Cell-to-Cell Spreading of HIV-1 in Myeloid Target Cells Escapes SAMHD1 Restriction.

Maorong Xie,Rémi Mascarau,Camille Ciccone,Alain Schmitt,Serge Benichou,Brigitte Raynaud-Messina,Christel Vérollet,Marie Woottum,Maeva Dupont,Héloïse Leroy,Lucie Bracq,Jérôme Bouchet

doi:10.1128/mbio.02457-19

Abstract

Dendritic cells (DCs) and macrophages as well as osteoclasts (OCs) are emerging as target cells of HIV-1 involved in virus transmission, dissemination, and establishment of persistent tissue virus reservoirs. While these myeloid cells are poorly infected by cell-free viruses because of the high expression levels of cellular restriction factors such as SAMHD1, we show here that HIV-1 uses a specific and common cell-to-cell fusion mechanism for virus transfer and dissemination from infected T lymphocytes to the target cells of the myeloid lineage, including immature DCs (iDCs), OCs, and macrophages, but not monocytes and mature DCs. The establishment of contacts with infected T cells leads to heterotypic cell fusion for the fast and massive transfer of viral material into OC and iDC targets, which subsequently triggers homotypic fusion with noninfected neighboring OCs and iDCs for virus dissemination. These two cell-to-cell fusion processes are not restricted by SAMHD1 and allow very efficient spreading of virus in myeloid cells, resulting in the formation of highly virus-productive multinucleated giant cells. These results reveal the cellular mechanism for SAMHD1-independent cell-to-cell spreading of HIV-1 in myeloid cell targets through the formation of the infected multinucleated giant cells observed in vivo in lymphoid and nonlymphoid tissues of HIV-1-infected patients.IMPORTANCE We demonstrate that HIV-1 uses a common two-step cell-to-cell fusion mechanism for massive virus transfer from infected T lymphocytes and dissemination to myeloid target cells, including dendritic cells and macrophages as well as osteoclasts. This cell-to-cell infection process bypasses the restriction imposed by the SAMHD1 host cell restriction factor for HIV-1 replication, leading to the formation of highly virus-productive multinucleated giant cells as observed in vivo in lymphoid and nonlymphoid tissues of HIV-1-infected patients. Since myeloid cells are emerging as important target cells of HIV-1, these results contribute to a better understanding of the role of these myeloid cells in pathogenesis, including cell-associated virus sexual transmission, cell-to-cell virus spreading, and establishment of long-lived viral tissue reservoirs.

Highlights

Dendritic cells (DCs) and macrophages as well as osteoclasts (OCs) are emerging as target cells of HIV-1 involved in virus transmission, dissemination, and establishment of persistent tissue virus reservoirs
Since we and others have previously reported that HIV-1 could be efficiently transferred from T cells to macrophages through cell-to-cell contacts, we investigated whether HIV-1 could be transferred to other myeloid cell targets, i.e., DCs and OCs
In this report, we reveal that HIV-1 uses a specific and common two-step cell fusion process for cell-to-cell transfer and dissemination from infected CD4ϩ T cells to target cells of the myeloid lineage, including macrophages, OCs, and immature DCs (iDCs), but not monocytes and mDCs

Summary

Introduction

Dendritic cells (DCs) and macrophages as well as osteoclasts (OCs) are emerging as target cells of HIV-1 involved in virus transmission, dissemination, and establishment of persistent tissue virus reservoirs. This propagation route is very efficient and involves the different cell types targeted by HIV-1, including cells of the myeloid lineage (i.e., macrophages, DCs, and OCs) [22, 24,25,26], which are not infected by cell-free viruses, mainly because of the high expression of cellular restriction factors, including SAMHD1, an enzyme that cleaves deoxynucleoside triphosphates (dNTPs) and depletes the pool of intracellular nucleotides necessary for efficient HIV-1 replication in these noncycling myeloid cells [16, 27,28,29,30,31] This cell-to-cell mode of infection likely plays important roles at the level of genital and rectal mucosa and for virus spread in numerous host tissues. While it was reported previously by the group of Quentin Sattentau that macrophages could be infected via selective capture or phagocytosis of HIV-1-infected T cells [26], we have reported that HIV-1 is mainly transferred to macrophages from infected T cells by a two-step cell fusion process [25]

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