TCR-Independent Activation of Extrathymically Developed, Self Antigen-Specific T Cells by IL-2/IL-15

Yamada, Hisakata; Nakamura, Takahiko; Matsuzaki, Goro; Iwamoto, Yukihide; Nomoto, Kikuo

doi:10.4049/jimmunol.164.4.1746

Cited by 16 publications

(27 citation statements)

References 39 publications

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“…Previous studies had shown that the expansion of self-specific CD8 T cells in response to either IL-2 or IL-15 in vitro was independent of self-Ag interactions (32). Our studies have suggested that self-Ag interactions played a role in the proliferation of self-specific CD8 T cells in vivo during LM infection (26).…”

Section: Self-ag Interactions Are Crucial For Maintaining the Memory supporting

confidence: 63%

“…Previous reports have shown that self-specific CD8 T cells can proliferate and become activated in vitro in response to IL-2 or IL-15 (32). The expression of IL-2R␤ (CD122) in conjunction with common ␥ chain (CD132) is sufficient to confer lymphocytes with the ability to respond to both IL-2 and IL-15 (33,34).…”

Section: Il-15-activated Cells Provide Protection Against Lm Infectionmentioning

confidence: 99%

See 1 more Smart Citation

Self-Antigen Maintains the Innate Antibacterial Function of Self-Specific CD8 T Cells In Vivo

Dhanji

Chow

Teh

2006

The Journal of Immunology

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Self-specific CD8 T cells, which are selected by high-affinity interactions with self-Ags, develop into a lineage distinct from conventional CD8 T cells. We have previously shown that these self-specific cells acquire phenotypic and functional similarities to cells of the innate immune system including the expression of functional receptors associated with NK cells. In this study, we show that these self-specific cells have the ability to produce large amounts of IFN-γ in response to infection with Listeria monocytogenes in a bystander fashion. The rapid production of IFN-γ is associated with a dramatic reduction in the number of viable bacteria at the peak of infection. Self-specific CD8 T cells provide only marginal innate protection in the absence of self-Ag; however, the presence of self-Ag dramatically increases their protective ability. Exposure to self-Ag is necessary for the maintenance of the memory phenotype and responsiveness to inflammatory cytokines such as IL-15. Significantly, self-specific CD8 T cells are also more efficient in the production of IFN-γ and TNF-α, thus providing more cytokine-dependent protection against bacterial infection when compared with NK cells. These findings illustrate that self-reactive CD8 T cells can play an important innate function in the early defense against bacterial infection.

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Section: Self-ag Interactions Are Crucial For Maintaining the Memory supporting

confidence: 63%

Section: Il-15-activated Cells Provide Protection Against Lm Infectionmentioning

confidence: 99%

Self-Antigen Maintains the Innate Antibacterial Function of Self-Specific CD8 T Cells In Vivo

Dhanji

Chow

Teh

2006

The Journal of Immunology

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“…However, memory phenotype CD4 cells are also found in naive mice maintained under germfree conditions, suggesting that their development is not foreign Ag dependent (51). Because T cells from male anti-H-Y TCR-transgenic mice can develop extrathymically and display memory markers, it is possible that the development of memory phenotype CD8 T cells in naive mice is driven by the interaction of the ␣␤TCR with self-Ags and developed extrathymically (13,18,19). However, our finding that only a small percentage of CD8␣␤ cells develop in Txbm DKO mice compared with thymusintact bm chimeras suggests that most non-class Ia-selected CD8␣␤ cells are from the thymus-dependent pathway.…”

Section: Discussionmentioning

confidence: 99%

“…IL-2-activated CD8CD44 high cells are able to kill syngeneic tumor cells, suggesting that they may play a role in the surveillance of host cells that have been altered through infection or transformation (17). By analogy with H-Y Ag-specific TCR-transgenic mice, it has been suggested that the development of a significant portion of memory phenotype CD8 T cells in naive wild-type mice is driven by the interaction of ␣␤TCR with self-Ags and occurs extrathymically (13,18,19 (20). In the thymus of DKO mice, most mature single-positive CD8␣␤ T cells are CD44 low , similar to those in B6 mice (21).…”

Section: Thymus-dependent Memory Phenotype Cd8 T Cells Inmentioning

confidence: 99%

Thymus-Dependent Memory Phenotype CD8 T Cells in Naive B6.H-2Kb−/−Db−/− Animals Mediate an Antigen-Specific Response against Listeria monocytogenes

Berg

Murray

et al. 2005

The Journal of Immunology

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B6.H-2Kb−/−Db−/− (DKO) mice have greatly reduced numbers of mature CD8αβ T cells in their periphery. However, these non-class Ia-selected CD8αβ T cells are able to mediate immune responses to a number of pathogens. Approximately 60% of the CD8αβ T cells in the spleen and peripheral lymph nodes of naive DKO mice display a memory (CD44high) phenotype. To investigate the origins of these non-class Ia-selected CD8αβCD44high cells, we traced the phenotype of recent thymic emigrants and found that most were CD44low. We also determined whether their appearance was thymus dependent and found that only a small percentage of non-class Ia-selected CD8αβCD44high cells develop in a thymus-independent pathway. Functionally, CD8αβCD44high cells from DKO mice are able to secrete IFN-γ in response to IL-12 and IL-18 in the absence of cognate Ag. When challenged with anti-CD3 in vivo, nearly half of these cells produce IFN-γ within 3 h. When purified CD8αβCD44high cells from Thy1.2.DKO mice were transferred into Thy1.1 DKO recipients and then challenged with Listeria monocytogenes, an Ag-specific anti-L. monocytogenes response was observed 6 days later. Our data suggest that non-class Ia-selected CD8αβCD44high cells in naive animals can respond rapidly to Ag and play a role in the innate as well as the early phase of the acquired immune response.

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“…Another unusual feature of these CD8 lo T cells is that they proliferate in response to cytokines such as IL-2 and IL-15 in an antigen-independent manner. 9 However, the CD8 lo cells are similar to conventional memory T cells with regard to the ability to rapidly produce interferon ␥ (IFN-␥) upon TCR stimulation 10 and in respect to the killing of susceptible target cells without the need for additional reactivation with antigen. 11,12 CD8 ϩ T cells that develop via an extrathymic pathway and possessing similar functional characteristics are also found in normal (non-TCR transgenic) mice.…”

Section: Introductionmentioning

confidence: 99%

Self-reactive memory-phenotype CD8 T cells exhibit both MHC-restricted and non-MHC-restricted cytotoxicity: a role for the T-cell receptor and natural killer cell receptors

Dhanji

Teh

Oble

et al. 2004

Blood

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TCR-Independent Activation of Extrathymically Developed, Self Antigen-Specific T Cells by IL-2/IL-15

Cited by 16 publications

References 39 publications

Self-Antigen Maintains the Innate Antibacterial Function of Self-Specific CD8 T Cells In Vivo

Self-Antigen Maintains the Innate Antibacterial Function of Self-Specific CD8 T Cells In Vivo

Thymus-Dependent Memory Phenotype CD8 T Cells in Naive B6.H-2Kb−/−Db−/− Animals Mediate an Antigen-Specific Response against Listeria monocytogenes

Self-reactive memory-phenotype CD8 T cells exhibit both MHC-restricted and non-MHC-restricted cytotoxicity: a role for the T-cell receptor and natural killer cell receptors

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