Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells

Amelie Cattin; Vanessa Sue Wacleche; Natalia Fonseca Do Rosario; Laurence Raymond Marchand; Jonathan Dias; Annie Gosselin; Eric A. Cohen; Jerome Estaquier; Nicolas Chomont; Jean Pierre Routy; Petronela Ancuta

doi:10.4049/jimmunol.2001436

Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells

Amelie Cattin
, Vanessa Sue Wacleche
, Natalia Fonseca Do Rosario
, Laurence Raymond Marchand
, Jonathan Dias
, Annie Gosselin
, Eric A. Cohen
, Jerome Estaquier
, Nicolas Chomont
, Jean Pierre Routy
, Petronela Ancuta

Veterinary and Biomedical Sciences

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

HIV reservoirs persist in gut-homing CD4+ T cells of people living with HIV and receiving antiretroviral therapy, but the antigenic specificity of such reservoirs remains poorly documented. The imprinting for gut homing is mediated by retinoic acid (RA), a vitamin A_derived metabolite produced by dendritic cells (DCs) exhibiting RA-synthesizing (RALDH) activity. RALDH activity in DCs can be induced by TLR2 ligands, such as bacterial peptidoglycans and fungal zymosan. Thus, we hypothesized that bacterial/fungal pathogens triggering RALDH activity in DCs fuel HIV reservoir establishment/outgrowth in pathogenreactive CD4+ T cells. Our results demonstrate that DCs derived from intermediate/nonclassical CD16+ compared with classical CD162 monocytes exhibited superior RALDH activity and higher capacity to transmit HIV infection to autologous Staphylococcus aureus_reactive T cells. Exposure of total monocyte-derived DCs (MDDCs) to S. aureus lysates as well as TLR2 (zymosan and heat-killed preparation of Listeria monocytogenes) and TLR4 (LPS) agonists but not CMV lysates resulted in a robust upregulation of RALDH activity. MDDCs loaded with S. aureus or zymosan induced the proliferation of T cells with a CCR5+integrin β7⁺CCR6⁺phenotype and efficiently transmitted HIV infection to these T cells via RALDH/RA_dependent mechanisms. Finally, S. aureus_ and zymosan-reactive CD4+ T cells of antiretroviral therapy-treated people living with HIV carried replication-competent integrated HIV-DNA, as demonstrated by an MDDC-based viral outgrowth assay. Together, these results support a model in which bacterial/fungal pathogens in the gut promote RALDH activity in MDDCs, especially in CD16+ MDDCs, and subsequently imprint CD4+ T cells with gut-homing potential and HIV permissiveness. Thus, nonviral pathogens play key roles in fueling HIV reservoir establishment/outgrowth via RALDH/RA_dependent mechanisms that may be therapeutically targeted.

Original language	English (US)
Pages (from-to)	2638-2651
Number of pages	14
Journal	Journal of Immunology
Volume	206
Issue number	11
DOIs	https://doi.org/10.4049/jimmunol.2001436
State	Published - Jun 1 2021

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

All Science Journal Classification (ASJC) codes

Immunology and Allergy
Immunology

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10.4049/jimmunol.2001436

Cite this

Cattin, A., Wacleche, V. S., Do Rosario, N. F., Marchand, L. R., Dias, J., Gosselin, A., Cohen, E. A., Estaquier, J., Chomont, N., Routy, J. P., & Ancuta, P. (2021). Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells. Journal of Immunology, 206(11), 2638-2651. https://doi.org/10.4049/jimmunol.2001436

@article{e29e5e40944649d99ecdf87e2d24d992,

title = "Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells",

abstract = "HIV reservoirs persist in gut-homing CD4+ T cells of people living with HIV and receiving antiretroviral therapy, but the antigenic specificity of such reservoirs remains poorly documented. The imprinting for gut homing is mediated by retinoic acid (RA), a vitamin A\_derived metabolite produced by dendritic cells (DCs) exhibiting RA-synthesizing (RALDH) activity. RALDH activity in DCs can be induced by TLR2 ligands, such as bacterial peptidoglycans and fungal zymosan. Thus, we hypothesized that bacterial/fungal pathogens triggering RALDH activity in DCs fuel HIV reservoir establishment/outgrowth in pathogenreactive CD4+ T cells. Our results demonstrate that DCs derived from intermediate/nonclassical CD16+ compared with classical CD162 monocytes exhibited superior RALDH activity and higher capacity to transmit HIV infection to autologous Staphylococcus aureus\_reactive T cells. Exposure of total monocyte-derived DCs (MDDCs) to S. aureus lysates as well as TLR2 (zymosan and heat-killed preparation of Listeria monocytogenes) and TLR4 (LPS) agonists but not CMV lysates resulted in a robust upregulation of RALDH activity. MDDCs loaded with S. aureus or zymosan induced the proliferation of T cells with a CCR5+integrin β7+CCR6+phenotype and efficiently transmitted HIV infection to these T cells via RALDH/RA\_dependent mechanisms. Finally, S. aureus\_ and zymosan-reactive CD4+ T cells of antiretroviral therapy-treated people living with HIV carried replication-competent integrated HIV-DNA, as demonstrated by an MDDC-based viral outgrowth assay. Together, these results support a model in which bacterial/fungal pathogens in the gut promote RALDH activity in MDDCs, especially in CD16+ MDDCs, and subsequently imprint CD4+ T cells with gut-homing potential and HIV permissiveness. Thus, nonviral pathogens play key roles in fueling HIV reservoir establishment/outgrowth via RALDH/RA\_dependent mechanisms that may be therapeutically targeted.",

author = "Amelie Cattin and Wacleche, \{Vanessa Sue\} and \{Do Rosario\}, \{Natalia Fonseca\} and Marchand, \{Laurence Raymond\} and Jonathan Dias and Annie Gosselin and Cohen, \{Eric A.\} and Jerome Estaquier and Nicolas Chomont and Routy, \{Jean Pierre\} and Petronela Ancuta",

year = "2021",

month = jun,

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doi = "10.4049/jimmunol.2001436",

