Literature DB >> 26339043

Th1/17 Polarization of CD4 T Cells Supports HIV-1 Persistence during Antiretroviral Therapy.

Hong Sun1, Dhohyung Kim2, Xiaodong Li2, Maja Kiselinova3, Zhengyu Ouyang2, Linos Vandekerckhove4, Hong Shang5, Eric S Rosenberg6, Xu G Yu2, Mathias Lichterfeld7.   

Abstract

UNLABELLED: The ability to persist long term in latently infected CD4 T cells represents a characteristic feature of HIV-1 infection and the predominant barrier to efforts aiming at viral eradication and cure. Yet, increasing evidence suggests that only small subsets of CD4 T cells with specific developmental and maturational profiles are able to effectively support HIV-1 long-term persistence. Here, we analyzed how the functional polarization of CD4 T cells shapes and structures the reservoirs of HIV-1-infected cells. We found that CD4 T cells enriched for a Th1/17 polarization had elevated susceptibilities to HIV-1 infection in ex vivo assays, harbored high levels of HIV-1 DNA in persons treated with antiretroviral therapy, and made a disproportionately increased contribution to the viral reservoir relative to their contribution to the CD4 T memory cell pool. Moreover, HIV-1 DNA levels in Th1/17 cells remained stable over many years of antiretroviral therapy, resulting in a progressively increasing contribution of these cells to the viral reservoir, and phylogenetic studies suggested preferential long-term persistence of identical viral sequences during prolonged antiretroviral treatment in this cell compartment. Together, these data suggest that Th1/17 CD4 T cells represent a preferred site for HIV-1 DNA long-term persistence in patients receiving antiretroviral therapy. IMPORTANCE: Current antiretroviral therapy is very effective in suppressing active HIV-1 replication but does not fully eliminate virally infected cells. The ability of HIV-1 to persist long term despite suppressive antiretroviral combination therapy represents a perplexing aspect of HIV-1 disease pathogenesis, since most HIV-1 target cells are activated, short-lived CD4 T cells. This study suggests that CD4 T helper cells with Th1/17 polarization have a preferential role as a long-term reservoir for HIV-1 infection during antiretroviral therapy, possibly because these cells may imitate some of the functional properties traditionally attributed to stem cells, such as the ability to persist for extremely long periods of time and to repopulate their own pool size through homeostatic self-renewal. These observations support the hypothesis that HIV-1 persistence is driven by small subsets of long-lasting stem cell-like CD4 T cells that may represent particularly promising targets for clinical strategies aiming at HIV-1 eradication and cure.
Copyright © 2015, American Society for Microbiology. All Rights Reserved.

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Year:  2015        PMID: 26339043      PMCID: PMC4645661          DOI: 10.1128/JVI.01595-15

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  47 in total

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Journal:  Nat Rev Immunol       Date:  2013-12-13       Impact factor: 53.106

4.  Human TH17 cells are long-lived effector memory cells.

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Authors:  David Bending; Hugo De la Peña; Marc Veldhoen; Jenny M Phillips; Catherine Uyttenhove; Brigitta Stockinger; Anne Cooke
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6.  Human circulating PD-1+CXCR3-CXCR5+ memory Tfh cells are highly functional and correlate with broadly neutralizing HIV antibody responses.

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7.  HIV reservoir size and persistence are driven by T cell survival and homeostatic proliferation.

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10.  Limited HIV infection of central memory and stem cell memory CD4+ T cells is associated with lack of progression in viremic individuals.

Authors:  Nichole R Klatt; Steven E Bosinger; Melicent Peck; Laura E Richert-Spuhler; Anke Heigele; Jillian P Gile; Nirav Patel; Jessica Taaffe; Boris Julg; David Camerini; Carlo Torti; Jeffrey N Martin; Steven G Deeks; Elizabeth Sinclair; Frederick M Hecht; Michael M Lederman; Mirko Paiardini; Frank Kirchhoff; Jason M Brenchley; Peter W Hunt; Guido Silvestri
Journal:  PLoS Pathog       Date:  2014-08-28       Impact factor: 6.823

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Review 6.  Differentiating Immune Cell Targets in Gut-Associated Lymphoid Tissue for HIV Cure.

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8.  Differential effects of HIV transmission from monocyte-derived dendritic cells vs. monocytes to IL-17+CD4+ T cells.

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9.  Phenotypic analysis of the unstimulated in vivo HIV CD4 T cell reservoir.

Authors:  Jason Neidleman; Xiaoyu Luo; Julie Frouard; Guorui Xie; Feng Hsiao; Tongcui Ma; Vincent Morcilla; Ashley Lee; Sushama Telwatte; Reuben Thomas; Whitney Tamaki; Benjamin Wheeler; Rebecca Hoh; Ma Somsouk; Poonam Vohra; Jeffrey Milush; Katherine Sholtis James; Nancie M Archin; Peter W Hunt; Steven G Deeks; Steven A Yukl; Sarah Palmer; Warner C Greene; Nadia R Roan
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