximal ADCC activity of VH1 antibodies correlated with mutation frequency. The polyclonality and low mutation frequency of these VH1 antibodies reveal fundamental differences in the regulation and maturation of these ADCC-mediating responses compared to VH1 bNAbs.

Published

2012

5. Phase I Safety and Immunogenicity Evaluations of an Alphavirus Replicon HIV-1 Subtype CgagVaccine in Healthy HIV-1-Uninfected Adults

Author

Nina D. Russell, Michael Pensiero, Donald S. Burke, Jeffrey D. Chulay, Ya Lin Chiu, Peter B. Gilbert, S. S. Abdool Karim, Mary Allen, John Hural, and M. Wecker

Subjects

Adult, Male, Microbiology (medical), Enzyme-Linked Immunospot Assay, Adolescent, Clinical Biochemistry, Immunology, Enzyme-Linked Immunosorbent Assay, HIV Infections, Viremia, Alphavirus, HIV Antibodies, gag Gene Products, Human Immunodeficiency Virus, Interferon-gamma, South Africa, Young Adult, Double-Blind Method, medicine, Humans, Immunology and Allergy, Interferon gamma, Adverse effect, AIDS Vaccines, Vaccines, Botswana, Reactogenicity, biology, business.industry, ELISPOT, Immunogenicity, Encephalomyelitis, Venezuelan Equine, Middle Aged, biology.organism_classification, medicine.disease, Virology, United States, Clinical trial, HIV-1, Cytokines, Female, business, T-Lymphocytes, Cytotoxic, medicine.drug

Abstract

On the basis of positive preclinical data, we evaluated the safety and immunogenicity of an alphavirus replicon HIV-1 subtype Cgagvaccine (AVX101), expressing a nonmyristoylated form of Gag, in two double-blind, randomized, placebo-controlled clinical trials in healthy HIV-1-uninfected adults. Escalating doses of AVX101 or placebo were administered subcutaneously to participants in the United States and Southern Africa. Because of vaccine stability issues, the first trial was halted prior to completion of all dose levels and a second trial was implemented. The second trial was also stopped prematurely due to documentation issues with the contract manufacturer. Safety and immunogenicity were evaluated through assessments of reactogenicity, reports of adverse events, and assessment of replication-competent and Venezuelan equine encephalitis (VEE) viremia. Immunogenicity was measured using the following assays: enzyme-linked immunosorbent assay (ELISA), chromium 51 (51Cr)-release cytotoxic T lymphocyte (CTL), gamma interferon (IFN-γ) ELISpot, intracellular cytokine staining (ICS), and lymphoproliferation assay (LPA). Anti-vector antibodies were also measured. AVX101 was well tolerated and exhibited only modest local reactogenicity. There were 5 serious adverse events reported during the trials; none were considered related to the study vaccine. In contrast to the preclinical data, immune responses in humans were limited. Only low levels of binding antibodies and T-cell responses were seen at the highest doses. This trial also highlighted the difficulties in developing a novel vector for HIV.

Published

2012

6. Low-Dose Penile SIVmac251 Exposure of Rhesus Macaques Infected with Adenovirus Type 5 (Ad5) and Then Immunized with a Replication-Defective Ad5-Based SIV gag/pol/nef Vaccine Recapitulates the Results of the Phase IIb Step Trial of a Similar HIV-1 Vaccine

Author

Michael B. McChesney, Michael A. Thomas, John W. Shiver, Huma Qureshi, Peter B. Gilbert, Zhong-Min Ma, Danilo R. Casimiro, Linda Fritts, Andrew J. Bett, Ying Huang, Christopher J. Miller, Veronique Desilva, Janet DiPasquale, Marjorie Robert-Guroff, Gregory Hodge, and Michael N. Robertson

Subjects

biology, animal diseases, viruses, T cell, Immunology, virus diseases, biochemical phenomena, metabolism, and nutrition, Microbiology, Virology, Virus, Tissue culture, medicine.anatomical_structure, Immunization, Insect Science, biology.protein, medicine, Vector (molecular biology), Antibody, Viral load, CD8

