Human Immunodeficiency Virus Viremia Induces Plasmacytoid Dendritic Cell Activation In Vivo and Diminished Alpha Interferon Production In Vitro

Tilton, John C.; Manion, Maura; Luskin, Marlise R.; Johnson, Alison J.; Patamawenu, Andy; Hallahan, Claire W.; Cogliano-Shutta, Nancy A.; Mican, Jo Ann M.; Davey, Richard T.; Kottilil, Shyam; Lifson, Jeffrey D.; Metcalf, Julia A.; Lempicki, Richard A.; Connors, Mark

doi:10.1128/jvi.01545-07

Cited by 75 publications

(110 citation statements)

References 66 publications

(60 reference statements)

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“…In addition, a strong increase in pDC density in the T cell zone in lymph nodes of asymptomatic HIV-infected patients was reported in an earlier study (37). Furthermore, it has been recently shown that pDCs are indeed chronically stimulated in HIV-infected patients and produce type I IFNs, which in turn contributes to their hyporesponsiveness to subsequent in vitro stimulation, probably through a negative regulatory feedback mechanism (38). Viral activation of pDCs can be regulated by either of the two TLRs, TLR7 or TLR9, which are considered to be the receptors that human and mouse pDCs use for recognition of RNA/retroviruses (39) and DNA (40), respectively.…”

Section: Discussionmentioning

confidence: 88%

The Absence of IDO Upregulates Type I IFN Production, Resulting in Suppression of Viral Replication in the Retrovirus-Infected Mouse

Hoshi¹,

Saito

Hara

et al. 2010

The Journal of Immunology

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Indoleamine 2,3-dioxygenase, the l-tryptophan–degrading enzyme, plays a key role in the powerful immunomodulatory effects on several different types of cells. Because modulation of IDO activities after viral infection may have great impact on disease progression, we investigated the role of IDO following infection with LP-BM5 murine leukemia virus. We found suppressed BM5 provirus copies and increased type I IFNs in the spleen from IDO knockout (IDO−/−) and 1-methyl-d-l-tryptophan–treated mice compared with those from wild-type (WT) mice. Additionally, the number of plasmacytoid dendritic cells in IDO−/− mice was higher in the former than in the WT mice. In addition, neutralization of type I IFNs in IDO−/− mice resulted in an increase in LP-BM5 viral replication. Moreover, the survival rate of IDO−/− mice or 1-methyl-d-l-tryptophan–treated mice infected with LP-BM5 alone or with both Toxoplasma gondii and LP-BM5 was clearly greater than the survival rate of WT mice. To our knowledge, the present study is the first report to observe suppressed virus replication with upregulated type I IFN in IDO−/− mice, suggesting that modulation of the IDO pathway may be an effective strategy for treatment of virus infection.

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Section: Discussionmentioning

confidence: 88%

The Absence of IDO Upregulates Type I IFN Production, Resulting in Suppression of Viral Replication in the Retrovirus-Infected Mouse

Hoshi¹,

Saito

Hara

et al. 2010

The Journal of Immunology

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“…[18][19][20] Third, pDCs became unresponsive to secondary stimulation once the acute IFN-I response was over, suggesting that they were desensitized for IFN-I production in vivo as observed previously for human pDCs in vitro after primary stimulation with Toll-like receptor-9 ligand 41 and consistent with the reduced ability of pDCs to produce IFN-I in response to in vitro stimulation in patients infected with HIV. 42 Fourth, we did not evidence IFN-I-positive cell clusters outside the pDCs gate in our in vitro stimulation studies.For the first time, our study monitored the acute transient burst of IDO activity in parallel with acute changes in pDCs dynamics and IFN-I concentration in the early phase of viremia. The kinetic of IDO activity in cynomolgus macaques in our study and the positive correlation observed between IDO activity and viral load are consistent with observations made in Indian rhesus macaques.…”

mentioning

confidence: 93%

“…on May 10, 2018. by guest www.bloodjournal.org From in vitro production of IFN-I in patients infected with HIV. 42 As IFN-I became undetectable soon after its concentration peaked in the plasma, despite the persistence of high viral loads in our study, we compared the capacity of pDCs to respond to SIV and HSV-1 stimulation before and after this peak, to evaluate a possible refractory phase in vivo.In vitro, cynomolgus macaque pDCs underwent rapid IFN-␣ synthesis in response to SIV stimulation ( Figure 5A), as previously shown in response to HSV stimulation. 24 These cells were also characterized extensively by flow cytometry ( Figure S3).…”

mentioning

confidence: 99%

Primary infection with simian immunodeficiency virus: plasmacytoid dendritic cell homing to lymph nodes, type I interferon, and immune suppression

