Plasma Levels of Bacterial DNA Correlate with Immune Activation and the Magnitude of Immune Restoration in Persons with Antiretroviral‐Treated HIV Infection

Jiang, Wei; Lederman, Michael M.; Hunt, Peter W.; Sieg, Scott F.; Haley, Kathryn P.; Rodrı́guez, Benigno; Landay, Alan; Martin, Jeffrey N.; Sinclair, Elizabeth; Asher, Ava I.; Deeks, Steven G.; Douek, Daniel C.; Brenchley, Jason M.

doi:10.1086/597476

Cited by 513 publications

(557 citation statements)

References 34 publications

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“…However, the underlying pathogenic mechanisms are still a topic of debate. Three potential causes of immune activation have been identified, as follows: 1) increased translocation of microbial products across the gut wall (12), 2) CMV coinfection (13,14), and 3) residual low-level HIV replication, identified in studies of ART intensification therapy with HIV integrase inhibitors (15,16). Irrespective of whether one or more of these factors cause persistent immune activation, we and others have demonstrated that elevated expression of IFNstimulated genes (ISG) in separated CD4 + T cells (17), separated accessory cells (18), or PBMC (19) is the strongest correlate of persistent CD4 + T cell deficiency in treated HIV patients.…”

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confidence: 99%

IFN-α Exerts Opposing Effects on Activation-Induced and IL-7–Induced Proliferation of T Cells That May Impair Homeostatic Maintenance of CD4+ T Cell Numbers in Treated HIV Infection

Cha

Jong

French

et al. 2014

The Journal of Immunology

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To determine whether IFN-α is a cause of the T cell hyperactivation and IL-7 signaling pathway defects that are observed in some HIV patients receiving antiretroviral therapy, we have investigated the effect of IFN-α on the proliferation of CD4+ and CD8+ T cells from healthy donors (n = 30) and treated HIV+ donors (n = 20). PBMC were cultured for 7 d with staphylococcal enterotoxin B or IL-7 in the absence or presence of 100 U/ml IFN-α8. Total and naive CD4+ and CD8+ T cells were assessed for proliferation (via Ki67 expression), CD127 expression, and phosphorylated STAT5 levels using flow cytometry. IFN-α significantly enhanced activation-induced proliferation (via staphylococcal enterotoxin B stimulation) but inhibited homeostatic proliferation (IL-7 induced) of CD4+ and CD8+ T cells. Both of these effects may adversely affect CD4+ T cell homeostasis in HIV patients. CD127 expression was increased in both healthy and HIV+ donors following culture with IFN-α8, and levels of IL-7–induced phosphorylated STAT5 were increased by IFN-α8 in healthy donors only. Hence, the inhibitory effects of IFN-α on IL-7–induced proliferation of CD4+ T cells are unlikely to be mediated by downregulation of CD127 expression or inhibition of STAT5 phosphorylation. These data suggest that increased IFN-α activity may promote the loss of T cells by accelerating cell turnover and activation-induced cell death while decreasing the renewal of T cells by inhibiting the proliferative effect of IL-7.

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confidence: 99%

IFN-α Exerts Opposing Effects on Activation-Induced and IL-7–Induced Proliferation of T Cells That May Impair Homeostatic Maintenance of CD4+ T Cell Numbers in Treated HIV Infection

Cha

Jong

French

et al. 2014

The Journal of Immunology

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“…So as CD4+ T-cell numbers decrease in HIV condition, HLA-DR+ and CD38+ CD8+ T lymphocytes rather appreciate in numbers [5]. Further studies has also established that viral load cannot separately determine the rate of progression to AIDS, and that immune activation better reflects variations in CD4+ T-cell stronger and independent of viral load [6][7][8][9].…”

Section: Open Access Http://scidocorg/ijmaiphpmentioning

confidence: 99%

Lymphocyte Subset (CD3, CD4 and CD8 Cells) and their Ratios in HIV patients on Highly Active Antiretroviral Therapy (HAART) and HAART Naïve Patients

OK¹,

FJ²

2018

IJMAI

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“…Bacterial translocation from the GI tract to the peripheral circulation has been extensively studied in HIV infection, but is also common in liver disease and other conditions (24)(25)(26)(27). Translocation occurs early in HIV infection due to depletion of gut CD41 lymphocytes and is not completely eradicated by ART, particularly in patients with a suboptimal CD4 cell count or HIV viral level responses (25,28). Persistent systemic exposure to bacterial antigens from MT triggers immune activation and inflammation in HIVinfected adults (25,26).…”

Section: Bacteria and The Gi Tractmentioning

confidence: 99%

“…Translocation occurs early in HIV infection due to depletion of gut CD41 lymphocytes and is not completely eradicated by ART, particularly in patients with a suboptimal CD4 cell count or HIV viral level responses (25,28). Persistent systemic exposure to bacterial antigens from MT triggers immune activation and inflammation in HIVinfected adults (25,26). MT is associated with T-cell activation, which predicts systemic inflammation, mortality, HIV progression, and progression of comorbidities such as cardiovascular disease (25,26,(29)(30)(31).…”

Section: Bacteria and The Gi Tractmentioning

confidence: 99%

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Heart–Lung Interaction via Infection

Morris

2014

Annals ATS

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Lung and cardiovascular disease are increasingly recognized to occur in the same patient populations. Infections, either through stimulation of inflammation or through direct infection, can lead to end-organ damage and have been postulated as a potential link between lung and cardiovascular diseases. Mechanisms by which infections may link lung and cardiac diseases include effects of systemic infections, microbial translocation of pathogens from the gastrointestinal tract or other sites, damaging effects of metabolic products, or influences of smoking on the microbiome.Other mechanisms, such as alterations in the local microbiome, environmental exposures, or immune regulation by microbial communities, may be important. These relationships are likely quite complex, with multiple routes between infection and disease possible. A better understanding of the links of infection to lung and heart disease can improve our understanding of the pathogenesis of these disorders and uncover novel therapeutic approaches.Keywords: microbial translocation; metabolomics; pulmonary function; cardiovascular; HIV Correspondence and requests for reprints should be addressed to Alison Morris, M.D., M.S.,

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Plasma Levels of Bacterial DNA Correlate with Immune Activation and the Magnitude of Immune Restoration in Persons with Antiretroviral‐Treated HIV Infection

Cited by 513 publications

References 34 publications

IFN-α Exerts Opposing Effects on Activation-Induced and IL-7–Induced Proliferation of T Cells That May Impair Homeostatic Maintenance of CD4+ T Cell Numbers in Treated HIV Infection

IFN-α Exerts Opposing Effects on Activation-Induced and IL-7–Induced Proliferation of T Cells That May Impair Homeostatic Maintenance of CD4+ T Cell Numbers in Treated HIV Infection

Lymphocyte Subset (CD3, CD4 and CD8 Cells) and their Ratios in HIV patients on Highly Active Antiretroviral Therapy (HAART) and HAART Naïve Patients

Heart–Lung Interaction via Infection

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