Bcl-2 Allows Effector and Memory CD8+ T Cells To Tolerate Higher Expression of Bim

Kurtuluş, Sema; Tripathi, Pulak; Moreno‐Fernandez, Maria E.; Sholl, Allyson; Katz, Jonathan D.; Grimes, H. Leighton; Hildeman, David A.

doi:10.4049/jimmunol.1100102

Cited by 90 publications

(128 citation statements)

References 43 publications

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“…34 Such IL-15 limitation likely enhances Puma expression in KLRG1 hi CD127 lo cells relative to KLRG1 lo CD127 hi cells as the latter cells can utilize both IL-7 and IL-15 for survival. 33 Further, we confirm and extend prior results, showing that Puma has a preferential effect on contraction of KLRG1 hi CD127 lo cells. 15 Thus, in the absence of Bim, the enormous numbers of KLRG1 hi CD127 lo cells act as a sink for IL-15 and likely other nutrients (glucose, amino acids) that prevent engagement of other BH3-only proteins.…”

Section: Discussionsupporting

confidence: 89%

“…1,32-34 IL-15 is critical for maintaining expression of Bcl-2, a major Bim antagonist in effector CD8 þ T cells. 33 The huge size of the anti-LCMV CD8 þ T-cell response, even in WT mice, likely limits the effector response by restricting IL-15 availability. 34 Such IL-15 limitation likely enhances Puma expression in KLRG1 hi CD127 lo cells relative to KLRG1 lo CD127 hi cells as the latter cells can utilize both IL-7 and IL-15 for survival.…”

Section: Discussionmentioning

confidence: 99%

“…Second, the absence of Bim may protect KLRG1 lo CD127 hi cells from death as many of these cells die in WT mice. 1,14,33 KLRG1 lo CD127 hi cells are more protected from death because they express increased levels of Bcl-2, as genetic loss or pharmacologic inhibition of Bcl-2 enhanced their Bimdriven death. 33,43 Further, we have shown that a common g chain cytokine/STAT5/Bcl-2 network acts downstream of IL-7 and IL-15 to protect KLRG1 lo CD127 hi effector T cells from Bim and likely Puma, favoring memory cell development.…”

Section: Discussionmentioning

confidence: 99%

“…1,14,33 KLRG1 lo CD127 hi cells are more protected from death because they express increased levels of Bcl-2, as genetic loss or pharmacologic inhibition of Bcl-2 enhanced their Bimdriven death. 33,43 Further, we have shown that a common g chain cytokine/STAT5/Bcl-2 network acts downstream of IL-7 and IL-15 to protect KLRG1 lo CD127 hi effector T cells from Bim and likely Puma, favoring memory cell development. 34 Third, as mentioned above, the massive expansion of effector and pre-memory subsets in Bim À / À mice severely restricts IL-15 availability for KLRG1 hi CD127 lo cells.…”

Section: Discussionmentioning

confidence: 99%

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Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Kurtuluş

Sholl

et al. 2014

Cell Death Differ

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During the effector CD8 þ T-cell response, transcriptional differentiation programs are engaged that promote effector T cells with varying memory potential. Although these differentiation programs have been used to explain which cells die as effectors and which cells survive and become memory cells, it is unclear if the lack of cell death enhances memory. Here, we investigated effector CD8 þ T-cell fate in mice whose death program has been largely disabled because of the loss of Bim. Interestingly, the absence of Bim resulted in a significant enhancement of effector CD8 þ T cells with more memory potential. Bim-driven control of memory T-cell development required T-cell-specific, but not dendritic cell-specific, expression of Bim. Both total and T-cell-specific loss of Bim promoted skewing toward memory precursors, by enhancing the survival of memory precursors, and limiting the availability of IL-15. Decreased IL-15 availability in Bim-deficient mice facilitated the elimination of cells with less memory potential via the additional pro-apoptotic molecules Noxa and Puma. Combined, these data show that Bim controls memory development by limiting the survival of pre-memory effector cells. Further, by preventing the consumption of IL-15, Bim limits the role of Noxa and Puma in causing the death of effector cells with less memory potential.

