Brief Antigenic Stimulation Generates Effector CD8 T Cells with Low Cytotoxic Activity and High IL-2 Production

Usharauli, David; Kamala, Tirumalai

doi:10.4049/jimmunol.180.7.4507

Cited by 6 publications

(5 citation statements)

References 41 publications

(40 reference statements)

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“…However, it is known that virus-specific CD8 T cells down-regulate CD27 during latent MCMV infection (24, 66), and we found that the expression of this surface marker was further reduced in IL-10 −/− mice. One possible functional consequence of CD27 down-regulation in this study was reduced IL-2 production in response to antigen stimulation; this is consistent with previous studies linking cellular differentiation to the loss of IL-2 expression (67, 68) and suggests a role for CD4 T cell help in the maintenance of polyfunctional memory CD8 T cells (69). Furthermore, highly differentiated CD8 T cells express high levels of granzyme and perforin (66, 70, 71) thereby suggesting that these cells are cytotoxic.…”

Section: Discussionsupporting

confidence: 92%

IL-10 Restricts Memory T Cell Inflation during Cytomegalovirus Infection

Jones

Ladell

Wynn

et al. 2010

The Journal of Immunology

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Section: Discussionsupporting

confidence: 92%

IL-10 Restricts Memory T Cell Inflation during Cytomegalovirus Infection

Jones

Ladell

Wynn

et al. 2010

The Journal of Immunology

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“…43,44 Studies evaluating the influence of antigen signaling duration rather than DC maturation state have demonstrated that CD8 ϩ T cells receiving a brief antigenic stimulus similarly acquire a central memory phenotype and produce significantly more IL2 compared with T cells receiving prolonged antigen stimulation, which developed cytotoxic activity and a reduced ability to produce IL2. 45 This reduced differentiation of primed T cells is in agreement with a progressive differentiation model in which differences in costimulation or cytokines provided in the local milieu result in varying signal strength provided to individual naive T cells, promoting a response composed of a spectrum of T cells that have acquired different amounts of effector functions and differentiation. 46 Our results suggest that the enhanced number of CD8 ϩ T cells acquiring limited effector functions and retaining CD28 generated by priming with LPS/R848-matured DCs may result from T cells primed in the presence of the incompletely mature subpopulations of DCs that provide a reduced signal for expansion, resulting in a reduced differentiation of T cells.…”

Section: Tlr-enhanced Generation Of Cd28mentioning

confidence: 52%

Priming CD8+ T cells with dendritic cells matured using TLR4 and TLR7/8 ligands together enhances generation of CD8+ T cells retaining CD28

Pufnock¹,

Cigal²,

Rolczynski³

et al. 2011

Blood

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“…Umbilical cord cells are known to produce high amounts of IL‐2, in both CD4+ and CD8+ T cell subsets (21), and constitutive production in CD4+ T cells may decrease over time as culture substrate is depleted. Brief antigen stimulation also results in increased IL‐2 production in CD8+ T cells without concurrent increase in cytotoxic activity (22). It is possible that introduction of antigen through delivery, sample collection or processing could provide enough stimulus to increase background IL‐2 production of CD8+ T cells in a the given period of time; this effect may be more evident in umbilical cord samples which produce high amounts of IL‐2 at baseline.…”

Section: Discussionmentioning

confidence: 99%

Stability of T cell phenotype and functional assays following heparinized umbilical cord blood collection

et al. 2012

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Umbilical cord blood has been used for a wide variety of immunologic investigations including assessments of developmental perturbations by antenatal exposures. Recent advances in multiparameter flow cytometry have allowed finer characterization of lymphocyte phenotype and function, revealing important differences between the fetal and adult immune systems. The degree of variability between human subjects confounds the ability to draw firm conclusions. Artifacts resulting from processing techniques exacerbate this variability. The unpredictable nature of deliveries, especially of premature infants, makes it difficult to control variables such as timing of umbilical cord mononuclear cell (UCMC) isolation and method of collection. Additionally, in multicenter studies dependent on central processing, delays are inevitable. However, little available literature describes systematic testing of the degree to which processing variations affect UCMC phenotype and function. Using multiparameter flow cytometry, we tested the effect of collection technique and length of time prior to UCMC isolation on T cell phenotype and function, with the goal of creating a standardized operating procedure for a multicenter investigation. The study also provides a benchmark data set including extensive surface and functional phenotyping of umbilical cord T cells. UCMC isolation delay of up to 24 h produced similar T cell phenotype and function as tested by in vitro SEB stimulation. There were few statistically significant differences between time points based on data medians. We conclude that, for the purpose of immunologic investigations, a 24-h time delay from sample collection to mononuclear cell isolation does not introduce a significant degree of variation in T cell phenotype and function when adhering to strict standard operating procedures.

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Brief Antigenic Stimulation Generates Effector CD8 T Cells with Low Cytotoxic Activity and High IL-2 Production

Cited by 6 publications

References 41 publications

IL-10 Restricts Memory T Cell Inflation during Cytomegalovirus Infection

IL-10 Restricts Memory T Cell Inflation during Cytomegalovirus Infection

Priming CD8+ T cells with dendritic cells matured using TLR4 and TLR7/8 ligands together enhances generation of CD8+ T cells retaining CD28

Stability of T cell phenotype and functional assays following heparinized umbilical cord blood collection

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