Influence of the Envelope gp120 Phe 43 Cavity on HIV-1 Sensitivity to Antibody-Dependent Cell-Mediated Cytotoxicity Responses

Prévost, Jérémie; Zoubchenok, Daria; Richard, Jonathan; Veillette, Maxime; Pacheco, Beatriz; Coutu, Mathieu; Brassard, Nathalie; Parsons, Matthew S.; Ruxrungtham, Kiat; Bunupuradah, Torsak; Tovanabutra, Sodsai; Hwang, Kwan‐Ki; Moody, M. Anthony; Haynes, Barton F.; Bonsignori, Mattia; Sodroski, Joseph; Kaufmann, Daniel E.; Shaw, George M.; Chenine, Agnès Laurence; Finzi, Andrés

doi:10.1128/jvi.02452-16

Cited by 53 publications

(68 citation statements)

References 61 publications

(113 reference statements)

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“…To exclude any possible impact of this technical aspect of IMCs with LucR on our ADCC results, full length IMCs (n=7) that do not contain a report gene were used to evaluate ADCC of the affinity matured RV305 C1C2-specific antibodies DH677.3 and DH677.4 and A32 [2], against target cells positive for intracellular p24 (p24+) and with downregulated CD4 (CD4-). As clade CRF01_AE possess a histidine at Env HXB2 position 375 that influences sensitivity to CD4i antibody binding and ADCC [16, 17] only clade B and clade C isolates were used.…”

Section: Resultsmentioning

confidence: 99%

Boosting with ALVAC-HIV and AIDSVAX B/E enhances Env constant region 1 and 2 antibody-dependent cellular cytotoxicity

Easterhoff

Pollara

Luo

et al. 2019

Preprint

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Significance 26Over one million people become infected with HIV-1 each year making the development 27 of an efficacious HIV-1 vaccine an important unmet medical need. The RV144 human 28 HIV-1 vaccine-regimen is the only HIV-1 clinical trial to date to demonstrate vaccine- 29 efficacy. An area of focus has been on identifying ways by which to improve upon 30 RV144 vaccine-efficacy. The RV305 HIV-1 vaccine-regimen was a follow-up boost of 31 RV144 vaccine-recipients that occurred 6-8 years after the conclusion of RV144. Our 32 2 studies focused on the effect of delayed boosting in humans on the vaccine-induced 33 antibody repertoire. It was found that boosting with a HIV-1 Env vaccine increased 34 antibody-mediated effector function potency and breadth. 35Abstract 36 Induction of protective antibodies is a critical goal of HIV-1 vaccine development. One 37 strategy is to induce non-neutralizing antibodies that kill virus-infected cells as these 38 antibody specificities have been implicated in slowing HIV-1 disease progression and in 39 protection. HIV-1 Env constant region 1 and 2 (C1C2) antibodies frequently contain 40 potent antibody dependent cellular cytotoxicity (ADCC) making them a vaccine target. 41Here we explore the effect of delayed and repetitive boosting of RV144 vaccinee 42 recipients with ALVAC/AIDSVAX B/E on the C1C2-specific antibody repertoire. It was 43 found that boosting increased clonal lineage specific ADCC breadth and potency. A 44 ligand crystal structure of a vaccine-induced broad and potent ADCC-mediating C1C2-45 specific antibody showed that it bound a highly conserved Env gp120 epitope. Thus, 46 rationally designed boosting strategies to affinity mature these type of IgG C1C2-47 specific antibody responses may be one method by which to make an improved HIV 48 vaccine with higher efficacy than seen in the RV144 trial. 49 INTRODUCTION 50CD4-inducible (CD4i) epitopes within HIV-1 envelope (Env) constant regions 1 and 51 2 (C1C2) are targets for antibodies that mediate antibody dependent cellular cytotoxicity 52 (ADCC) [1]. C1C2-specific antibody epitopes have been termed Cluster A [1] and defined 53 by two Env-targeted monoclonal antibodies (mAbs), A32 [2] and C11 [1]. Structural 54 analyses of antigen complexes formed by A32, A32-like [3-5] and C11-like antibodies [6] 55 3 indicate that these antibodies bind distinct Env epitopes. The A32 epitope involves a 56 discontinuous sequence within layers 1 and 2 of the inner domain [4, 5] while the C11 57 epitope maps to the inner domain eight-stranded β sandwich [6]. Importantly, both 58 antibodies are non-neutralizing for tier 2 HIV strains, but are capable of broad and potent 59 ADCC [1, 2]. 60 The secondary analysis of HIV-1 infection risk in RV114 (NCT00223080) 61 indicated that ADCC in the presence of low anti-Env IgA responses correlated with 62 decreased HIV-1 acquisition [7]. While antibodies representative of the Env variable 63 region 2 (V2) response inversely correlated with HIV-1 acquisition [7], we previously 64 demo...

