Uncoupling of Proliferative Potential and Gain of Effector Function by CD8+ T Cells Responding to Self-Antigens

Hernández, Javier; Aung, Sandra; Marquardt, Kristi; Sherman, Linda A.

doi:10.1084/jem.20011612

Cited by 122 publications

(148 citation statements)

References 57 publications

(83 reference statements)

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“…3c). Therefore, the presence of HCVcore during the initial activation of memory cells (and possibly the priming of naive cells) induces a dichotomy between the expansion and the differentiation of these cells, affecting only the latter and supporting the view that expansion and differentiation of memory cells can be two dissociated events [11,12,17].…”

Section: Hcvcore Does Not Inhibit Memory Ctl Proliferationsupporting

confidence: 57%

“…The sustained antigenic stimulation in our in vitro system might, however, hide the further option that in vivo CTL priming is impaired, because circulating HCVcore may affect professional APC (i.e. DC), leading to CTL expansion, but impaired effector differentiation [8][9][10][11][12][13][14][15][16][17][42][43][44].…”

Section: Discussionmentioning

confidence: 99%

“…A successful CTL response is dependent on a wide array of stimulatory signals present during priming, such as those provided by professional APC, duration of antigenic stimulus, CD4 help, and the type of cytokines [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19]. Efficient simultaneous signals (or such compensating among themselves) are mandatory for maintaining long-term central memory CCR7 + cells proliferating even in the absence of antigen (that is, in response to homeostatic cytokines), and differentiating in full CCR7 -effector cells, upon a possible re-encounter with the antigen [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19].…”

Section: Introductionmentioning

confidence: 99%

“…Efficient simultaneous signals (or such compensating among themselves) are mandatory for maintaining long-term central memory CCR7 + cells proliferating even in the absence of antigen (that is, in response to homeostatic cytokines), and differentiating in full CCR7 -effector cells, upon a possible re-encounter with the antigen [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19]. By contrast, subthreshold signal levels may provide different scenarios ranging from anergy to a high expansion of memory cells that are devoid of effector functions [10][11][12][13][14][15][16][17][18][19][20]. The signals governing the strength of CTL activation can be deeply affected by the intervention of different mechanisms of immune subversion established by several viruses, known to interact with CTL development [21].…”

Section: Introductionmentioning

confidence: 99%

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Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Accapezzato¹,

Francavilla²,

Rawson³

et al. 2004

Eur J Immunol

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In a companion study, we showed a dichotomy between the expansion of central memory (CCR7 + ) hepatitis C virus (HCV)-specific CTL and the incomplete memory effector differentiation in patients with acute HCV infection. Indeed, effector cells were unable to perform immediate functions, despite expressing the tissue-homing phenotype of effector memory cells (CCR7 -; semi-effectors). However, since they promptly differentiated into full-effectors upon IL-2 contact, we suggested that the inhibitory effect by environmental (possibly viral) factors on IL-2 production may have a pivotal role in generating the large population of semieffector CCR7 -/IFN-+ -CTL. In accord with this view, we report here strong evidence in support of circulating HCV core protein (HCVcore) playing a central role in inhibiting effector CTL differentiation, but not memory CTL expansion. The regulatory HCVcore effect is related to inhibition of the signal transduction pathway instrumental for IL-2 production, supporting the evidence that IL-2 was capable both of pushing semi-effector CTL to complete their effector cell program and of restoring the HCVcore-dependent inhibitory effect. Therefore, the strength of CTL activation is dependent on the balance between the threshold of stimulatory signals and the viral interference capacities provided during priming.

