HIV Persistence in Adipose Tissue Reservoirs

Couturier, Jacob; Lewis, Dorothy E.

doi:10.1007/s11904-018-0378-z

Cited by 46 publications

(34 citation statements)

References 132 publications

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“…The results presented here demonstrate that adipocytes have significant impact on ART distribution and activity within AT, which is newly believed to constitute a reservoir for latently infected HIV-/SIV-infected CD4 T cells (Couturier et al, 2015; Damouche et al, 2015; Couturier et al, 2016; Damouche et al, 2017; Hsu et al, 2017; Koethe et al, 2017; Couturier et al, 2018). In particular, these data suggest that adipocytes markedly diminish the antiretroviral effectiveness of NRTIs, particularly tenofovir, which constitutes an important “backbone” component of many antiretroviral regimens and is a first line agent for the treatment of HIV infection.…”

Section: Discussionmentioning

confidence: 66%

“…They observed that NNRTI concentrations were significantly higher in AT lysates compared to PI concentrations, whereas N(t)RTIs were undetectable. Others and we have recently demonstrated that latently-infected CD4 T cells accumulate in AT and establish replication-competent reservoirs during chronic HIV infection, indicating the need for better understanding of antiretroviral pharmacology in AT (Couturier et al, 2015; Damouche et al, 2015; Couturier et al, 2016; Damouche et al, 2017; Hsu et al, 2017; Koethe et al, 2017; Couturier et al, 2018). …”

Section: Introductionmentioning

confidence: 93%

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Adipocytes impair efficacy of antiretroviral therapy

et al. 2018

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Adequate distribution of antiretroviral drugs to infected cells in HIV patients is critical for viral suppression. In humans and primates, HIV- and SIV-infected CD4 T cells in adipose tissues have recently been identified as reservoirs for infectious virus. To better characterize adipose tissue as a pharmacological sanctuary for HIV-infected cells, in vitro experiments were conducted to assess antiretroviral drug efficacy in the presence of adipocytes, and drug penetration in adipose tissue cells (stromal-vascular-fraction cells and mature adipocytes) was examined in treated humans and monkeys. Co-culture experiments between HIV-1-infected CD4 T cells and primary human adipocytes showed that adipocytes consistently reduced the antiviral efficacy of the nucleotide reverse transcriptase inhibitor tenofovir and its prodrug forms tenofovir disoproxil fumarate (TDF) and tenofovir alafenamide (TAF). In HIV-infected persons, LC-MS/MS analysis of intracellular lysates derived from adipose tissue stromal-vascular-fraction cells or mature adipocytes suggested that integrase inhibitors penetrate adipose tissue, whereas penetration of nucleoside/nucleotide reverse transcriptase inhibitors such as TDF, emtricitabine, abacavir, and lamivudine is restricted. The limited distribution and functions of key antiretroviral drugs within fat depots may contribute to viral persistence in adipose tissue.

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Section: Discussionmentioning

confidence: 66%

Section: Introductionmentioning

confidence: 93%

Adipocytes impair efficacy of antiretroviral therapy

et al. 2018

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“…Latest data also provided evidence for a decreased NK cell number in mice orally infected with Salmonella Typhimurium, which also may contribute to an impaired susceptibility for infections in obese individuals (174). Interestingly, it has been proposed that selective therapeutic drugs might get trapped in adipose tissue in the treatment of HIV infections and, furthermore, immune cells, including NK cells, could be retained in adipose tissue, blocking their immunosurveillance elsewhere in the body (175).…”

Section: The Impact Of Obesity-related Altered Nk Cell Functionality mentioning

confidence: 99%

Obesity-Associated Alterations of Natural Killer Cells and Immunosurveillance of Cancer