Abstract

The Step Trial showed that the MRKAd5 HIV-1 subtype B Gag/Pol/Nef vaccine did not protect men from HIV infection or reduce setpoint plasma viral RNA (vRNA) levels but, unexpectedly, it did modestly enhance susceptibility to HIV infection in adenovirus type 5 (Ad5)-seropositive, uncircumcised men. As part of the process to understand the results of the Step Trial, we designed a study to determine whether rhesus macaques chronically infected with a host-range mutant Ad5 (Ad5hr) and then immunized with a replication defective Ad5 SIVmac239 Gag/Pol/Nef vaccine were more resistant or susceptible to SIV infection than unimmunized rhesus macaques challenged with a series of escalating dose penile exposures to SIVmac 251. The Ad5 SIV vaccine induced CD8 + T cell responses in 70% of the monkeys, which is similar to the proportion of humans that responded to the vaccine in the Step Trial. However, the vaccine did not protect vaccinated animals from penile SIV challenge. At the lowest SIV exposure dose (10 3 50% tissue culture infective doses), 2 of 9 Ad5-seropositive animals immunized with the Ad5 SIV vaccine became infected compared to 0 of 34 animals infected in the other animal groups (naive animals, Ad5-seropositive animals immunized with the empty Ad5 vector, Ad5-seronegative animals immunized with the Ad5 SIV vaccine, and Ad5-seronegative animals immunized with the empty Ad5 vector). Penile exposure to more concentrated virus inocula produced similar rates of infection in all animal groups. Although setpoint viral loads were unaffected in Step vaccinees, the Ad5 SIV-immunized animals had significantly lower acute-phase plasma vRNA levels compared to unimmunized animals. Thus, the results of the nonhuman primate (NHP) study described here recapitulate the lack of protection against HIV acquisition seen in the Step Trial and suggest a greater risk of infection in the Ad5-seropositive animals immunized with the Ad5 SIV vaccine. Further studies are necessary to confirm the enhancement of virus acquisition and to discern associated mechanisms.

Published

2012

7. Antibody Specificities Associated with Neutralization Breadth in Plasma from Human Immunodeficiency Virus Type 1 Subtype C-Infected Blood Donors

Author

John R. Mascola, Natasha Taylor, George M. Shaw, Blake Wood, Elin S. Gray, Allan C. deCamp, Diane Wycuff, Adrian Puren, David C. Montefiori, Georgia D. Tomaras, Lynn Morris, James M. Binley, Penny L. Moore, Peter B. Gilbert, Constantinos Kurt Wibmer, and Barton F. Haynes

Subjects

Immunology, Blood Donors, Cross Reactions, HIV Antibodies, Microbiology, Virus, Epitope, Neutralization, Antibody Specificity, Neutralization Tests, Virology, Humans, chemistry.chemical_classification, biology, Antibody titer, biology.organism_classification, Molecular biology, Epitope mapping, chemistry, Antibodies, Anticardiolipin, Insect Science, Lentivirus, HIV-1, biology.protein, Pathogenesis and Immunity, Antibody, Glycoprotein, Epitope Mapping

Abstract

Defining the specificities of the anti-human immunodeficiency virus type 1 (HIV-1) envelope antibodies able to mediate broad heterologous neutralization will assist in identifying targets for an HIV-1 vaccine. We screened 70 plasmas from chronically HIV-1-infected individuals for neutralization breadth. Of these, 16 (23%) were found to neutralize 80% or more of the viruses tested. Anti-CD4 binding site (CD4bs) antibodies were found in almost all plasmas independent of their neutralization breadth, but they mainly mediated neutralization of the laboratory strain HxB2 with little effect on the primary virus, Du151. Adsorption with Du151 monomeric gp120 reduced neutralizing activity to some extent in most plasma samples when tested against the matched virus, although these antibodies did not always confer cross-neutralization. For one plasma, this activity was mapped to a site overlapping the CD4-induced (CD4i) epitope and CD4bs. Anti-membrane-proximal external region (MPER) ( r = 0.69; P < 0.001) and anti-CD4i ( r = 0.49; P < 0.001) antibody titers were found to be correlated with the neutralization breadth. These anti-MPER antibodies were not 4E10- or 2F5-like but spanned the 4E10 epitope. Furthermore, we found that anti-cardiolipin antibodies were correlated with the neutralization breadth ( r = 0.67; P < 0.001) and anti-MPER antibodies ( r = 0.6; P < 0.001). Our study suggests that more than one epitope on the envelope glycoprotein is involved in the cross-reactive neutralization elicited during natural HIV-1 infection, many of which are yet to be determined, and that polyreactive antibodies are possibly involved in this phenomenon.