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Section: Hcvcore Does Not Inhibit Memory Ctl Proliferationsupporting

confidence: 57%

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Accapezzato¹,

Francavilla²,

Rawson³

et al. 2004

Eur J Immunol

View full text Add to dashboard Cite

show abstract

“…Central memory cells express CCR7 and CD62L enabling homing to peripheral lymphoid tissues, where they promptly proliferate in response to antigen, generating a large expansion of effector memory cells, which in turn migrate into inflamed tissues, upon CCR7 and CD62L down-regulation [3,[6][7][8][9]. The success of a CTL priming is dependent on efficient and sustained signals such as those provided by professional APC, duration of antigenic stimulation, CD4 help, and the type of cytokine milieu [10][11][12][13][14][15][16][17][18][19]. By contrast, the lack or the defective performance of one or more of these signals may evolve into different scenarios ranging from abortive CTL divisions (tolerance) to a high expansion of memory cells that are devoid of effector functions [10][11][12][13][14][15][16][17][18][19][20].…”

Section: Introductionmentioning

confidence: 99%

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: exploring the immunological mechanisms

et al. 2004

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Hallmark of acute hepatitis C virus (HCV) infection is a severe virus-specific effector CD8 + T cell dysfunction that seems to be a critical factor in preventing the resolution of infection and in favoring the onset of chronic liver immunopathology. We suggest that this dysfunction is critical in the establishment of HCV persistence, unless it is compensated by multispecific responses, as found in individuals resolving infection. Analyses on purified populations indicate that central memory HCV-specific CCR7 + /CD8 + T cells efficiently proliferate and differentiate in vitro, although the large population of memory effector CCR7 -cells found in the peripheral blood of acutely infected patients display poor effector functions ex vivo (semieffectors). However, we report strong evidence in support of IL-2 being capable of pushing semi-effector CTL to complete their effector cell program. Therefore, IL-2 deficiency during T cell activation may be responsible for the dichotomy between memory CTL expansion and incomplete effector differentiation shown in patients with acute HCV infection. These data are consistent with the possible therapeutic treatment with IL-2 to rebuild the effector T cell pool in these patients.

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Transient gain of effector function by CD8⁺ T cells undergoing peripheral tolerance to high‐dose self‐antigen

Huang¹,

Yang²

2004

Eur J Immunol

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Induction of peripheral T cell tolerance is mediated by bone marrow-derived dendritic cells that cross-present self-antigen to self-reactive T cells. The current model for peripheral CD8 + T cell tolerance is that TCR engagement by self-antigen in the absence of costimulation results in abortive activation without development of effector function. Here we demonstrate in vivo that high-dose self-antigen ("signal 1") can compensate for lack of costimulation ("signal 2"), leading to full activation of and development of effector function by self-reactive T cells. In the setting of low-dose self-antigen, acquisition of effector function by selfreactive T cells is dependent on costimulation via CD40 ligation in vivo. However, gain of effector function in either setting does not prevent eventual tolerance of self-reactive CD8 + T cells. These results suggest that the mechanisms for peripheral CD8 + T cell tolerance are more complex than the proposed "signal 1 in the absence of signal 2" hypothesis. Further exploration of these mechanisms will have direct impact on the design of effective immunotherapy for autoimmune diseases, chronic infections and cancers.

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Uncoupling of Proliferative Potential and Gain of Effector Function by CD8+ T Cells Responding to Self-Antigens

Cited by 122 publications

References 57 publications

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: exploring the immunological mechanisms

Transient gain of effector function by CD8⁺ T cells undergoing peripheral tolerance to high‐dose self‐antigen

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Uncoupling of Proliferative Potential and Gain of Effector Function by CD8+ T Cells Responding to Self-Antigens

Cited by 122 publications

References 57 publications

Subversion of effector CD8+ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8+ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8+ T cell differentiation in acute hepatitis C virus infection: exploring the immunological mechanisms

Transient gain of effector function by CD8+ T cells undergoing peripheral tolerance to high‐dose self‐antigen

Contact Info

Product

Resources

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Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: the role of the virus

Subversion of effector CD8⁺ T cell differentiation in acute hepatitis C virus infection: exploring the immunological mechanisms

Transient gain of effector function by CD8⁺ T cells undergoing peripheral tolerance to high‐dose self‐antigen