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Cattin, A, Wacleche, VS, Do Rosario, NF, Marchand, LR, Dias, J, Gosselin, A, Cohen, EA, Estaquier, J, Chomont, N, Routy, JP & Ancuta, P 2021, 'Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells', Journal of Immunology, vol. 206, no. 11, pp. 2638-2651. https://doi.org/10.4049/jimmunol.2001436

TY - JOUR

T1 - Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells

AU - Cattin, Amelie

AU - Wacleche, Vanessa Sue

AU - Do Rosario, Natalia Fonseca

AU - Marchand, Laurence Raymond

AU - Dias, Jonathan

AU - Gosselin, Annie

AU - Cohen, Eric A.

AU - Estaquier, Jerome

AU - Chomont, Nicolas

AU - Routy, Jean Pierre

AU - Ancuta, Petronela

PY - 2021/6/1

Y1 - 2021/6/1

N2 - HIV reservoirs persist in gut-homing CD4+ T cells of people living with HIV and receiving antiretroviral therapy, but the antigenic specificity of such reservoirs remains poorly documented. The imprinting for gut homing is mediated by retinoic acid (RA), a vitamin A_derived metabolite produced by dendritic cells (DCs) exhibiting RA-synthesizing (RALDH) activity. RALDH activity in DCs can be induced by TLR2 ligands, such as bacterial peptidoglycans and fungal zymosan. Thus, we hypothesized that bacterial/fungal pathogens triggering RALDH activity in DCs fuel HIV reservoir establishment/outgrowth in pathogenreactive CD4+ T cells. Our results demonstrate that DCs derived from intermediate/nonclassical CD16+ compared with classical CD162 monocytes exhibited superior RALDH activity and higher capacity to transmit HIV infection to autologous Staphylococcus aureus_reactive T cells. Exposure of total monocyte-derived DCs (MDDCs) to S. aureus lysates as well as TLR2 (zymosan and heat-killed preparation of Listeria monocytogenes) and TLR4 (LPS) agonists but not CMV lysates resulted in a robust upregulation of RALDH activity. MDDCs loaded with S. aureus or zymosan induced the proliferation of T cells with a CCR5+integrin β7+CCR6+phenotype and efficiently transmitted HIV infection to these T cells via RALDH/RA_dependent mechanisms. Finally, S. aureus_ and zymosan-reactive CD4+ T cells of antiretroviral therapy-treated people living with HIV carried replication-competent integrated HIV-DNA, as demonstrated by an MDDC-based viral outgrowth assay. Together, these results support a model in which bacterial/fungal pathogens in the gut promote RALDH activity in MDDCs, especially in CD16+ MDDCs, and subsequently imprint CD4+ T cells with gut-homing potential and HIV permissiveness. Thus, nonviral pathogens play key roles in fueling HIV reservoir establishment/outgrowth via RALDH/RA_dependent mechanisms that may be therapeutically targeted.

AB - HIV reservoirs persist in gut-homing CD4+ T cells of people living with HIV and receiving antiretroviral therapy, but the antigenic specificity of such reservoirs remains poorly documented. The imprinting for gut homing is mediated by retinoic acid (RA), a vitamin A_derived metabolite produced by dendritic cells (DCs) exhibiting RA-synthesizing (RALDH) activity. RALDH activity in DCs can be induced by TLR2 ligands, such as bacterial peptidoglycans and fungal zymosan. Thus, we hypothesized that bacterial/fungal pathogens triggering RALDH activity in DCs fuel HIV reservoir establishment/outgrowth in pathogenreactive CD4+ T cells. Our results demonstrate that DCs derived from intermediate/nonclassical CD16+ compared with classical CD162 monocytes exhibited superior RALDH activity and higher capacity to transmit HIV infection to autologous Staphylococcus aureus_reactive T cells. Exposure of total monocyte-derived DCs (MDDCs) to S. aureus lysates as well as TLR2 (zymosan and heat-killed preparation of Listeria monocytogenes) and TLR4 (LPS) agonists but not CMV lysates resulted in a robust upregulation of RALDH activity. MDDCs loaded with S. aureus or zymosan induced the proliferation of T cells with a CCR5+integrin β7+CCR6+phenotype and efficiently transmitted HIV infection to these T cells via RALDH/RA_dependent mechanisms. Finally, S. aureus_ and zymosan-reactive CD4+ T cells of antiretroviral therapy-treated people living with HIV carried replication-competent integrated HIV-DNA, as demonstrated by an MDDC-based viral outgrowth assay. Together, these results support a model in which bacterial/fungal pathogens in the gut promote RALDH activity in MDDCs, especially in CD16+ MDDCs, and subsequently imprint CD4+ T cells with gut-homing potential and HIV permissiveness. Thus, nonviral pathogens play key roles in fueling HIV reservoir establishment/outgrowth via RALDH/RA_dependent mechanisms that may be therapeutically targeted.

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Raldh activity induced by bacterial/fungal pathogens in cd16+ monocyte-derived dendritic cells boosts hiv infection and outgrowth in cd4+ t cells

Abstract

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