Published

2009

8. Association between Virus-Specific T-Cell Responses and Plasma Viral Load in Human Immunodeficiency Virus Type 1 Subtype C Infection

Author

Ibou Thior, Natasha Rybak, MF McLane, Peter B. Gilbert, Tak H. Lee, Thumbi Ndung'u, Vladimir Novitsky, S. Gaolekwe, Richard Marlink, Trevor Peter, and Myron Essex

Subjects

T-Lymphocytes, viruses, T cell, Immunology, Gene Products, gag, Gene Products, pol, HIV Infections, Viremia, Human leukocyte antigen, Major histocompatibility complex, Microbiology, Virus, Immune system, Virology, MHC class I, medicine, Humans, biology, Gene Products, env, virus diseases, Viral Load, medicine.disease, medicine.anatomical_structure, Insect Science, HIV-1, biology.protein, Pathogenesis and Immunity, Viral load

Abstract

Virus-specific T-cell immune responses are important in restraint of human immunodeficiency virus type 1 (HIV-1) replication and control of disease. Plasma viral load is a key determinant of disease progression and infectiousness in HIV infection. Although HIV-1 subtype C (HIV-1C) is the predominant virus in the AIDS epidemic worldwide, the relationship between HIV-1C-specific T-cell immune responses and plasma viral load has not been elucidated. In the present study we address (i) the association between the level of plasma viral load and virus-specific immune responses to different HIV-1C proteins and their subregions and (ii) the specifics of correlation between plasma viral load and T-cell responses within the major histocompatibility complex (MHC) class I HLA supertypes. Virus-specific immune responses in the natural course of HIV-1C infection were analyzed in the gamma interferon (IFN-γ)-enzyme-linked immunospot assay by using synthetic overlapping peptides corresponding to the HIV-1C consensus sequence. For Gag p24, a correlation was seen between better T-cell responses and lower plasma viral load. For Nef, an opposite trend was observed where a higher T-cell response was more likely to be associated with a higher viral load. At the level of the HLA supertypes, a lower viral load was associated with higher T-cell responses to Gag p24 within the HLA A2, A24, B27, and B58 supertypes, in contrast to the absence of such a correlation within the HLA B44 supertype. The present study demonstrated differential correlations (or trends to correlation) in various HIV-1C proteins, suggesting (i) an important role of the HIV-1C Gag p24-specific immune responses in control of viremia and (ii) more rapid viral escape from immune responses to Nef with no restraint of plasma viral load. Correlations between the level of IFN-γ-secreting T cells and viral load within the MHC class I HLA supertypes should be considered in HIV vaccine design and efficacy trials.

Published

2003

9. Magnitude and Frequency of Cytotoxic T-Lymphocyte Responses: Identification of Immunodominant Regions of Human Immunodeficiency Virus Type 1 Subtype C

Author

Peter B. Gilbert, Richard Marlink, Ibou Thior, Huyen Cao, S. Gaolekwe, Thumbi Ndung'u, Trevor Peter, Vladimir Novitsky, MF McLane, Max Essex, Tak H. Lee, and Natasha Rybak

Subjects

HIV Antigens, viruses, Molecular Sequence Data, Immunology, Population, Epitopes, T-Lymphocyte, HIV Infections, Human leukocyte antigen, Biology, Major histocompatibility complex, Microbiology, Virus, Immune system, Virology, Humans, Amino Acid Sequence, HIV vaccine, education, education.field_of_study, Immunodominant Epitopes, virus diseases, CTL, Insect Science, HIV-1, biology.protein, Pathogenesis and Immunity, Epitope Mapping, T-Lymphocytes, Cytotoxic

Abstract

A systematic analysis of immune responses on a population level is critical for a human immunodeficiency virus type 1 (HIV-1) vaccine design. Our studies in Botswana on (i) molecular analysis of the HIV-1 subtype C (HIV-1C) epidemic, (ii) frequencies of major histocompatibility complex class I HLA types, and (iii) cytotoxic T-lymphocyte (CTL) responses in the course of natural infection allowed us to address HIV-1C-specific immune responses on a population level. We analyzed the magnitude and frequency of the gamma interferon ELISPOT-based CTL responses and translated them into normalized cumulative CTL responses. The introduction of population-based cumulative CTL responses reflected both (i) essentials of the predominant virus circulating locally in Botswana and (ii) specificities of the genetic background of the Botswana population, and it allowed the identification of immunodominant regions across the entire HIV-1C. The most robust and vigorous immune responses were found within the HIV-1C proteins Gag p24, Vpr, Tat, and Nef. In addition, moderately strong responses were scattered across Gag p24, Pol reverse transcriptase and integrase, Vif, Tat, Env gp120 and gp41, and Nef. Assuming that at least some of the immune responses are protective, these identified immunodominant regions could be utilized in designing an HIV vaccine candidate for the population of southern Africa. Targeting multiple immunodominant regions should improve the overall vaccine immunogenicity in the local population and minimize viral escape from immune recognition. Furthermore, the analysis of HIV-1C-specific immune responses on a population level represents a comprehensive systematic approach in HIV vaccine design and should be considered for other HIV-1 subtypes and/or different geographic areas.

