HSV-2-driven increase in the expression of α_4β_7 correlates with increased susceptibility to vaginal SHIV_SF162P3 infection

Authors

Diana J. Goode, Population Council
Rosaline Truong, Population Council
Guillermo Villegas, Population Council
Giulia Calenda, Population Council
Natalia Guerra-Perez, Population Council
Michael Piatak Jr.
Jeffrey D. Lifson
James Blanchard
Agegnehu Gettie
Melissa Robbiani, Population Council
Elena Martinelli, Population Council

Document Type

Article (peer-reviewed)

Publication Date

2014

Abstract

The availability of highly susceptible HIV target cells that can rapidly reach the mucosal lymphoid tissues may increase the chances of an otherwise rare transmission event to occur. Expression of α_4β_7 is required for trafficking of immune cells to gut inductive sites where HIV can expand and it is expressed at high level on cells particularly susceptible to HIV infection. We hypothesized that HSV-2 modulates the expression of α_4β_7 and other homing receptors in the vaginal tissue and that this correlates with the increased risk of HIV acquisition in HSV-2 positive individuals. To test this hypothesis we used an in vivo rhesus macaque (RM) model of HSV-2 vaginal infection and a new ex vivo model of macaque vaginal explants. In vivo we found that HSV-2 latently infected RMs appeared to be more susceptible to vaginal SHIV_SF162P3 infection, had higher frequency of α_4β_7^high CD4+ T cells in the vaginal tissue and higher expression of α_4β_7 and CD11c on vaginal DCs. Similarly, ex vivo HSV-2 infection increased the susceptibility of the vaginal tissue to SHIV_SF162P3. HSV-2 infection increased the frequencies of α_4β_7^high CD4+ T cells and this directly correlated with HSV-2 replication. A higher amount of inflammatory cytokines in vaginal fluids of the HSV-2 infected animals was similar to those found in the supernatants of the infected explants. Remarkably, the HSV-2-driven increase in the frequency of α_4β_7^high CD4+ T cells directly correlated with SHIV replication in the HSV-2 infected tissues. Our results suggest that the HSV-2-driven increase in availability of CD4+ T cells and DCs that express high levels of α_4β_7 is associated with the increase in susceptibility to SHIV due to HSV-2. This may persists in absence of HSV-2 shedding. Hence, higher availability of α_4β_7 positive HIV target cells in the vaginal tissue may constitute a risk factor for HIV transmission.

Recommended Citation

Goode, Diana J., Rosaline Truong, Guillermo Villegas, Giulia Calenda, Natalia Guerra-Perez, Michael Piatak Jr., Jeffrey D. Lifson, James Blanchard, Agegnehu Gettie, Melissa Robbiani, and Elena Martinelli. 2014. "HSV-2-driven increase in the expression of α_4β_7 correlates with increased susceptibility to vaginal SHIV_SF162P3 infection," PLoS Pathogens 10(12): e1004567.

DOI

10.1371/journal.ppat.1004567

Language

English