PLoS ONE (Jan 2019)

Sexually transmitted founder HIV-1 viruses are relatively resistant to Langerhans cell-mediated restriction.

  • Nina Hertoghs,
  • Bernadien M Nijmeijer,
  • Nienke H van Teijlingen,
  • Angharad E Fenton-May,
  • Tanja M Kaptein,
  • John L van Hamme,
  • John C Kappes,
  • Neeltje A Kootstra,
  • Beatrice H Hahn,
  • Persephone Borrow,
  • Carla M S Ribeiro,
  • Teunis B H Geijtenbeek

DOI
https://doi.org/10.1371/journal.pone.0226651
Journal volume & issue
Vol. 14, no. 12
p. e0226651

Abstract

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A single HIV-1 variant establishes infection of the host after sexual contact. Identifying the phenotypic characteristics of these Transmitted Founder (T/F) viruses is important to understand the restriction mechanisms during transmission. Langerhans cells (LCs) are the mucosal dendritic cell subset that has been shown to have a protective role in HIV-1 transmission. Immature LCs efficiently capture and degrade HIV-1 via langerin-mediated restriction. Here we have investigated the capacity of T/F HIV-1 strains to infect mucosal Langerhans cells (LCs). Notably, most T/F variants efficiently infected immature LCs derived from skin and vaginal tissue in contrast to chronic HIV-1 laboratory strains. Next we screened a panel of T/F viruses and their matched 6-month consensus sequence viruses. Interestingly most T/F variants infected immature LCs whereas donor-matched 6-month consensus sequence viruses had lost the ability to infect LCs. However, we also identified 6-month consensus sequence viruses that had retained an ability to infect LCs similar to that of the donor-matched T/F virus. Moreover, some T/F viruses and 6-month consensus sequence viruses were unable to infect immature LCs. Further analyses indicated that T/F viruses are less sensitive to langerin-mediated restriction. These data suggest that T/F HIV-1 variants have the ability to infect immature LCs, which will facilitate transmission.