Published

2002

10. Human Immunodeficiency Virus Type 1 Subtype C Molecular Phylogeny: Consensus Sequence for an AIDS Vaccine Design?

Author

Simani Gaseitsiwe, Sui-Yuan Chang, MF McLane, Peter B. Gilbert, Vladimir Novitsky, Brian T. Foley, Carolyn Williamson, Ibou Thior, Isaac A. Klein, Pride Chigwedere, Richard Marlink, Fredrik O. Vannberg, Thumbi Ndung'u, Tak H. Lee, U. R. Smith, Trevor Peter, S. Gaolekwe, Max Essex, and Natasha Rybak

Subjects

Molecular Sequence Data, Immunology, Gene Products, gag, HIV Infections, Biology, Microbiology, Genome, Nucleotide diversity, Phylogenetics, Virology, Consensus Sequence, Consensus sequence, Humans, Amino Acid Sequence, HIV vaccine, Phylogeny, HIV Long Terminal Repeat, AIDS Vaccines, Genetics, Acquired Immunodeficiency Syndrome, Genetic diversity, Base Sequence, Phylogenetic tree, virus diseases, Drug Design, Insect Science, DNA, Viral, Molecular phylogenetics, HIV-1, Recombination and Evolution

Abstract

An evolving dominance of human immunodeficiency virus type 1 subtype C (HIV-1C) in the AIDS epidemic has been associated with a high prevalence of HIV-1C infection in the southern African countries and with an expanding epidemic in India and China. Understanding the molecular phylogeny and genetic diversity of HIV-1C viruses may be important for the design and evaluation of an HIV vaccine for ultimate use in the developing world. In this study we analyzed the phylogenetic relationships (i) between 73 nonrecombinant HIV-1C near-full-length genome sequences, including 51 isolates from Botswana; (ii) between HIV-1C consensus sequences that represent different geographic subsets; and (iii) between specific isolates and consensus sequences. Based on the phylogenetic analyses of 73 near-full-length genomes, 16 “lineages” (a term that is used hereafter for discussion purposes and does not imply taxonomic standing) were identified within HIV-1C. The lineages were supported by high bootstrap values in maximum-parsimony and neighbor-joining analyses and were confirmed by the maximum-likelihood method. The nucleotide diversity between the 73 HIV-1C isolates (mean value of 8.93%; range, 2.9 to 11.7%) was significantly higher than the diversity of the samples to the consensus sequence (mean value of 4.86%; range, 3.3 to 7.2%, P < 0.0001). The translated amino acid distances to the consensus sequence were significantly lower than distances between samples within all HIV-1C proteins. The consensus sequences of HIV-1C proteins accompanied by amino acid frequencies were presented (that of Gag is presented in this work; those of Pol, Vif, Vpr, Tat, Rev, Vpu, Env, and Nef are presented elsewhere [ http://www.aids.harvard.edu/lab_research/concensus_sequence.htm ]). Additionally, in the promoter region three NF-κB sites (GGGRNNYYCC) were identified within the consensus sequences of the entire set or any subset of HIV-1C isolates. This study suggests that the consensus sequence approach could overcome the high genetic diversity of HIV-1C and facilitate an AIDS vaccine design, particularly if the assumption that an HIV-1C antigen with a more extensive match to the circulating viruses is likely to be more efficacious is proven in efficacy trials.

Published

2002

11. Analysis of HLA A*02 Association with Vaccine Efficacy in the RV144 HIV-1 Vaccine Trial

Author

Adam Bates, Wenjie Deng, James I. Mullins, Merlin L. Robb, Tomer Hertz, Daniel E. Geraghty, Michelle Lazzaro, Kim G. Wong, Snehal Nariya, John McNevin, Grace Ibitamuno, Allan C. deCamp, Raphael Gottardo, Andrea Bradfield, Georgia D. Tomaras, Lennie Chen, Gustavo H. Kijak, Julia N. Stoddard, Annemarie O'Sullivan, Meera Bose, Sue Li, Jerome H. Kim, Philip Konopa, Eric Sanders-Buell, Daryl E. Morris, Supachai Rerks-Ngarm, Hasan Ahmed, Craig A. Magaret, Robert J. O'Connell, Sorachai Nitayaphan, David C. Montefiori, M. Juliana McElrath, Youyi Fong, Mark S. deSouza, Paul T. Edlefsen, Shana Howell, Vatcharain Assawadarachai, Sodsai Tovanabutra, Jodie P. Goodridge, Esther Lei, John Sidney, Nicole Frahm, Holly Janes, Peter B. Gilbert, Brendan B. Larsen, Alessandro Sette, Hong Zhao, Susan Zolla-Pazner, Andrew J. Gartland, and Brandon S. Maust

