Magnitude and Breadth of the Neutralizing Antibody Response in the RV144 and Vax003 HIV-1 Vaccine Efficacy Trials

Montefiori, David C.; Karnasuta, Chitraporn; Huang, Ying; Ahmed, Hasan; Gilbert, Peter B.; Souza, Mark S. de; McLinden, Robert; Tovanabutra, Sodsai; Laurence-Chenine, Agnes; Sanders‐Buell, Eric; Moody, M. Anthony; Bonsignori, Mattia; Ochsenbauer, Christina; Kappes, John C.; Tang, Haili; Greene, Kelli; Gao, Hongmei; LaBranche, Celia C.; Andrews, Charla; Polonis, Victoria R.; Rerks-Ngarm, Supachai; Pitisuttithum, Punnee; Nitayaphan, Sorachai; Kaewkungwal, Jaranit; Self, Steve; Berman, Phillip W.; Francis, Donald P.; Sinangil, Faruk; Lee, Carter; Tartaglia, Jim; Robb, Merlin L.; Haynes, Barton F.; Michael, Nelson L.; Kim, Jerome H.

doi:10.1093/infdis/jis367

Cited by 261 publications

(319 citation statements)

References 47 publications

Supporting

Mentioning

303

Contrasting

Unclassified

Order By: Relevance

“…Moreover, the NAbs measured here in vaccinated macaques are higher than nAb responses in immune sera from human clinical trials using Env immunogens. In the Vax003 trial, neutralization of Tier 2 viruses using the A3R5 assay was infrequent and weak and no Tier 2 neutralization with this assay was seen in the RV144 trial (52).…”

Section: Neutralization Breadth Is Induced Against Heterologous Tier mentioning

confidence: 98%

Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens

Hessell

Malherbe

Pissani

et al. 2016

The Journal of Immunology

View full text Add to dashboard Cite

Advancement in immunogen selection and vaccine design that will rapidly elicit a protective Ab response is considered critical for HIV vaccine protective efficacy. Vaccine-elicited Ab responses must therefore have the capacity to prevent infection by neutralization-resistant phenotypes of transmitted/founder (T/F) viruses that establish infection in humans. Most vaccine candidates to date have been ineffective at generating Abs that neutralize T/F or early variants. In this study, we report that coimmunizing rhesus macaques with HIV-1 gp160 DNA and gp140 trimeric protein selected from native envelope gene sequences (envs) induced neutralizing Abs against Tier 2 autologous viruses expressing cognate envelope (Env). The Env immunogens were selected from envs emerging during the earliest stages of neutralization breadth developing within the first 2 years of infection in two clade B–infected human subjects. Moreover, the IgG responses in macaques emulated the targeting to specific regions of Env known to be associated with autologous and heterologous neutralizing Abs developed within the human subjects. Furthermore, we measured increasing affinity of macaque polyclonal IgG responses over the course of the immunization regimen that correlated with Tier 1 neutralization. In addition, we report firm correlations between Tier 2 autologous neutralization and Tier 1 heterologous neutralization, as well as overall TZM-bl breadth scores. Additionally, the activation of Env-specific follicular helper CD4 T cells in lymphocytes isolated from inguinal lymph nodes of vaccinated macaques correlated with Tier 2 autologous neutralization. These results demonstrate the potential for native Env derived from subjects at the time of neutralization broadening as effective HIV vaccine elements.

show abstract

Section: Neutralization Breadth Is Induced Against Heterologous Tier mentioning

confidence: 98%

Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens

Hessell

Malherbe

Pissani

et al. 2016

The Journal of Immunology

View full text Add to dashboard Cite

show abstract

“…First, the ability of the passively transferred b12 broadly neutralizing antibody to protect macaques from simian/HIV (SHIV) infection is reduced if the constant region (Fc) of the antibody is modified in a manner that abrogates binding to Fc receptors on cells of the innate immune system [1]. Secondly, the recent RV144 vaccine trial in Thailand provided a modest level of protection from HIV infection, despite not inducing robust cytotoxic T lymphocyte (CTL) responses or broadly neutralizing antibodies [2,3]. A correlate of protection analysis of this trial revealed that the presence of antibodies capable of mediating antibody-dependent cellular cytotoxicity (ADCC) corresponded with protection when vaccinated individuals also had low levels of immunoglobulin (Ig)A antibodies that could inhibit IgG binding and induction of ADCC [4,5].…”

