HIV-1 Vaccine Development:  Constrained Peptide Immunogens Show Improved Binding to the Anti-HIV-1 gp41 MAb

McGaughey, Georgia B.; Citron, Michael; Danzeisen, Renee; Freidinger, Roger; Garsky, Victor M.; Hurni, William M.; Joyce, Joseph G.; Liang, Xiaoping; Miller, Michael D.; Shiver, John W.; Bogusky, Michael J.

doi:10.1021/bi026952u

Cited by 98 publications

(93 citation statements)

References 49 publications

(77 reference statements)

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“…A more plausible cause is that conformational f lexibility in the oligomannan arms is still high, and the immune response is ''diluted'' by recognition of improper structures within the chemical space. This complicating factor has been proposed as a reason for the inability to mimic the broad neutralizing characteristics of other HIV-1-directed mAbs (4,10,33).…”

Section: 00e+04mentioning

confidence: 99%

“…For several of these mAbs, identification and extensive characterization of the neutralizing epitopes have been realized (4)(5)(6)(7). This structural knowledge has been used to design antigens intended to direct the primary immune response toward the neutralizing epitope (8)(9)(10). However, in all immunization studies performed to date these vaccine candidates have failed to elicit broadly neutralizing antibodies.…”

mentioning

confidence: 99%

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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

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

124

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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

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Section: 00e+04mentioning

confidence: 99%

mentioning

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

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

124

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“…In addition to simple linear or structurally constrained peptide immunogens, recombinant protein immunogens including displays of constrained 2F5 epitope in the contexts of various protein scaffolds have been also pursued [28][29][30][31][32][33][34][35][36][37]. While inducing high antibody titers against the primary amino acid sequence of the epitope, these immunogens have failed to elicit NAbs against primary HIV-1.…”

Section: Introductionmentioning

confidence: 99%

Immunogenicity of recombinant human immunodeficiency virus type 1-like particles expressing gp41 derivatives in a pre-fusion state

Kim

Qiao

et al. 2007

Vaccine

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The conserved membrane proximal external region (MPER) of the ectodomain of human immunodeficiency virus type 1 (HIV-1) gp41 is the target of two broadly neutralizing antibodies, 2F5 and 4E10. However, no neutralizing antibodies have been elicited against immunogens bearing these epitopes. Given that structural and biochemical studies suggest that the lipid membrane of the virion is involved in their proper configuration, HIV-1 gp41 derivatives in a pre-fusion state were expressed on the surface of immature virus like particles (VLP) derived from Sf9 cells. Guinea pigs were immunized with three doses of VLPs or Sf9 cells presenting gp41 derivatives with or without E. coli heat-labile enterotoxin (LT) as an adjuvant. While immune sera contained high titer anti-VLP antibodies, the specific anti-gp41 antibody responses were low with no neutralizing antibodies detected. An explanation for this absence may be the low level of gp41 expression relative to the many other proteins derived from host cells which are incorporated onto the VLP surface. In addition, the anti-gp41 immune response was preferentially directed to the C-helical domain, away from the MPER. Future vaccine design needs to contend with the complexity of epitope display as well as immunodominance.

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“…10,20,[23][24][25][26] First, synthetic peptide antigens representing monomeric gp41 peptides are conformationally unstable. Since stability and bioactive conformation are intimately associated with trimeric quaternary structure, they are difficult to duplicate using monomeric peptides.…”

Section: Introductionmentioning

confidence: 99%

“…Consequently, attempts to exploit these peptides as immunogens, alone or with additional variable regions, have been unsuccessful. [23][24][25][26] Golding et al 10 and Louis et al 20 showed that antibodies gp41 Protein Mimetics Elicit Neutralizing Antibodies 321 generated against complexed peptides or engineered trimeric peptides based on the N-HR or C-HR domains possess viral neutralizing activity. These results suggest that targeting the bioactive conformations of the N-HR or C-HR domains is a viable vaccine design strategy.…”

Section: Introductionmentioning

confidence: 99%

Quaternary protein mimetics of gp41 elicit neutralizing antibodies against HIV fusion‐active intermediate state

Sadler

Zhang

et al. 2008

Biopolymers

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During viral entry, the fusogenic state of human immunodeficiency virus Type 1 (HIV‐1) envelope protein gp41 is a quaternary structure consisting of three gp41 glycoproteins, each with two conserved helical domains (N‐HR and C‐HR). Thus far, the examination of monomeric gp41 peptides as an immunologically focused approach to vaccine design has not been successful. Here we report an approach using quaternary protein mimetics (called 3α mimetics) that are based on the gp41 N‐HR and C‐HR domains to closely mimic the fusogenic state and overcome the deficiencies of the monomeric peptide approach for synthetic vaccine design. The 3α mimetics are conveniently prepared by chemoselective ligation of unprotected monomeric peptides to an interstrand linker, and display enhanced conformational stability compared to the corresponding monomers. The 3α mimetics with or without a covalently attached T‐helper epitope were immunogenic and elicited antisera that bound both recombinant gp160, which contains gp41, and HIV‐1 virions and immunoprecipitated recombinant gp41. Anti‐3α mimetic antisera neutralized viral infectivity against R5‐ and X4‐tropic strains of HIV‐1 at 31.5°C. The results suggest that a quaternary protein approach to mimic conserved and functional domains of viral envelope proteins is desirable for HIV vaccine development as such antigens are more likely to produce immunologically‐focused and broadly neutralizing antibody responses. © 2008 Wiley Periodicals, Inc. Biopolymers (Pept Sci) 90: 320–329, 2008.This article was originally published online as an accepted preprint. The “Published Online” date corresponds to the preprint version. You can request a copy of the preprint by emailing the Biopolymers editorial office at biopolymers@wiley.com

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HIV-1 Vaccine Development: Constrained Peptide Immunogens Show Improved Binding to the Anti-HIV-1 gp41 MAb

Cited by 98 publications

References 49 publications

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

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

Immunogenicity of recombinant human immunodeficiency virus type 1-like particles expressing gp41 derivatives in a pre-fusion state

Quaternary protein mimetics of gp41 elicit neutralizing antibodies against HIV fusion‐active intermediate state

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