Subjects

T-Lymphocytes, Immunology, HIV Infections, Human leukocyte antigen, HIV Envelope Protein gp120, Microbiology, Cohort Studies, Immunity, Virology, Vaccines and Antiviral Agents, HLA-A2 Antigen, Humans, HIV vaccine, Genetic Association Studies, AIDS Vaccines, biology, Vaccine trial, Vaccine efficacy, HLA-A, Insect Science, biology.protein, HIV-1, Antibody, Viral load

Abstract

The RV144 HIV-1 vaccine trial demonstrated partial efficacy of 31% against HIV-1 infection. Studies into possible correlates of protection found that antibodies specific to the V1 and V2 (V1/V2) region of envelope correlated inversely with infection risk and that viruses isolated from trial participants contained genetic signatures of vaccine-induced pressure in the V1/V2 region. We explored the hypothesis that the genetic signatures in V1 and V2 could be partly attributed to selection by vaccine-primed T cells. We performed a T-cell-based sieve analysis of breakthrough viruses in the RV144 trial and found evidence of predicted HLA binding escape that was greater in vaccine versus placebo recipients. The predicted escape depended on class I HLA A*02- and A*11-restricted epitopes in the MN strain rgp120 vaccine immunogen. Though we hypothesized that this was indicative of postacquisition selection pressure, we also found that vaccine efficacy (VE) was greater in A*02-positive (A*02 + ) participants than in A*02 − participants (VE = 54% versus 3%, P = 0.05). Vaccine efficacy against viruses with a lysine residue at site 169, important to antibody binding and implicated in vaccine-induced immune pressure, was also greater in A*02 + participants (VE = 74% versus 15%, P = 0.02). Additionally, a reanalysis of vaccine-induced immune responses that focused on those that were shown to correlate with infection risk suggested that the humoral responses may have differed in A*02 + participants. These exploratory and hypothesis-generating analyses indicate there may be an association between a class I HLA allele and vaccine efficacy, highlighting the importance of considering HLA alleles and host immune genetics in HIV vaccine trials. IMPORTANCE The RV144 trial was the first to show efficacy against HIV-1 infection. Subsequently, much effort has been directed toward understanding the mechanisms of protection. Here, we conducted a T-cell-based sieve analysis, which compared the genetic sequences of viruses isolated from infected vaccine and placebo recipients. Though we hypothesized that the observed sieve effect indicated postacquisition T-cell selection, we also found that vaccine efficacy was greater for participants who expressed HLA A*02, an allele implicated in the sieve analysis. Though HLA alleles have been associated with disease progression and viral load in HIV-1 infection, these data are the first to suggest the association of a class I HLA allele and vaccine efficacy. While these statistical analyses do not provide mechanistic evidence of protection in RV144, they generate testable hypotheses for the HIV vaccine community and they highlight the importance of assessing the impact of host immune genetics in vaccine-induced immunity and protection. (This study has been registered at ClinicalTrials.gov under registration no. NCT00223080.)

Published

2014

12. Identification of Human Immunodeficiency Virus Type 1 Subtype C Gag-, Tat-, Rev-, and Nef-Specific Elispot-Based Cytotoxic T-Lymphocyte Responses for AIDS Vaccine Design

Author

Ibou Thior, Peter B. Gilbert, Natasha Rybak, Sui-Yuan Chang, Max Essex, Fredrik O. Vannberg, Richard Marlink, Isaac A. Klein, Tak H. Lee, S. Gaolekwe, Trevor Peter, Brian T. Foley, Thumbi Ndung'u, MF McLane, Vladimir Novitsky, and Pride Chigwedere