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Section: Resultsmentioning

confidence: 99%

Boosting with ALVAC-HIV and AIDSVAX B/E enhances Env constant region 1 and 2 antibody-dependent cellular cytotoxicity

Easterhoff

Pollara

Luo

et al. 2019

Preprint

Self Cite

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“…Overall, our data concur with findings of Zoubchenok et al except for the lower prevalence of His at position 105 which is likely a bias caused by small sample size. In another study, Prevost et al showed that AE subtype expose the ADCC epitopes on the Env glycoprotein as a consequence of the H375 substitution (Prevost et al, 2017). Furthermore, the insensitivity of AE subtype to broadly neutralizing antibodies that bind the CD4 interacting region on Env has been well documented (Chen et al, 2016; Utachee et al, 2014).…”

Section: Discussionmentioning

confidence: 99%

HIV-1 subtype CRF01_AE and B differ in utilization of low levels of CCR5, Maraviroc susceptibility and potential N-glycosylation sites

et al. 2017

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HIV subtypes not only predominate in different geographical regions but also differ in key phenotypic characteristics. To determine if genotypic and/or phenotypic differences in the Envelope (Env) glycoprotein can explain subtype related differences, we cloned 37 full length Envs from Subtype B and AE HIV infected individuals from Singapore. Our data demonstrates that CRF01_AE Envs have lower Potential N Glycosylation Sites and higher risk of X4 development. Phenotypically, CRF01_AE were less infectious than subtype B Envs in cells expressing low levels of CCR5. Moreover, the Maraviroc IC50 was higher for subtype B Envs and correlated with infectivity in low CCR5 expressing cells as well as PNGS. Specifically, the glycosylation site N301 in the V3 loop was seen less frequently in AE subtype and CXCR4 topic viruses. CRF01_AE differs from B subtype in terms of CCR5 usage and Maraviroc susceptibility which may have implications for HIV pathogenesis and virus evolution.

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“…Most HIV-1 group M Envs have an empty Phe 43 cavity due to the presence of a small residue such as serine at position 375 (S375), which favors a closed Env conformation [13,14]; however, CRF01_AE isolates have a naturally occurring histidine (H375) at this position [15]. The substitution of S375 with bulky hydrophobic residues fills the Phe 43 cavity and predisposes Env to adopt more "open" conformations [13,15,16]. Accordingly, histidine or tryptophan substitutions at this position (S375H or S375W) increase the susceptibility of cells infected with HIV-1 clade B (or other clades) to ADCC mediated by CD4i antibodies such as the cluster A antibody A32 ( Figure 1B) [16].…”

Section: Hiv-1 Env Residue 375 Modulates Sensitivity To Cd4i Antibodiesmentioning

confidence: 99%

Exposing HIV-1 Env: Implications for therapeutic strategies

Finzi

2019

CIM

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The human immunodeficiency virus (HIV-1) envelope glycoprotein trimer (Env) is exposed on the surfaces of both virions and infected cells. Thus, Env is the principal target for neutralizing antibodies and antibodies able to mediate antibodydependent cellular cytotoxicity (ADCC). The HIV-1 Env is a flexible molecule known to exist in at least three different conformational states: states 1, 2 and 3. Before interacting with the primary receptor, CD4, Env preferentially adopts a compact, "closed" conformation (state 1) that is largely antibody-resistant. The CD4 binding "opens" Env increasing the vulnerability of infected cells to ADCC mediated by non-neutralizing antibodies, as these easily-elicited antibodies preferentially recognize epitopes exposed in the open conformational states (states 2/3). These antibodies include the anti-coreceptor binding site and the anti-cluster A families of antibodies that, in combination with small CD4-mimetic compounds, stabilize a new asymmetric Env conformation (state 2A) that is vulnerable to ADCC. Approaches aimed at stabilizing this "open" conformation represent new interventional approaches to fight HIV-1 infection.

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Influence of the Envelope gp120 Phe 43 Cavity on HIV-1 Sensitivity to Antibody-Dependent Cell-Mediated Cytotoxicity Responses

Cited by 53 publications

References 61 publications

Boosting with ALVAC-HIV and AIDSVAX B/E enhances Env constant region 1 and 2 antibody-dependent cellular cytotoxicity

Boosting with ALVAC-HIV and AIDSVAX B/E enhances Env constant region 1 and 2 antibody-dependent cellular cytotoxicity

HIV-1 subtype CRF01_AE and B differ in utilization of low levels of CCR5, Maraviroc susceptibility and potential N-glycosylation sites

Exposing HIV-1 Env: Implications for therapeutic strategies

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