PLoS ONE (Jan 2011)

The glycan shield of HIV is predominantly oligomannose independently of production system or viral clade.

  • Camille Bonomelli,
  • Katie J Doores,
  • D Cameron Dunlop,
  • Victoria Thaney,
  • Raymond A Dwek,
  • Dennis R Burton,
  • Max Crispin,
  • Christopher N Scanlan

DOI
https://doi.org/10.1371/journal.pone.0023521
Journal volume & issue
Vol. 6, no. 8
p. e23521

Abstract

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The N-linked oligomannose glycans of HIV gp120 are a target for both microbicide and vaccine design. The extent of cross-clade conservation of HIV oligomannose glycans is therefore a critical consideration for the development of HIV prophylaxes. We measured the oligomannose content of virion-associated gp120 from primary virus from PBMCs for a range of viral isolates and showed cross-clade elevation (62-79%) of these glycans relative to recombinant, monomeric gp120 (∼30%). We also confirmed that pseudoviral production systems can give rise to notably elevated gp120 oligomannose levels (∼98%), compared to gp120 derived from a single-plasmid viral system using the HIV(LAI) backbone (56%). This study highlights differences in glycosylation between virion-associated and recombinant gp120.