Malleret

Manéglier

Karlsson

et al. 2008

Blood

141

130

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Plasmacytoid dendritic cells (pDCs) are antigen-presenting cells that develop into type-I interferon (IFN-I IntroductionPlasmacytoid dendritic cells (pDCs) are major type I interferon (IFN-I) producing cells in response to viral infections 1 as a result of selective expression of Toll-like receptors 7 and 9 and constitutive expression of interferon response factor 7. They migrate to inflamed lymph nodes (LN) through high endothelium venules during viral and bacterial infections 2,3 and provide an important link between innate and adaptive immunity, enhancing natural killer (NK) cell activity and adaptive immune responses.Blood pDC counts and pDC-dependent IFN-I production levels in vitro decrease in patients infected with human immunodeficiency virus (HIV). [4][5][6][7][8] These decreases are generally correlated with a fall in CD4 ϩ T-cell counts, inversely correlated with plasma viral load, and are associated with opportunistic infections. 5,6,[9][10][11][12] The reduction in circulating pDC numbers during HIV infection may be related to their direct infection, 6,9,13 or to redistribution to lymphoid organs, as suggested in the chronic asymptomatic stage of HIV infection. 14 In nonhuman primate models of HIV infection, the IFN-I innate response is an early immunologic event. [15][16][17] Rhesus macaque (Macaca mulatta) pDCs are activated and produce IFN-I in vitro in response to pathogenic simian immunodeficiency virus (SIV) 18,19 like their human counterparts in response to HIV. 20,21 Strong depletion of pDCs from blood and lymphoid tissues are reported in the end stage of SIV infection 19,22 and attributed to infection and to higher levels of apoptosis.However, although the HIV/SIV interplay with the host immune response during primary infection is a key event, probably determining the later progression to disease, little is known about the role of pDCs in immune regulation at this early stage.We predicted that HIV/SIV infection may have an impact on the dynamics of circulating and LN dendritic cells (DCs) and on their functions in the first few days of infection 23,24 and that it may induce immune suppression through IFN-I production and indoleamine-2,3-dioxygenase (IDO) activity. IDO is the ratelimiting enzyme responsible for the extrahepatic catabolism of the essential amino acid tryptophan (Trp) and is triggered by type I and type II interferons. [25][26][27] Abnormal production/activation of IDO is associated with inefficient immunologic responses to infections, including HIV/SIV and cancer 26,[28][29][30] and is induced by HIV in human pDCs in vitro. 20,21 Growing evidence suggests that pDCs are involved in the induction of tolerance through IDO-dependent mechanisms. 31 This suggests that pDCs may target immune suppression during the acute phase of HIV/SIV infection.We focused on the dynamics of pDCs during primary infection by carrying out fine time-resolution sampling of blood, and a longitudinal analysis of peripheral lymph nodes, using absolute quantification, to investigate the possible homing of ...

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“…Significantly, a higher level of IRF7 RNA in ART naïve viremic subjects is in discrepancy with lower IFNα production by these subjects. There is some recent evidence which suggests that IFNα production is high in vivo in HIV infected progressors but a combination of feedback inhibition and prior direct activation through TLRs by HIV RNA leads to diminished ex-vivo IFNα production upon exposure to CpG-A or HIV particles [45]. While the IRF7 gene expression was assessed in terms of its mRNA abundance in the peripheral blood of the subjects, the IFNα levels were based on an in vitro stimulation assay, the two parameters could not be correlated and may be the reason of this discrepancy.…”

Section: Discussionmentioning

confidence: 99%

Increased Activity of NK Cells and Plasmacytoid Dendritic Cells in HIV-Exposed Seronegative (ESN) Individuals

Singla¹,

Jacobs²,

Schmidt³

et al. 2012

WJA

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The mechanisms involved in resistance to HIV-1 infection, especially the role of innate immune response, have not been thoroughly explored in individuals who are repeatedly exposed to HIV-1, but do not get the infection, termed as Exposed sero-negative or ESN. Frequency and activation state of natural killer (NK) cells and plasmacytoid dendritic cells (pDC) in ESNs from North India were compared with those in recently infected HIV positives (RHIV), chronically infected HIV positives (HIV+) and healthy controls (HC). The activation state of NK cells in terms of cytokine response (IFNγ & TNFα) was significantly higher in ESNs compared to the healthy controls, recently infected HIV+ and chronically infected HIV+. Although the number of circulating pDC in different study groups was not significantly different, yet these cells seem to have significantly higher activation state in terms of IFNα production (ex-vivo in response to CpG ODN) in ESNs when compared with other groups. Increased activation status of NK cells and pDC in Exposed but Seronegative individuals indicates their continuous stimulation with HIV antigens due to regular exposure with infected partners and which might be imparting resistance to viral infection in these individuals

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Human Immunodeficiency Virus Viremia Induces Plasmacytoid Dendritic Cell Activation In Vivo and Diminished Alpha Interferon Production In Vitro

Cited by 75 publications

References 66 publications

The Absence of IDO Upregulates Type I IFN Production, Resulting in Suppression of Viral Replication in the Retrovirus-Infected Mouse

The Absence of IDO Upregulates Type I IFN Production, Resulting in Suppression of Viral Replication in the Retrovirus-Infected Mouse

Primary infection with simian immunodeficiency virus: plasmacytoid dendritic cell homing to lymph nodes, type I interferon, and immune suppression

Increased Activity of NK Cells and Plasmacytoid Dendritic Cells in HIV-Exposed Seronegative (ESN) Individuals

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