Effector differentiation is not prerequisite for generation of memory cytotoxic T lymphocytes

Manjunath, N.; Shankar, Premlata; Wan, Junmei; Weninger, Wolfgang; Crowley, Maura; Hieshima, Kunio; Springer, Timothy A.; Fan, Xueli; Shen, Hao; Lieberman, Judy; Andrian, U.H. von

doi:10.1172/jci13296

Cited by 361 publications

(381 citation statements)

References 45 publications

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“…2C). These data are well in line with previous reports that exposure of antigenstimulated P14 or pmel-1 T cells to IL-2 or IL-15 generates effector or central memory-like CD8 T cells, respectively [6,[8][9][10]12]. We also noted that P14 IL-2 and P14 IL-15 cells differed in functional CD95L/Fas ligand expression since co-culture of P14 IL-2 cells and L1210 target cells expressing CD95/Fas resulted in antigen-independent cell killing whereas co-culture of the same target cells and P14 IL-15 cells had no effect (Fig.…”

Section: Resultssupporting

confidence: 93%

“…Phenotype and functional activity of P14 IL-2 and P14 IL-15 cells P14 IL-2 and P14 IL-15 cells were generated in vitro using the protocol originally described by Manjunath et al [6]. Briefly, CD8 T cells from P14 TCR-tg mice specific for the LCMV gp33 epitope were stimulated with gp33 peptide for 2 days to induce lymphoblasts.…”

Section: Resultsmentioning

confidence: 99%

“…Besides IL-2, IL-15 also supports CD8 T-cell growth [5]; however, the phenotype and the functional activity of IL-2-versus IL-15-cultured CD8 T cells differ considerably. Manjunath et al [6] were the first to show that CD8 T cells from P14 TCR-tg mice specific for gp33 epitope of lymphocytic choriomeningitis virus (LCMV) acquired an effector memory phenotype with high cytolytic activity when cultured in the presence of IL-2 whereas addition of IL-15 led to a central memory phenotype with low effector cell functions. Further analysis in the same TCR transgenic system revealed that these two cytokines were equivalent mitogens for antigen-stimulated CD8 T cells but that IL-2 was more potent in inducing amino acid uptake and protein synthesis [7].…”

Section: Introductionmentioning

confidence: 99%

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Efficacy of IL‐2‐ versus IL‐15‐stimulated CD8 T cells in adoptive immunotherapy

2008

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We determined the efficacy of in vitro expanded P14 TCR transgenic CD8 T cells to mediate tumor cell elimination and to protect against viral infection in mice. Contrary to previous studies, an adoptive transfer model without lymphodepletion, vaccination or cytokine treatment was used. Antigen-activated P14 T cells cultured in IL-2-containing medium for 7 days (P14 IL-2 ) exhibited potent effector cell functions in vitro but did not confer protection against melanoma growth or viral infection. In contrast, P14 T cells cultured in IL-15 (P14 ) were highly effective in vivo although they displayed only moderate effector functions in vitro. Therapeutic efficacy correlated with the survival of the transferred T cells in the recipients: P14 IL-2 cells disappeared rapidly whereas P14 IL-15 cells persisted for prolonged time. Decreasing the IL-2 concentration in the culture media improved in vivo survival and efficacy but also lowered the cell yield of the cultures. Finally, we could extend the findings with monoclonal P14 T cells to polyclonal CD8 T cells. Thus, in vitro expansion of antigen-specific CD8 T cells in IL-15 allowed the generation of substantial numbers of T cells without inducing terminally differentiated effector cells that turned out to be unfavorable in the transfer model examined here.Key words: Cytotoxic T cells . Rodent . Tumor immunity . Viral IntroductionAdoptive transfer of antigen-specific CD8 T cells into hosts represents a promising approach to treat tumors and viral infections [1][2][3][4]. To generate sufficient numbers of T cells for this therapy, T cells have to be stimulated and expanded in vitro. In most protocols used today, IL-2 is added to the culture medium to ensure T-cell proliferation, differentiation and survival. Besides IL-2, IL-15 also supports CD8 T-cell growth [5]; however, the phenotype and the functional activity of IL-2-versus IL-15-cultured CD8 T cells differ considerably. Manjunath et al. [6] were the first to show that CD8 T cells from P14 TCR-tg mice specific for gp33 epitope of lymphocytic choriomeningitis virus (LCMV) acquired an effector memory phenotype with high cytolytic activity when cultured in the presence of IL-2 whereas addition of IL-15 led to a central memory phenotype with low effector cell functions. Further analysis in the same TCR transgenic system revealed that these two cytokines were equivalent mitogens for antigen-stimulated CD8 T cells but that IL-2 was more potent in inducing amino acid uptake and protein synthesis [7].For adoptive T-cell therapy, it is important to generate CD8 T cells in vitro, which are efficient in inducing tumor regression or virus clearance in vivo. The degree of specific target cell lysis and the amount of antigen-triggered IFN-g production are frequently used to predict the efficacy of CD8 T cells in vivo. However, several recent studies in the pmel-1 TCR-tg model specific for the self/tumor antigen gp100 of B16 melanoma cells indicated that antigen-stimulated CD8 T cells with a less differentiated phenotype were sup...