et al. 2020

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Obesity is accompanied by a systemic chronic low-grade inflammation as well as dysfunctions of several innate and adaptive immune cells. Recent findings emphasize an impaired functionality and phenotype of natural killer (NK) cells under obese conditions. This review provides a detailed overview on research related to overweight and obesity with a particular focus on NK cells. We discuss obesity-associated alterations in subsets, distribution, phenotype, cytotoxicity, cytokine secretion, and signaling cascades of NK cells investigated in vitro as well as in animal and human studies. In addition, we provide recent insights into the effects of physical activity and obesity-associated nutritional factors as well as the reduction of body weight and fat mass on NK cell functions of obese individuals. Finally, we highlight the impact of impaired NK cell physiology on obesity-associated diseases, focusing on the elevated susceptibility for viral infections and increased risk for cancer development and impaired treatment response.NK cells are large granular lymphocytes that mediate rapid innate immunity against viruses, bacteria, parasites, and tumor cells without prior sensitization. NK cells primarily develop and mature in the bone marrow, migrate through the bloodstream, and seed into secondary lymphoid organs, like thymus, spleen, and lymph nodes as well as in other peripheral tissues, like lung, liver, kidney, uterus, and the gastrointestinal tract (23). In blood, NK cells represent 1-6% of all leukocytes and comprise up to 15% of human peripheral blood mononuclear cells (PBMCs). Human NK cells have been defined by the expression of adhesion molecule CD56 and by the absence of the T cell marker CD3. Based on their expression level of CD56 and the Fcγ receptor CD16, NK cells are subdivided into different subpopulations. The two major and classically defined subsets are the CD56 dim CD16 bright NK cells and the CD56 bright CD16 dim/neg NK cells. CD56 dim CD16 bright NK cells represent about 90% of all NK cells and are predominantly found in peripheral blood (24). They are mostly responsible for cytotoxic activity and target cell killing but are also a source of pro-inflammatory Abbreviations: ACM, adipocyte-conditioned media; Adamts3, a disintegrin-like and metallopeptidase with thrombospondin type 1 motif, 3; AdipoR, adiponectin receptor; Anxa8, annexin A8; AT, adipose tissue; Bax, Bcl-2-associated X protein; Bcl, B-cell lymphoma; BMI, body mass index; CCR, CC chemokine receptor; Csf1r, colony stimulating factor 1 receptor; CX3CR1, C-X3-C-motif chemokine receptor 1; DNAM-1, DNAX accessory molecule-1; ESR, estrogen receptor; FasL, Fas ligand; IFN-γ, interferon; GM-CSF; granulocyte macrophage colony-stimulating factor; H6pd, hexose-6-phosphate dehydrogenase; Hk2, hexokinase 2; IL, interleukinIL-6R; interleukin-6 receptor; Il18rap, interleukin 18 receptor accessory protein; IP-10, interferon gamma-induced protein 10; JAK, Janus kinase; KIR, killer immunoglobulin-like receptor; Klra1, killer lectin-like receptor subfamil...

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“…Lastly, the discovery of memory T cell accumulation in AT as a means of providing efficient secondary responses against pathogens constituted a major breakthrough; it became clear that AT is an immune partner in both local and systemic immune responses (Han et al, 2017; Figure 5). However, AT is a reservoir for pathogens in various infectious contexts (Nishimura et al, 2000;Neyrolles et al, 2006;Desruisseaux et al, 2007;Dhurandhar, 2011;Nagajyothi et al, 2012;Couturier et al, 2015Couturier et al, , 2016Damouche et al, 2015;Trindade et al, 2016;Beigier-Bompadre et al, 2017;Tanowitz et al, 2017;Couturier and Lewis, 2018;Contreras et al, 2019; Table 2). The detection of various bacterial DNAs in AT also constitutes an argument in favor of the tissue-specific microbiota hypothesis (Burcelin et al, 2013).…”

Section: Adipose Tissue and Infectionsmentioning

confidence: 99%

Specific Biological Features of Adipose Tissue, and Their Impact on HIV Persistence

et al. 2019

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Although white AT can contribute to anti-infectious immune responses, it can also be targeted and perturbed by pathogens. The AT's immune involvement is primarily due to strong pro-inflammatory responses (with both local and paracrine effects), and the large number of fat-resident macrophages. Adipocytes also exert direct antimicrobial responses. In recent years, it has been found that memory T cells accumulate in AT, where they provide efficient secondary responses against viral pathogens. These observations have prompted researchers to re-evaluate the links between obesity and susceptibility to infections. In contrast, AT serves as a reservoir for several persistence pathogens, such as human adenovirus Ad-36, Trypanosoma gondii, Mycobacterium tuberculosis, influenza A virus, and cytomegalovirus (CMV). The presence and persistence of bacterial DNA in AT has led to the concept of a tissuespecific microbiota. The unexpected coexistence of immune cells and pathogens within the specific AT environment is intriguing, and its impact on anti-infectious immune responses requires further evaluation. AT has been recently identified as a site of HIV persistence. In the context of HIV infection, AT is targeted by both the virus and the antiretroviral drugs. AT's intrinsic metabolic features, large overall mass, and wide distribution make it a major tissue reservoir, and one that may contribute to the pathophysiology of chronic HIV infections. Here, we review the immune, metabolic, viral, and pharmacological aspects that contribute to HIV persistence in AT. We also evaluate the respective impacts of both intrinsic and HIV-induced factors on AT's involvement as a viral reservoir. Lastly, we examine the potential consequences of HIV persistence on the metabolic and immune activities of AT.

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HIV Persistence in Adipose Tissue Reservoirs

Cited by 46 publications

References 132 publications

Adipocytes impair efficacy of antiretroviral therapy

Adipocytes impair efficacy of antiretroviral therapy

Obesity-Associated Alterations of Natural Killer Cells and Immunosurveillance of Cancer

Specific Biological Features of Adipose Tissue, and Their Impact on HIV Persistence

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