PLoS Pathogens (Jan 2012)

Transmitted/founder and chronic subtype C HIV-1 use CD4 and CCR5 receptors with equal efficiency and are not inhibited by blocking the integrin α4β7.

  • Nicholas F Parrish,
  • Craig B Wilen,
  • Lauren B Banks,
  • Shilpa S Iyer,
  • Jennifer M Pfaff,
  • Jesus F Salazar-Gonzalez,
  • Maria G Salazar,
  • Julie M Decker,
  • Erica H Parrish,
  • Anna Berg,
  • Jennifer Hopper,
  • Bhavna Hora,
  • Amit Kumar,
  • Tatenda Mahlokozera,
  • Sally Yuan,
  • Charl Coleman,
  • Marion Vermeulen,
  • Haitao Ding,
  • Christina Ochsenbauer,
  • John C Tilton,
  • Sallie R Permar,
  • John C Kappes,
  • Michael R Betts,
  • Michael P Busch,
  • Feng Gao,
  • David Montefiori,
  • Barton F Haynes,
  • George M Shaw,
  • Beatrice H Hahn,
  • Robert W Doms

DOI
https://doi.org/10.1371/journal.ppat.1002686
Journal volume & issue
Vol. 8, no. 5
p. e1002686

Abstract

Read online

Sexual transmission of human immunodeficiency virus type 1 (HIV-1) most often results from productive infection by a single transmitted/founder (T/F) virus, indicating a stringent mucosal bottleneck. Understanding the viral traits that overcome this bottleneck could have important implications for HIV-1 vaccine design and other prevention strategies. Most T/F viruses use CCR5 to infect target cells and some encode envelope glycoproteins (Envs) that contain fewer potential N-linked glycosylation sites and shorter V1/V2 variable loops than Envs from chronic viruses. Moreover, it has been reported that the gp120 subunits of certain transmitted Envs bind to the gut-homing integrin α4β7, possibly enhancing virus entry and cell-to-cell spread. Here we sought to determine whether subtype C T/F viruses, which are responsible for the majority of new HIV-1 infections worldwide, share biological properties that increase their transmission fitness, including preferential α4β7 engagement. Using single genome amplification, we generated panels of both T/F (n = 20) and chronic (n = 20) Env constructs as well as full-length T/F (n = 6) and chronic (n = 4) infectious molecular clones (IMCs). We found that T/F and chronic control Envs were indistinguishable in the efficiency with which they used CD4 and CCR5. Both groups of Envs also exhibited the same CD4+ T cell subset tropism and showed similar sensitivity to neutralization by CD4 binding site (CD4bs) antibodies. Finally, saturating concentrations of anti-α4β7 antibodies failed to inhibit infection and replication of T/F as well as chronic control viruses, although the growth of the tissue culture-adapted strain SF162 was modestly impaired. These results indicate that the population bottleneck associated with mucosal HIV-1 acquisition is not due to the selection of T/F viruses that use α4β7, CD4 or CCR5 more efficiently.