Naive T Cells Are Resistant to Anergy Induction by Anti-CD3 Antibodies

Andris, Fabienne; Denanglaire, Sébastien; Mattia, Fabrizio De; Urbain, Jacques; Léo, Oberdan

doi:10.4049/jimmunol.173.5.3201

Cited by 24 publications

(14 citation statements)

References 48 publications

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“…This was examined in Th1 clones, which represents the classical cellular model of T cell anergy (27–29). Anergy was induced using immobilized anti-CD3 mAb, as we and others have reported previously (12, 30).…”

Section: Resultsmentioning

confidence: 99%

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Locke

Zha

Zheng

et al. 2013

The Journal of Immunology

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PTEN is thought to play a critical role in T cell activation by negatively regulating the PI3K signaling pathway important for cellular activation, growth, and proliferation. To directly eliminate PTEN in post-thymic T cells for studies of functional effects, we utilized CAR Tg x PTENflox/flox mice which enabled gene deletion using a Cre adenovirus in vitro. These mice were also immunized to generate stable Th1 clones that could have PTEN deleted when desired. PTEN-deleted T cells exhibited enhanced IL-2 production, proliferation, and Akt phosphorylation upon TCR/CD28 engagement, whereas T cell survival was not potentiated. Gene expression profiling revealed a small subset of induced genes that were augmented upon PTEN deletion. However, PTEN-deficient T cells still required CD28 costimulation for IL-2 production and remained susceptible to anti-CD3-induced anergy. The absence of PTEN within the CD8 T cell compartment led to markedly increased cytolytic activity following an allogeneic MLR in vitro, without increasing autologous MLR activity. Our results indicate that deletion of PTEN can augment the activation of post-thymic T cells but does not mediate CD28-independence or anergy resistance. Nonetheless, PTEN inhibition may be a viable target for immune potentiation due to increased cytokine production by activated CD4+ cells, and increased cytotoxicity by CD8+ T cells.

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Section: Resultsmentioning

confidence: 99%

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Locke

Zha

Zheng

et al. 2013

The Journal of Immunology

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“…Conflicting reports indicate that under some circumstances memory CD4 1 T cells are resistant to tolerance induction [20,21], whereas under others, effector CD4 1 T cells appear susceptible [22,23]. In contrast to this, in vitro observations indicate that memory or post-activated CD4 1 T cells are more sensitive than naïve CD4 1 T cells to anergy induction in vitro by fixed APC or agents such as ionomycin and anti-CD3 mAb [24][25][26]. We now demonstrate that CD4 1 effector/memory T-cell responses can be also terminated by cognate antigen-expressing DC.…”

mentioning

confidence: 99%

“…Alternatively, the different findings could implicate induction of different molecular pathways for induction of peripheral tolerance in CD4 1 T cells by different APC types. For instance, induction of anergy, or adaptive tolerance, requires induction of many calcium-induced regulatory proteins and pathways such as E3 ubiquitin ligases [34,35] which may be readily induced following Ca 11 mobilization in vitro (or in vivo) by the agents listed above [24][25][26] or by transient antigen presentation in vivo. In contrast, deletion, which requires induction of apoptotic pathways [36], may occur only with the sustained antigen signalling that occurs when antigen is transgenically expressed.…”

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confidence: 99%

Steady‐state antigen‐expressing dendritic cells terminate CD4⁺ memory T‐cell responses

et al. 2010

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CD4 1 T cells are important effectors of inflammation and tissue destruction in many diseases of immune dysregulation. As memory T cells develop early during the preclinical stages of autoimmune and inflammatory diseases, immunotherapeutic approaches to treatment of these diseases, once established, must include the means to terminate memory T-cell responses. Traditionally, it has been considered that, due to their terminally differentiated nature, memory T cells are resistant to tolerance induction, although emerging evidence indicates that some immunotherapeutic approaches can terminate memory T-cell responses. Here, we demonstrate that CD4 1 memory T-cell responses can be terminated when cognate antigen is transgenically expressed in steady-state DC. Transfer of in-vitrogenerated CD4 1 memory T cells establishes, in nontransgenic recipients, a stable and readily recalled memory response to cognate antigen. In contrast, upon transfer to mice expressing cognate antigen targeted to DC, memory CD4 1 T cells undergo a phase of limited proliferation followed by substantial deletion, and recall responses are effectively silenced. This finding is important in understanding how to effectively apply immunotherapy to ongoing T-cell-mediated autoimmune and inflammatory diseases.Key words: CD4 1 T cells . DC . Tolerance See accompanying Commentary by Kurts IntroductionNegative selection and peripheral tolerance mechanisms jointly serve to limit the development of autoaggressive self-reactive T-cell responses. However, in autoimmune-prone individuals these control mechanisms can fail and autoimmune disease ensues. As autoimmune diseases progress, intra-and intermolecular determinant spreading occurs [1] and populations of effector and memory T cells become established. Therefore, unlike strategies directed at preventing the development of autoimmune disease, where induction of tolerance in naïve T cells may be all that is required, therapies aimed at terminating ongoing autoimmune disease must be capable of inactivating established populations of memory or activated effector T cells.Although naïve T cells are highly dependent on the presence or absence of costimulatory signals to determine the outcome of activation, costimulation appears to play little role in controlling the responses of memory and effector T cells [2,3] and these cells are considered costimulation independent. Because of this, in contrast to naïve T cells which are readily deleted or inactivated in the absence of costimulation memory T cells are widely regarded as potentially resistant to tolerance induction. If this were indeed the case, then effector and memory T cells represent a significant hurdle to therapeutic strategies aimed at treating autoimmune diseases. However, we have recently shown that memory and effector CD8 1 T cells are susceptible to tolerance induction when cognate antigen is expressed in DC and other APC types [4]. 2016The relative roles of CD4 1 and CD8 1 T cells in disease progression differ depending on the autoimmune disease bu...

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“…Both lymphoproliferation and IFN-gamma production in response to recall antigens remain unchanged in the PBMC of splenectomized patients [14]. ''Memory'' cells also respond well to stimulation with anti-CD3 antibodies [34]. With regard to this, normal responses to anti-CD3 stimulation of PBMC from the CA patients (proliferation, IFN-gamma, TNF-alfa, and IL-6 production) may suggest that the functional status of memory cells remains normal in the CA patients, at least concerning certain parameters studied here.…”

Section: Discussionmentioning

confidence: 99%

Peripheral blood T lymphocyte subsets in children with congenital asplenia

et al. 2012

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Naive T Cells Are Resistant to Anergy Induction by Anti-CD3 Antibodies

Cited by 24 publications

References 48 publications

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Steady‐state antigen‐expressing dendritic cells terminate CD4⁺ memory T‐cell responses

Peripheral blood T lymphocyte subsets in children with congenital asplenia

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Naive T Cells Are Resistant to Anergy Induction by Anti-CD3 Antibodies

Cited by 24 publications

References 48 publications

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Conditional Deletion of PTEN in Peripheral T Cells Augments TCR-Mediated Activation but Does Not Abrogate CD28 Dependency or Prevent Anergy Induction

Steady‐state antigen‐expressing dendritic cells terminate CD4+ memory T‐cell responses

Peripheral blood T lymphocyte subsets in children with congenital asplenia

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Steady‐state antigen‐expressing dendritic cells terminate CD4⁺ memory T‐cell responses