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Section: Resultssupporting

confidence: 93%

Section: Resultsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Efficacy of IL‐2‐ versus IL‐15‐stimulated CD8 T cells in adoptive immunotherapy

2008

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“…Although the pattern of lineage differentiation of T cell functional subsets is still a matter of debate, evidence from others has confirmed the ability of CCR7 expression to discriminate populations with different functional properties. [23][24][25] In this study we have analyzed the effect of polyclonal expansion and subsequent transduction on the function of primary human T-lymphocytes, and then explored the underlying mechanisms. Our results show that PHA can lead to an impairment of the immune competence of these cells in vitro, as determined by allogeneic and viral antigen-specific responses.…”

Section: Pha and Cd3/cd28 On The Distribution Of Ccr7/cd45ra T Cell Fmentioning

confidence: 99%

“…Nevertheless, this does not imply that CD8 + T EM cells would not provide long-term immune responses, and we and others have shown that expression of CCR7 can be up-regulated by CD8 + T EM cells in some circumstances, a process that depends on the stimulus and the cytokine environment. [23][24][25]39 Further analysis of these rel-evant aspects is not possible from the design of our in vitro study.…”

Section: Cells Subsets Are Designated As T N (Naive) T CM (Central Mmentioning

confidence: 99%

Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

et al. 2002

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T cell priming by dendritic cells: thresholds for proliferation, differentiation and death and intraclonal functional diversification

Langenkamp¹,

et al. 2002

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The variables that influence priming of human naive CD4+ T cells by dendritic cells (DC) were dissected in vitro by analyzing the response to the bacterial superantigen toxicshock syndrome toxin or to alloantigens. We show that under conditions that force DC‐T cell interactions a single DC can prime up to 20 naive T cells. Moreover, the strength of antigenic stimulation, as determined by DC numbers, antigen dose, TCR avidity and duration of DC‐T cell interactions, drives the progressive differentiation of proliferating T cells from a non‐effector CCR7+ stage, to an effector CCR7– stage and, eventually, to cell death. We also show that the proliferating CCR7+ and CCR7– populations share clonotypic sequences, demonstrating that the two cell fates can be generated within a single clone. Taken together these results indicate that the strength of antigenic stimulation regulates T cell progression through thresholds of proliferation, differentiation and death. However, the random nature of DC‐T cell encounters introduces a critical stochastic element in T cell stimulation, which leads to the generation of cells endowed with distinct homing potentials and effector functions within a given T cell clone.

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Effector differentiation is not prerequisite for generation of memory cytotoxic T lymphocytes

Cited by 361 publications

References 45 publications

Efficacy of IL‐2‐ versus IL‐15‐stimulated CD8 T cells in adoptive immunotherapy

Efficacy of IL‐2‐ versus IL‐15‐stimulated CD8 T cells in adoptive immunotherapy

Functional impairment of human T-lymphocytes following PHA-induced expansion and retroviral transduction: implications for gene therapy

T cell priming by dendritic cells: thresholds for proliferation, differentiation and death and intraclonal functional diversification

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