Section: Introductionmentioning

confidence: 99%

Phenotypical and functional profiles of natural killer cells exhibiting matrix metalloproteinase-mediated CD16 cleavage after anti-HIV antibody-dependent activation

Tang

Isitman

Bruneau

et al. 2015

Clinical and Experimental Immunology

View full text Add to dashboard Cite

SummaryNatural killer (NK) cell-mediated antibody-dependent cellular cytotoxicity (ADCC) has been linked to protection from HIV infection and slower progression towards AIDS. However, antibody-dependent activation of NK cells results in phenotypical alterations similar to those observed on NK cells from individuals with progressive HIV infection. Activation of NK cells induces matrix metalloproteinase (MMP)-mediated cleavage of cell surface CD16. In the present study we assessed the phenotype and functional profile of NK cells exhibiting post-activation MMP-mediated CD16 cleavage. We found that NK cells achieving the highest levels of activation during stimulation exhibit the most profound decreases in CD16 expression. Further, we observed that educated KIR3DL1

show abstract

“…This was most clearly seen in the ALVAC/AIDSVAX RV144 HIV-1 vaccine efficacy trial, in which Env immunogens 92TH023 and A244 CRFAE_01 gp120s both expressed a dominant linear V2 epitope and bound with high-nanomolar affinity to the glycandependent V1V2 BnAbs PG9 and CH01 (16). Although both linear and glycan-dependent V2 epitopes were expressed on the A244 immunogen, the dominant V2 plasma antibody responses in this trial were targeted to linear V2 epitopes and not to the glycan-dependent BnAb epitope (14)(15)(16). A series of mAbs, the prototype of which is the mAb CH58, has been isolated from RV144 vaccines and shown to bind to linear V2 epitopes that include lysine 169 (16).…”

mentioning

confidence: 71%

“…Immunization of humans with Env proteins has not resulted in high plasma titers of BnAbs (14,15). Rather, dominant strainspecific neutralizing epitopes have selectively been induced.…”

mentioning

confidence: 99%

Recognition of synthetic glycopeptides by HIV-1 broadly neutralizing antibodies and their unmutated ancestors

Alam

Dennison

Aussedat

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

View full text Add to dashboard Cite

Current HIV-1 vaccines elicit strain-specific neutralizing antibodies. Broadly neutralizing antibodies (BnAbs) are not induced by current vaccines, but are found in plasma in ∼20% of HIV-1-infected individuals after several years of infection. One strategy for induction of unfavored antibody responses is to produce homogeneous immunogens that selectively express BnAb epitopes but minimally express dominant strain-specific epitopes. Here we report that synthetic, homogeneously glycosylated peptides that bind avidly to variable loop 1/2 (V1V2) BnAbs PG9 and CH01 bind minimally to strain-specific neutralizing V2 antibodies that are targeted to the same envelope polypeptide site. Both oligomannose derivatization and conformational stabilization by disulfide-linked dimer formation of synthetic V1V2 peptides were required for strong binding of V1V2 BnAbs. An HIV-1 vaccine should target BnAb unmutated common ancestor (UCA) B-cell receptors of naïve B cells, but to date no HIV-1 envelope constructs have been found that bind to the UCA of V1V2 BnAb PG9. We demonstrate herein that V1V2 glycopeptide dimers bearing Man 5 GlcNAc 2 glycan units bind with apparent nanomolar affinities to UCAs of V1V2 BnAbs PG9 and CH01 and with micromolar affinity to the UCA of a V2 strainspecific antibody. The higher-affinity binding of these V1V2 glycopeptides to BnAbs and their UCAs renders these glycopeptide constructs particularly attractive immunogens for targeting subdominant HIV-1 envelope V1V2-neutralizing antibody-producing B cells.

show abstract

Magnitude and Breadth of the Neutralizing Antibody Response in the RV144 and Vax003 HIV-1 Vaccine Efficacy Trials

Cited by 261 publications

References 47 publications

Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens

Achieving Potent Autologous Neutralizing Antibody Responses against Tier 2 HIV-1 Viruses by Strategic Selection of Envelope Immunogens

Phenotypical and functional profiles of natural killer cells exhibiting matrix metalloproteinase-mediated CD16 cleavage after anti-HIV antibody-dependent activation

Recognition of synthetic glycopeptides by HIV-1 broadly neutralizing antibodies and their unmutated ancestors

Contact Info

Product

Resources

About