Influence of T Cell Coinhibitory Molecules on CD8+ Recall Responses

Morris, Anna B.; Adams, Layne E.; Ford, Mandy L.

doi:10.3389/fimmu.2018.01810

Cited by 18 publications

(16 citation statements)

References 58 publications

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“…In this respect we investigated expression of different ICRs by skin CD8 1 Trm cells. 22 We noticed that these cells expressed high levels of PD-1, 23 TIM-3, 24 or 2B4 (Fig 3, B), 25 as well as CD5, 26 but not T cell immunoreceptor with Ig and ITIM domains (TI-GIT), 27 Of note, the number of DNFB-specific IFN-g-producing T cells among CD8 1 PD-1 1 Trm cells was 2 times higher compared with that in their PD-1 2 counterparts, as revealed by using an ELISpot assay at day 30 The following day, the number of specific T cells was determined by using an IFN-g ELISpot assay. Results are expressed as mean 6 SEM numbers of spot-forming cells/10 6 CD8 1 T cells.…”

Section: Epidermal Cd8 1 Trm Cells Express a Restricted Set Of Icrsmentioning

confidence: 80%

Inhibitory checkpoint receptors control CD8+ resident memory T cells to prevent skin allergy

Gamradt

Laoubi

Nosbaum

et al. 2019

Journal of Allergy and Clinical Immunology

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Background: Tissue-resident memory T (Trm) cells are detrimental in patients with numerous chronic inflammatory diseases, including allergic contact dermatitis (ACD).Objectives: We sought to analyze the contribution of Trm cells to the chronicity and severity of ACD and to define the local parameters regulating their development and functions. Methods: We used an experimental model of ACD (ie, contact hypersensitivity to 2,4-dinitrofluorobenzene) that is mediated by CD8 1 T cells. Results: Our data show that early effector T cells accumulated in the skin during the acute contact hypersensitivity reaction and gave rise to epidermal CD8 1 Trm cells expressing a specific set of inhibitory checkpoint receptors (ICRs), such as programmed cell death protein 1 (PD-1) and T cell immunoglobulin and mucin domain 3 (TIM-3). Those Trm cells remained in the epidermis for several weeks and mediated the eczema exacerbations, which developed on allergen re-exposure without the contribution of circulating specific T cells. Furthermore, allergen-induced Trm cell reactivation was constrained because treatment with ICR antagonists dramatically enhanced the magnitude and severity of eczema exacerbations. Finally, we show that the persistence of the

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Section: Epidermal Cd8 1 Trm Cells Express a Restricted Set Of Icrsmentioning

confidence: 80%

Inhibitory checkpoint receptors control CD8+ resident memory T cells to prevent skin allergy

Gamradt

Laoubi

Nosbaum

et al. 2019

Journal of Allergy and Clinical Immunology

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“…Moreover, addition of CD244 to wild-type NK cells inhibited cell toxicity and IFN production, and the same inhibitory effect occurred in memory CD8 + T cells. In chronic infections, CD244 limited the recall response of CD8 + T cells by inhibiting their proliferation and function ( 37 ). The reason for these different results may be that CD244 binds to multiple protein receptors that transmit different intracellular signals.…”

Section: Molecular Characteristics Of Cd244mentioning

confidence: 99%

Advances in Understanding the Roles of CD244 (SLAMF4) in Immune Regulation and Associated Diseases

Sun

Gang

et al. 2021

Front. Immunol.

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Proteins in the signaling lymphocytic activating molecule (SLAM) family play crucial roles in regulating the immune system. CD244 (SLAMF4) is a protein in this family, and is also a member of the CD2 subset of the immunoglobulin (Ig) superfamily. CD244 is a cell surface protein expressed by NK cells, T cells, monocytes, eosinophils, myeloid-derived suppressor cells, and dendritic cells. CD244 binds to the ligand CD48 on adjacent cells and transmits stimulatory or inhibitory signals that regulate immune function. In-depth studies reported that CD244 functions in many immune-related diseases, such as autoimmune diseases, infectious diseases, and cancers, and its action is essential for the onset and progression of these diseases. The discovery of these essential roles of CD244 suggests it has potential as a prognostic indicator or therapeutic target. This review describes the molecular structure and function of CD244 and its roles in various immune cells and immune-related diseases.

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“…In contrast to the wealth of information detailing the roles of multiple TCR-independent determinants in shaping I o pathogen-specific CD8 + T E responses, considerably less information is available about the regulation of II o CD8 + T E immunity [72, 73]. Moreover, the notion of long-term CD8 + T cell memory as a progressively evolving trait has gained increasing traction over the past half decade and implies the potential remodeling of relevant recall response determinants; to date, however, their identities and possible contributions to altered II o CD8 + T E reactivity remain largely unknown.…”

Section: Discussionmentioning

confidence: 99%

Aging boosts antiviral CD8+T cell memory through improved engagement of diversified recall response determinants

et al. 2019

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The determinants of protective CD8+ memory T cell (CD8+TM) immunity remain incompletely defined and may in fact constitute an evolving agency as aging CD8+TM progressively acquire enhanced rather than impaired recall capacities. Here, we show that old as compared to young antiviral CD8+TM more effectively harness disparate molecular processes (cytokine signaling, trafficking, effector functions, and co-stimulation/inhibition) that in concert confer greater secondary reactivity. The relative reliance on these pathways is contingent on the nature of the secondary challenge (greater for chronic than acute viral infections) and over time, aging CD8+TM re-establish a dependence on the same accessory signals required for effective priming of naïve CD8+T cells in the first place. Thus, our findings reveal a temporal regulation of complementary recall response determinants that is consistent with the recently proposed “rebound model” according to which aging CD8+TM properties are gradually aligned with those of naïve CD8+T cells; our identification of a broadly diversified collection of immunomodulatory targets may further provide a foundation for the potential therapeutic “tuning” of CD8+TM immunity.

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Influence of T Cell Coinhibitory Molecules on CD8+ Recall Responses

Cited by 18 publications

References 58 publications

Inhibitory checkpoint receptors control CD8+ resident memory T cells to prevent skin allergy

Inhibitory checkpoint receptors control CD8+ resident memory T cells to prevent skin allergy

Advances in Understanding the Roles of CD244 (SLAMF4) in Immune Regulation and Associated Diseases

Aging boosts antiviral CD8+T cell memory through improved engagement of diversified recall response determinants

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