The TRAIL of Helpless CD8<sup>+</sup>T Cells in HIV Infection

Küerten, Stefanie; Asaad, Robert; Schoenberger, Stephen P.; Angelov, Doychin N.; Lehmann, Paul; Tary‐Lehmann, Magdalena

doi:10.1089/aid.2008.0062

Cited by 14 publications

(12 citation statements)

References 49 publications

(62 reference statements)

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“…These markers and cytokines are associated with exhaustion and/ or apoptosis. There are other markers and cytokines linked to P38 activation, which are also shown to be elevated in HIV-1 infection including TGF-b1 [49] and TRAIL [50]. Additional analysis of these immunological markers in HIV infection may further emphasize the critical role of P38 signaling in HIV infection.…”

Section: Hiv Infection and P38 Signalingmentioning

confidence: 98%

“…They concluded that sustained ERK activation was required to produce IL-2 through T-cell receptor activation. TNF-a Inflammation [42] HIV* TGF-bl, TRAIL Exhaustion, Apoptosis [49,50] * Biomarkers that are upregulated in HIV-1 infection and play a role in the P38 pathway, but without a reported connection between HIV and P38…”

Section: Hiv Infection and Erk Signalingmentioning

confidence: 99%

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Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Furler

Uíttenbogaart

2010

Immunol Res

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One of the defining characteristics of HIV is its ability to manipulate the human immune response to promote its own replication. Since the beginning of the epidemic, there has been controversy whether a robust immune response to the virus is beneficial or detrimental for the host. Therefore, the effects of HIV on signaling pathways and cytokine production need to be characterized in order to distinguish between protective immune responses and inappropriate immune activation. Cytokine and biomarker expression during HIV infection results from the combined effects of intracellular signaling pathways orchestrated by kinases like P38 and ERK. The P38 and ERK Mitogen-Activated Protein Kinase (MAPK) pathways govern the regulation of cytokines (IL-2, IL-10, and TNF-α) as well biomarkers (PD-1, Fas/FasL, among others) that are skewed in chronic HIV infection. HIV utilizes the P38 and ERK pathways to produce new virions and to deplete CD4+ T cells from the host's immune system. Understanding the interplay between HIV and the cytokines induced by activation of the P38 and ERK pathways may provide insights into HIV immunopathogenesis and the development of a protective vaccine.

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Section: Hiv Infection and P38 Signalingmentioning

confidence: 98%

Section: Hiv Infection and Erk Signalingmentioning

confidence: 99%

Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Furler

Uíttenbogaart

2010

Immunol Res

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“…Specifically, CD8 + T cells activated without CD4 + T cell help express TRAIL and undergo AICD upon secondary Ag stimulation (Janssen et al, 2005; Wolkers et al, 2011; Feau et al, 2012; Wolkers et al, 2012). Immune unresponsiveness associated with the generation of such TRAIL-expressing ‘helpless’ CD8 T cells has been reported in a number of experimental models and clinical settings (Hamilton et al, 2006; Griffith et al, 2007; Kuerten et al, 2008; Gurung et al, 2010; Unsinger et al, 2010; Griffith et al, 2011; Gurung et al, 2011), but this concept has proven to be more tenuous in some models of infection (see below) (Badovinac et al, 2006; Sacks & Bevan, 2008). However, apoptosis does not always result in tolerance, as it seems to be the case of lymphocyte apoptosis.…”

Section: Immunotherapy Involving Trail Receptor Agonists In Non-camentioning

confidence: 99%

Therapeutic applications of TRAIL receptor agonists in cancer and beyond

Amarante-Mendes

Griffith

2015

Pharmacology & Therapeutics

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TRAIL/Apo-2L is a member of the TNF superfamily first described as an apoptosis-inducing cytokine in 1995. Similar to TNF and Fas ligand, TRAIL induces apoptosis in caspase-dependent manner following TRAIL death receptor trimerization. Because tumor cells were shown to be particularly sensitive to this cytokine while normal cells/tissues proved to be resistant along with being able to synthesize and release TRAIL, it was rapidly appreciated that TRAIL likely served as one of our major physiologic weapons against cancer. In line with this, a number of research laboratories and pharmaceutical companies have attempted to exploit the ability of TRAIL to kill cancer cells by developing recombinant forms of TRAIL or TRAIL receptor agonists (e.g., receptor-specific mAb) for therapeutic purposes. In this review article we will describe the biochemical pathways used by TRAIL to induce different cell death programs. We will also summarize the clinical trials related to this pathway and discuss possible novel uses of TRAIL-related therapies. In recent years, the physiological importance of TRAIL has expanded beyond being a tumoricidal molecule to one critical for a number of clinical settings — ranging from infectious disease and autoimmunity to cardiovascular anomalies. We will also highlight some of these conditions where modulation of the TRAIL/TRAIL receptor system may be targeted in the future.

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“…204 It will be interesting to determine whether CD8 + T cells primarily express TRAIL within the intracellular inflammatory milieu of an HCV-infected liver and whether TRAIL blockade can restore T-cell function and reverse hepatotoxicity. 205 …”

Section: Pathogenesis Of Accelerated Liver Disease In Patients With Hmentioning

confidence: 99%

Coinfection With HIV-1 and HCV—A One-Two Punch

2009

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Hepatitis C virus (HCV) infection is a major cause of chronic liver disease, cirrhosis, and death; it is estimated that 180 million persons are infected with HCV worldwide. The consequences of HCV are worse in those who are coinfected with human immunodeficiency virus 1 (HIV-1), which is unfortunately a common scenario because of shared risk factors of the viruses. More studies into effects of HCV/HIV-1 coinfection are needed, but efforts have been hampered by limitations in our understanding of the combined pathogenesis of the 2 viruses. Gaining insight into the mechanisms that underlie the immunopathogenesis of these persistent viral infections could lead to new therapeutic strategies for patients with HCV/HIV-1 coinfection.

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The TRAIL of Helpless CD8⁺T Cells in HIV Infection

Cited by 14 publications

References 49 publications

Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Therapeutic applications of TRAIL receptor agonists in cancer and beyond

Coinfection With HIV-1 and HCV—A One-Two Punch

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The TRAIL of Helpless CD8+T Cells in HIV Infection

Cited by 14 publications

References 49 publications

Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Signaling through the P38 and ERK pathways: a common link between HIV replication and the immune response

Therapeutic applications of TRAIL receptor agonists in cancer and beyond

Coinfection With HIV-1 and HCV—A One-Two Punch

Contact Info

Product

Resources

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The TRAIL of Helpless CD8⁺T Cells in HIV Infection