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Section: Discussionsupporting

confidence: 89%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 2 more Smart Citations

Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Kurtuluş

Sholl

et al. 2014

Cell Death Differ

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“…7,8 Indeed, the BH3-only molecule Bim, acting through Bax/Bak, is required for the apoptosis of most effector T cells. 2,[9][10][11][12][13] Genetic ablation of Bim prevents the loss of effector CD4 þ and CD8…”

mentioning

confidence: 99%

Mcl-1 antagonizes Bax/Bak to promote effector CD4+ and CD8+ T-cell responses

et al. 2013

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IL‐2 and IL‐15 regulate CD8⁺ memory T‐cell differentiation but are dispensable for protective recall responses

et al. 2015

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Eur. J. Immunol. 2015. 45: 3324-3338 Immunity to Infection 3325 tightly regulated process during which cells pass through an effector state before establishing long-term immune protection [1]. The recognition of pathogen-encoded peptides and their stimulation through costimulatory and cytokine signals initiate a specific transcriptional program critical for CD8 + T-cell lineage choices and functions [2,3]. As the memory T-cell pool is the direct progeny of these effectors cells, understanding the cellular and molecular mechanisms involved in the transition from cytotoxic T lymphocytes (CTLs) to memory cells constitutes an area of intense investigation.In the quest to dissect these mechanisms, two effector CD8 + T-cell populations were identified, based on their distinct expression of CD127 and KLRG1, and correlated with their propensity to persist and become memory [4][5][6]. While KLRG1 hi CD127 lo ShortLived Effector Cells (SLECs) are destined to become terminal effectors, KLRG1 lo CD127 hi Memory Precursor Effector Cells (MPECs) are fated to develop into long-lived memory cells. Since, multiple factors were shown to modulate the lineage choices between these two effector subsets. Limited antigenic stimulation preferentially commits effector CD8 + T cells toward a MPEC phenotype while prolonged antigen encounter promotes terminal SLEC differentiation [7,8]. Similarly, inflammatory cytokines (in particular IL-12) enhance SLEC generation in a T-bet-dependent manner, whereas low levels of inflammation favor memory formation [6,9]. Finally, cytokines that signal through the common gamma (γ c ) chain (IL-2, IL-4, IL-7, IL-9, IL-15, IL-21) modify the CD8 + T-cell differentiation program upon infection and are indispensable for the generation of CD8 + memory T cells [10]. While IL-7promotes MPEC and CD8 + memory T-cell survival [11], IL-2 and IL-15 cooperate to sustain SLEC proliferation, differentiation, and survival [9,10,[12][13][14][15]. IL-15 is also a pivotal cytokine involved in the maintenance and homeostatic proliferation of the CD8 + memory T-cell pool [16,17]. Interestingly, IL-21, which is critical during chronic viral infection to limit exhaustion, has a minimal role on SLEC/MPEC lineage choices and CD8 + memory T-cell formation during an acute viral infection in help-independent infection models [18]. While the role of γ c -dependent signals on CD8 + memory T-cell development is indisputable, the biological impact of IL-2 and IL-15 on CD8 + memory T-cell functions remains controversial.Studies have demonstrated a critical role for IL-2 in the regulation of Blimp-1 and Eomes transcription [9,12], two transcription factors that have an opposite effect on the development of CD8 + memory T cells [19][20][21]. Moreover, some authors suggest that IL-2 present at the time of priming sustain the expansion of secondary effectors, while others do not [9,14,22,23]. Conversely, IL-15, a γ c -cytokine closely related to IL-2, appears dispensable for secondary effector expansion, while it may affect secondary e...

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Bcl-2 Allows Effector and Memory CD8+ T Cells To Tolerate Higher Expression of Bim

Cited by 90 publications

References 43 publications

Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Mcl-1 antagonizes Bax/Bak to promote effector CD4+ and CD8+ T-cell responses

IL‐2 and IL‐15 regulate CD8⁺ memory T‐cell differentiation but are dispensable for protective recall responses

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Bcl-2 Allows Effector and Memory CD8+ T Cells To Tolerate Higher Expression of Bim

Cited by 90 publications

References 43 publications

Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Bim controls IL-15 availability and limits engagement of multiple BH3-only proteins

Mcl-1 antagonizes Bax/Bak to promote effector CD4+ and CD8+ T-cell responses

IL‐2 and IL‐15 regulate CD8+ memory T‐cell differentiation but are dispensable for protective recall responses

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IL‐2 and IL‐15 regulate CD8⁺ memory T‐cell differentiation but are dispensable for protective recall responses