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CD4 binding determinant mimicry for HIV vaccine design. | LitMetric

CD4 binding determinant mimicry for HIV vaccine design.

Front Immunol

Chemical Immunology Research Center, Department of Pathology and Laboratory Medicine, University of Texas-Houston Medical School Houston, TX, USA.

Published: December 2012

AI Article Synopsis

  • - The HIV-1 envelope protein gp120 has highly mutable immunodominant epitopes, making it challenging to develop an effective vaccine; focusing on the conserved region that binds to CD4 receptors (CD4BD) shows more promise.
  • - Despite its potential, targeting CD4BD is complicated due to gp120's flexible structure and the virus's immune evasion strategies, particularly with its superantigenic properties that fail to elicit a strong adaptive immune response.
  • - A potential solution involves using an electrophilic gp120 analog (E-gp120) to covalently bond with B cell receptors, which could promote neutralizing antibody production by transforming the B cell response, although successful vaccination will need a stable immun

Article Abstract

The immunodominant epitopes expressed by the HIV-1 envelope protein gp120 are hypermutable, defeating attempts to develop an effective HIV vaccine. Targeting the structurally conserved gp120 determinant that binds host CD4 receptors (CD4BD) and initiates infection is a more promising route to vaccination, but this has proved difficult because of the conformational flexibility of gp120 and immune evasion mechanisms used by the virus. Mimicking the outer CD4BD conformational epitopes is difficult because of their discontinuous nature. The CD4BD region composed of residues 421-433 (CD4BD(core)) is a linear epitope, but this region possesses B cell superantigenic character. While superantigen epitopes are vulnerable to a small subset of spontaneously produced neutralizing antibodies present in humans without infection (innate antibodies), their non-covalent binding to B cell receptors (BCRs) does not stimulate an effective adaptive response from B cells. Covalent binding at naturally occurring nucleophilic sites of the BCRs by an electrophilic gp120 (E-gp120) analog is a promising solution. E-gp120 induces the synthesis of neutralizing antibodies the CD4BD(core). The highly energetic covalent reaction is hypothesized to convert the abortive superantigens-BCR interaction into a stimulatory signal, and the binding of a spatially distinct epitope at the traditional combining site of the BCRs may furnish a second stimulatory signal. Flexible synthetic peptides can detect pre-existing CD4BD(core)-specific neutralizing antibodies. However, induced-fit conformational transitions of the peptides dictated by the antibody combining site structure may induce the synthesis of non-neutralizing antibodies. Successful vaccine targeting of the CD4BD will require a sufficiently rigid immunogen that mimics the native epitope conformation and bypasses B cell checkpoints restricting synthesis of the neutralizing antibodies.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC3523313PMC
http://dx.doi.org/10.3389/fimmu.2012.00383DOI Listing

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