Targeting the carbohydrates on HIV-1: Interaction of oligomannose dendrons with human monoclonal antibody 2G12 and DC-SIGN

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The envelope spike of HIV is one of the most highly N-glycosylated structures found in nature. However, despite extensive research revealing essential functional roles in infection and immune evasion, the chemical structures of the glycans on the native viral envelope glycoprotein gp120-as opposed to recombinantly generated gp120 -have not been described. Here, we report on the identity of the N-linked glycans from primary isolates of HIV-1 (clades A, B, and C) and from the simian immunodeficiency virus. MS analysis reveals a remarkably simple and highly conserved virus-specific glycan profile almost entirely devoid of medial Golgi-mediated processing. In stark contrast to recombinant gp120, which shows extensive exposure to cellular glycosylation enzymes (>70% complex type glycans), the native envelope shows barely detectable processing beyond the biosynthetic intermediate Man 5 GlcNAc 2 (<2% complex type glycans). This oligomannose (Man 5-9 GlcNAc 2 ) profile is conserved across primary isolates and geographically divergent clades but is not reflected in the current generation of gp120 antigens used for vaccine trials. In the context of vaccine design, we also note that Manα1→2Man-terminating glycans (Man 6-9 GlcNAc 2 ) of the type recognized by the broadly neutralizing anti-HIV antibody 2G12 are 3-fold more abundant on the native envelope than on the recombinant monomer and are also found on isolates not neutralized by 2G12. The Manα1→2-Man residues of gp120 therefore provide a vaccine target that is physically larger and antigenically more conserved than the 2G12 epitope itself. This study revises and extends our understanding of the glycan shield of HIV with implications for AIDS vaccine design.HIV | 2G12 | gp120 | glycosylation | vaccine

Section: Discussionmentioning

confidence: 99%

Envelope glycans of immunodeficiency virions are almost entirely oligomannose antigens

Doores

Bonomelli

Harvey

et al. 2010

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374

“…Surface plasmon resonance studies of 2G12 binding to this construct yielded results nearly identical to ours in that the effect of clustering on enhanced antibody recognition was clearly evident. Similarly, synthetic multivalent dendrons presenting Man 4 or Man 9 oligosaccharides were shown to induce good binding of 2G12 and have been proposed as potential vaccine components (35). Although such approaches to ''direct'' the immune response to more relevant antibody generation are important, a successful strategy will likely need to encompass a method to ''lock'' the optimal oligosaccharide conformation in a preferred orientation.…”

Section: 00e+04mentioning

confidence: 99%

An oligosaccharide-based HIV-1 2G12 mimotope vaccine induces carbohydrate-specific antibodies that fail to neutralize HIV-1 virions

Joyce¹,

Krauss

Song³

et al. 2008

124

The conserved oligomannose epitope, Man9GlcNAc2, recognized by the broadly neutralizing human mAb 2G12 is an attractive prophylactic vaccine candidate for the prevention of HIV-1 infection. We recently reported total chemical synthesis of a series of glycopeptides incorporating one to three copies of Man 9GlcNAc2 coupled to a cyclic peptide scaffold. Surface plasmon resonance studies showed that divalent and trivalent, but not monovalent, compounds were capable of binding 2G12. To test the efficacy of the divalent glycopeptide as an immunogen capable of inducing a 2G12-like neutralizing antibody response, we covalently coupled the molecule to a powerful immune-stimulating protein carrier and evaluated immunogenicity of the conjugate in two animal species. We used a differential immunoassay to demonstrate induction of high levels of carbohydrate-specific antibodies; however, these antibodies showed poor recognition of recombinant gp160 and failed to neutralize a panel of viral isolates in entry-based neutralization assays. To ascertain whether antibodies produced during natural infection could recognize the mimetics, we screened a panel of HIV-1-positive and -negative sera for binding to gp120 and the synthetic antigens. We present evidence from both direct and competitive binding assays that no significant recognition of the glycopeptides was observed, although certain sera did contain antibodies that could compete with 2G12 for binding to recombinant gp120. molecular mimicry ͉ neutralizing antibody

“…A multivalent glycan vaccine or carbohydrate conjugated with a carrier protein and administered with an immunological adjuvant has been adopted to increase the immunogenicity of carbohydrates. As an example, a GH vaccine with ∼700 GH units conjugated to one keyhole limpet hemocyanin (KLH) protein was prepared and administered together with a mixture of saponins called QS21 adjuvant (18,(22)(23)(24)(25), and it had been shown that treatment of mice with GH-KLH/QS21 could induce antisera against GH-positive cell lines without autoimmune reactions (14,23). Furthermore, the vaccine was fairly well-tolerated in a phase I clinical trial for metastatic breast cancer patients.…”

mentioning

confidence: 99%

Carbohydrate-based vaccines with a glycolipid adjuvant for breast cancer

Huang

Hung

Cheung

et al. 2013

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Globo H (GH) is a hexasaccharide specifically overexpressed on a variety of cancer cells and therefore, a good candidate for cancer vaccine development. To identify the optimal carrier and adjuvant combination, we chemically synthesized and linked GH to a carrier protein, including keyhole limpet hemocyanion, diphtheria toxoid cross-reactive material (CRM) 197 (DT), tetanus toxoid, and BSA, and combined with an adjuvant, and it was administered to mice for the study of immune response. Glycan microarray analysis of the antiserum obtained indicated that the combination of GH-DT adjuvanted with the α-galactosylceramide C34 has the highest enhancement of anti-GH IgG. Compared with the phase III clinical trial vaccine, GHkeyhole limpet hemocyanion/QS21, the GH-DT/C34 vaccine elicited more IgG antibodies, which are more selective for GH and the GHrelated epitopes, stage-specific embryonic antigen 3 (SSEA3) and SSEA4, all of which were specifically overexpressed on breast cancer cells and breast cancer stem cells with SSEA4 at the highest level (>90%). We, therefore, further developed SSEA4-DT/C34 as a vaccine candidate, and after immunization, it was found that the elicited antibodies are also IgG-dominant and very specific for SSEA4.carbohydrate vaccine | diphtheria toxin