Subjects

Cytotoxicity, Immunologic, Molecular Sequence Data, Immunology, Population, chemical and pharmacologic phenomena, Human leukocyte antigen, Biology, Microbiology, Epitope, Virus, Epitopes, Immune system, T-Lymphocyte Subsets, Virology, Humans, Cytotoxic T cell, Amino Acid Sequence, education, Phylogeny, AIDS Vaccines, Acquired Immunodeficiency Syndrome, education.field_of_study, ELISPOT, virus diseases, Genes, gag, Genes, nef, Genes, rev, CTL, Genes, tat, Insect Science, HIV-1, Pathogenesis and Immunity

Abstract

The most severe human immunodeficiency virus type 1 (HIV-1) epidemic is occurring in southern Africa. It is caused by HIV-1 subtype C (HIV-1C). In this study we present the identification and analysis of cumulative cytotoxic T-lymphocyte (CTL) responses in the southern African country of Botswana. CTLs were shown to be an important component of the immune response to control HIV-1 infection. The definition of optimal and dominant epitopes across the HIV-1C genome that are targeted by CTL is critical for vaccine design. The characteristics of the predominant virus that causes the HIV-1 epidemic in a certain geographic area and also the genetic background of the population, through the distribution of common HLA class I alleles, might impact dominant CTL responses in the vaccinee and in the general population. The enzyme-linked immunospot (Elispot) gamma interferon assay has recently been shown to be a reliable tool to map optimal CTL epitopes, correlating well with other methods, such as intracellular staining, tetramer staining, and the classical chromium release assay. Using Elispot with overlapping synthetic peptides across Gag, Tat, Rev, and Nef, we analyzed HIV-1C-specific CTL responses of HIV-1-infected blood donors. Profiles of cumulative Elispot-based CTL responses combined with diversity and sequence consensus data provide an additional characterization of immunodominant regions across the HIV-1C genome. Results of the study suggest that the construction of a poly-epitope subtype-specific HIV-1 vaccine that includes multiple copies of immunodominant CTL epitopes across the viral genome, derived from predominant HIV-1 viruses, might be a logical approach to the design of a vaccine against AIDS.

Published

2001

13. Intrapatient Diversity and Its Correlation with Viral Setpoint in Human Immunodeficiency Virus Type 1 CRF02_A/G-IbNG Infection

Author

Peter B. Gilbert, J L Sankalé, Phyllis J. Kanki, Souleymane Mboup, Indu Mani, and Geoffrey Eisen

Subjects

Nonsynonymous substitution, Time Factors, Immunology, Molecular Sequence Data, Human immunodeficiency virus (HIV), Replication, HIV Infections, Biology, medicine.disease_cause, Microbiology, Setpoint, Correlation, Virology, Consensus Sequence, medicine, Humans, Phylogeny, Genetics, Genetic diversity, Base Sequence, Genetic Variation, Viral Load, Viral replication, Insect Science, DNA, Viral, HIV-1, RNA, Viral, Female, Viral load, Diversity (business)

Abstract

The human immunodeficiency virus type 1 (HIV-1) viral setpoint during the disease-free interval has been strongly associated with future risk of disease progression. An awareness of the correlation between viral setpoint and HIV-1 genetic evolution over time is important in the understanding of viral dynamics and infection. We examined genetic diversity in HIV-1 CRF02_A/G-IbNG-infected seroincident women in Dakar, Senegal; determined whether a viral setpoint kinetic pattern existed for CRF02_A/G-IbNG during the disease-free interval; and correlated viral load level and diversity. Samples were drawn during the disease-free interval from consenting CRF02_A/G-IbNG-infected, antiretroviral therapy-naïve female commercial sex workers in Dakar, Senegal. Based on sequential plasma RNA values, low and high viral setpoint groups were established. Intrapatient diversity and divergence over time was determined from earlier and later time point DNA samples from each person. Most individuals followed the viral setpoint paradigm. For each 1|−|log 10 copy/ml of plasma increase in viral load, intrapatient diversity increased by 1.4% ( P = 0.028). A greater diversification rate was observed in the high viral setpoint group than in the low viral setpoint group ( P = 0.01). Greater nucleotide ( P = 0.015) and amino acid ( P = 0.048) divergences and a greater nucleotide divergence rate ( P = 0.03) were found in the high viral setpoint group. There was no difference between the groups in the ratio of the number of nonsynonymous substitutions per nonsynonymous site to the number of synonymous substitutions per synonymous site. The greater intrapatient diversity, divergence, and diversification rates observed in the high viral setpoint group supports the notion that diversity is driven by cycles of viral replication resulting in accumulated mutations. Recognizing diversity potential based on viral load levels in individuals may inform the design of vaccines and therapies.

Published

2002