Abstract

Insight into the establishment and maintenance of HIV-1 infection in resting CD4+ T cell subsets is critical for the development of therapeutics targeting the HIV-1 reservoir. Although the frequency of HIV-1 infection, as quantified by the frequency of HIV-1 DNA, is lower in CD4+ naive T cells (TN) than in the memory T cell subsets, recent studies have shown that TN harbor a large pool of replication-competent virus. Interestingly, however, TN are highly resistant to direct (cis) HIV-1 infection in vitro, in particular to R5-tropic HIV-1, as TN do not express CCR5. In this study, we investigated whether TN could be efficiently HIV-1 trans infected by professional antigen-presenting B lymphocytes and myeloid dendritic cells (DC) in the absence of global T cell activation. We found that B cells, but not DC, have a unique ability to efficiently trans infect TNin vitro In contrast, both B cells and DC mediated HIV-1 trans infection of memory and activated CD4+ T cells. Moreover, we found that TN isolated from HIV-1-infected nonprogressors (NP) harbor significantly disproportionately lower levels of HIV-1 DNA than TN isolated from progressors. This is consistent with our previous finding that antigen-presenting cells (APC) derived from NP do not efficiently trans infect CD4+ T cells due to alterations in APC cholesterol metabolism and cell membrane lipid raft organization. These findings support that B cell-mediated trans infection of TN with HIV-1 has a more profound role than previously considered in establishing the viral reservoir and control of HIV-1 disease progression.IMPORTANCE The latent human immunodeficiency virus type 1 (HIV-1) reservoir in persons on antiretroviral therapy (ART) represents a major barrier to a cure. Although most studies have focused on the HIV-1 reservoir in the memory T cell subset, replication-competent HIV-1 has been isolated from TN, and CCR5-tropic HIV-1 has been recovered from CCR5neg TN from ART-suppressed HIV-1-infected individuals. In this study, we showed that CCR5neg TN are efficiently trans infected with R5-tropic HIV-1 by B lymphocytes, but not by myeloid dendritic cells. Furthermore, we found that TN isolated from NP harbor no or significantly fewer copies of HIV-1 DNA than those from ART-suppressed progressors. These findings support that B cell-mediated trans infection of TN with HIV-1 has a more profound role than previously considered in establishing the viral reservoir and control of HIV-1 disease progression. Understanding the establishment and maintenance of the HIV-1 latent reservoir is fundamental for the design of effective treatments for viral eradication.

Highlights

  • Insight into the establishment and maintenance of human immunodeficiency virus type 1 (HIV-1) infection in resting CD41 T cell subsets is critical for the development of therapeutics targeting the HIV-1 reservoir

  • We first extended this finding by demonstrating that B cells or dendritic cells (DC) loaded with a low, 1023 multiplicity of infection (MOI) of R5-tropic HIV-1BaL could trans infect phytohemagglutinin (PHA)/IL-2-activated CD41 T cells, with the efficiency of trans infection being significantly greater for B cells than DC

  • This is of importance because, as we showed previously, only about 10 to 15% of activated B cells express DC-specific intercellular adhesion molecule-3-grabbing nonintegrin (DC-SIGN), compared to 100% of DC, potentially implicating B cells as more efficient than DC in mediating HIV-1 trans infection

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Summary

Introduction

Insight into the establishment and maintenance of HIV-1 infection in resting CD41 T cell subsets is critical for the development of therapeutics targeting the HIV-1 reservoir. We found that TN isolated from HIV-1-infected nonprogressors (NP) harbor significantly disproportionately lower levels of HIV-1 DNA than TN isolated from progressors This is consistent with our previous finding that antigen-presenting cells (APC) derived from NP do not efficiently trans infect CD41 T cells due to alterations in APC cholesterol metabolism and cell membrane lipid raft organization. TN isolated from NP harbor significantly lower levels of HIV-1 DNA than do TN isolated from HIV-1 progressors (PR) These findings support that B cell-mediated trans infection of TN with HIV-1 has a more profound role than previously considered in establishing the viral reservoir and control of HIV-1 disease progression

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