Thymic HIV-2 infection uncovers posttranscriptional control of viral replication in human thymocytes

Helena Nunes-Cabaço; Paula Matoso; Russell B Foxall; Rita Tendeiro; Ana R Pires; Tânia Carvalho; Ana I Pinheiro; Rui S Soares; Ana E Sousa

doi:10.1128/JVI.03047-14

Thymic HIV-2 infection uncovers posttranscriptional control of viral replication in human thymocytes

J Virol. 2015 Feb;89(4):2201-8. doi: 10.1128/JVI.03047-14. Epub 2014 Dec 3.

Authors

Helena Nunes-Cabaço¹, Paula Matoso², Russell B Foxall², Rita Tendeiro², Ana R Pires², Tânia Carvalho², Ana I Pinheiro², Rui S Soares², Ana E Sousa¹

Affiliations

¹ Instituto de Medicina Molecular, Faculdade de Medicina, Universidade de Lisboa, Lisbon, Portugal hcabaco@medicina.ulisboa.pt asousa@medicina.ulisboa.pt.
² Instituto de Medicina Molecular, Faculdade de Medicina, Universidade de Lisboa, Lisbon, Portugal.

Abstract

A unique HIV-host equilibrium exists in untreated HIV-2-infected individuals. This equilibrium is characterized by low to undetectable levels of viremia throughout the disease course, despite the establishment of disseminated HIV-2 reservoirs at levels comparable to those observed in untreated HIV-1 infection. Although the clinical spectrum is similar in the two infections, HIV-2 infection is associated with a much lower rate of CD4 T-cell decline and has a limited impact on the mortality of infected adults. Here we investigated HIV-2 infection of the human thymus, the primary organ for T-cell production. Human thymic tissue and suspensions of total or purified CD4 single-positive thymocytes were infected with HIV-2 or HIV-1 primary isolates using either CCR5 or CXCR4 coreceptors. We found that HIV-2 infected both thymic organ cultures and thymocyte suspensions, as attested to by the total HIV DNA and cell-associated viral mRNA levels. Nevertheless, thymocytes featured reduced levels of intracellular Gag viral protein, irrespective of HIV-2 coreceptor tropism and cell differentiation stage, in agreement with the low viral load in culture supernatants. Our data show that HIV-2 is able to infect the human thymus, but the HIV-2 replication cycle in thymocytes is impaired, providing a new model to identify therapeutic targets for viral replication control.

Importance: HIV-1 infects the thymus, leading to a decrease in CD4 T-cell production that contributes to the characteristic CD4 T-cell loss. HIV-2 infection is associated with a very low rate of progression to AIDS and is therefore considered a unique naturally occurring model of attenuated HIV disease. HIV-2-infected individuals feature low to undetectable plasma viral loads, in spite of the numbers of circulating infected T cells being similar to those found in patients infected with HIV-1. We assessed, for the first time, the direct impact of HIV-2 infection on the human thymus. We show that HIV-2 is able to infect the thymus but that the HIV-2 replication cycle in thymocytes is impaired. We propose that this system will be important to devise immunotherapies that target viral production, aiding the design of future therapeutic strategies for HIV control.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adult
Cells, Cultured
Child, Preschool
HIV-1 / physiology
HIV-2 / physiology*
Host-Pathogen Interactions*
Humans
Infant
Infant, Newborn
Organ Culture Techniques
Thymocytes / virology*
Thymus Gland / pathology
Thymus Gland / virology*
Virus Replication*