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Characterization of the membrane-bound form of the chimeric, B/C recombinant HIV-1 Env, LT5.J4b12C. | LitMetric

AI Article Synopsis

  • HIV-1 diversity poses challenges for vaccine development, particularly with B/C recombinants which are common in China and India.
  • Some HIV-1 infected patients produce broadly neutralizing antibodies (bNAbs) that target HIV-1 envelopes (Envs), which can be used as immunogens if they cleave efficiently into subunits.
  • The study reports that the B/C recombinant Env LT5.J4b12C can be efficiently cleaved and selectively binds to bNAbs, highlighting its potential for vaccine design.

Article Abstract

Human immunodeficiency virus 1 (HIV-1) diversity is a significant challenge in developing a vaccine against the virus. B/C recombinants have been found in India and other places but are the predominant clade prevalent in China. HIV-1 envelopes (Envs) are the target of broadly neutralizing antibodies (bNAbs) which develop spontaneously in some HIV-1 infected patients. It has been previously reported with efficiently cleaved clade A, B and C Envs that preferential binding of Envs to bNAbs as opposed to non-NAbs, a desirable property for immunogens, is correlated with efficient cleavage of the Env precursor polypeptide into constituent subunits. These Envs are suitable for designing immunogens as soluble proteins, virus-like particles or for delivery by viral vectors/plasmid DNA. However, a B/C recombinant Env with similar properties has not been reported. Here we show that the chimeric, recombinant B/C clade Env LT5.J4b12C is efficiently cleaved on the plasma membrane and selectively binds to bNAbs.

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Source
http://dx.doi.org/10.1099/jgv.0.001141DOI Listing

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