Direct Expansion of Human Allospecific FoxP3+CD4+ Regulatory T Cells with Allogeneic B Cells for Therapeutic Application

Chen, Leo C.; Delgado, Julio; Jensen, Peter E.; Chen, Xinjian

doi:10.4049/jimmunol.0901081

Cited by 66 publications

(57 citation statements)

References 66 publications

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“…To isolate Foxp3 + GFP + cells, CD4 + T cells were first isolated from splenocytes of Foxp3EGFP mice (32) by negative selection using a CD4 T Cell Isolation Kit (Miltenyi Biotec), followed by sorting of GFP + cells by FACS (33). All of the isolated cells were rested in culture or treated with cyclosporine A (CsA) for 30 min before being processed for protein extracts.…”

Section: Cd25mentioning

confidence: 99%

Constitutive Nuclear Localization of NFAT in Foxp3+ Regulatory T Cells Independent of Calcineurin Activity

Shakya

Guo

et al. 2012

The Journal of Immunology

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Foxp3 plays an essential role in conferring suppressive functionality to CD4+/Foxp3+ regulatory T cells (Tregs). Although studies showed that Foxp3 has to form cooperative complexes with NFAT to bind to target genes, it remains unclear whether NFAT is available in the nucleus of primary Tregs for Foxp3 access. It is generally believed that NFAT in resting cells resides in the cytoplasm, and its nuclear translocation depends on calcineurin (CN) activation. We report that a fraction of NFAT protein constitutively localizes in the nucleus of primary Tregs, where it selectively binds to Foxp3 target genes. Treating Tregs with CN inhibitor does not induce export of NFAT from the nucleus, indicating that its nuclear translocation is independent of CN activity. Consistently, Tregs are resistant to CN inhibitors in the presence of IL-2 and continue to proliferate in response to anti-CD3 stimulation, whereas proliferation of non-Tregs is abrogated by CN inhibitors. In addition, PMA, which activates other transcription factors required for T cell activation but not NFAT, selectively induces Treg proliferation in the absence of ionomycin. TCR interaction with self-MHC class II is not required for PMA-induced Treg proliferation. Tregs expanded by PMA or in the presence of CN inhibitors maintain Treg phenotype and functionality. These findings shed light on Treg biology, paving the way for strategies to selectively activate Tregs.

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Section: Cd25mentioning

confidence: 99%

Constitutive Nuclear Localization of NFAT in Foxp3+ Regulatory T Cells Independent of Calcineurin Activity

Shakya

Guo

et al. 2012

The Journal of Immunology

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“…For example, coculturing of CD19 1 human B cells with CD4 1 CD25 1 alloreactive T cells in the presence of IL-2 and CD28-specific antibody (Ab) was reported to induce a 40-fold expansion of Treg. 12,13 The current hypothesis is that B cells exert dual and potentially opposing effects on T-cell responses. On the one hand, they can promote primary T-cell responses and the generation of memory T helper (Th)1 and Th2 cells through antigen-dependent but Ab-independent mechanisms.…”

Section: Introductionmentioning

confidence: 99%

Adenosine production by human B cells and B cell–mediated suppression of activated T cells

Saze

Schuler

Hong

et al. 2013

Blood

207

212

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However, in vitro-activated B cells downregulated CD73 expression, mainly produced 59-AMP, and inhibited T-cell proliferation and cytokine production. These B cells acquire the ability to restrict potentially harmful effects of activated T cells. Thus, B cells emerge as a key regulatory component of T cell-B cell interactions, and their dual regulatory activity is mediated by the products of ATP hydrolysis, 59-AMP, and ADO. (Blood. 2013;122(1):9-18)

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“…Allogeneic mature moDC-expanded nTregs are superior in suppressing alloantigen-induced proliferation by effector T cells compared with polyclonal Tregs. This is most likely the result of a skewing in the TCR repertoire imposed by application of an Ag-specific expansion protocol (10,20). This superior alloantigenspecific suppressive capacity, induced by applying an allogeneic stimulus during Treg expansion, was confirmed by several in vitro (18) and in vivo (9,26,66) studies.…”

Section: Discussionmentioning

confidence: 88%

“…This finding may also explain the observation that a simultaneous influx of both Ag-specific effector T cells and Tregs is observed after s.c. purified protein derivate injection (69). Expansion of alloantigen-specific Tregs through stimulation with other cell types like PBMCs (18,19) and B cells (10,20) has been documented previously. Our results with PBMCs as allogeneic stimulator cells for nTreg expansion are in line with previous publications, and relatively high stimulator/Treg ratios in combination with IL-2 and IL-15 are needed.…”

Section: Discussionmentioning

confidence: 90%

“…Addition of rapamycin to this cell culture is used to diminish outgrowth of the contaminating effector T cells (16,17). Alloantigen-specific Tregs with a much greater specificity can be generated by expansion in the presence of allogeneic PBMCs (18,19) or B cells (10,20). The potential benefit of these alloantigen-specific Tregs is targeted suppression rather than general immunosuppression and increased suppressive potency (9,(21)(22)(23)(24)(25)(26).…”

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confidence: 99%

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Allogeneic Mature Human Dendritic Cells Generate Superior Alloreactive Regulatory T Cells in the Presence of IL-15

Litjens

Boer

Zuijderwijk

et al. 2015

The Journal of Immunology

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Expansion of Ag-specific naturally occurring regulatory T cells (nTregs) is required to obtain sufficient numbers of cells for cellular immunotherapy. In this study, different allogeneic stimuli were studied for their capacity to generate functional alloantigen-specific nTregs. A highly enriched nTreg fraction (CD4+CD25brightCD127− T cells) was alloantigen-specific expanded using HLA-mismatched immature, mature monocyte-derived dendritic cells (moDCs), or PBMCs. The allogeneic mature moDC-expanded nTregs were fully characterized by analysis of the demethylation status within the Treg-specific demethylation region of the FOXP3 gene and the expression of both protein and mRNA of FOXP3, HELIOS, CTLA4, and cytokines. In addition, the Ag-specific suppressive capacity of these expanded nTregs was tested. Allogeneic mature moDCs and skin-derived DCs were superior in inducing nTreg expansion compared with immature moDCs or PBMCs in an HLA-DR– and CD80/CD86-dependent way. Remarkably, the presence of exogenous IL-15 without IL-2 could facilitate optimal mature moDC-induced nTreg expansion. Allogeneic mature moDC-expanded nTregs were at low ratios (<1:320), potent suppressors of alloantigen-induced proliferation without significant suppression of completely HLA-mismatched, Ag-induced proliferation. Mature moDC-expanded nTregs were highly demethylated at the Treg-specific demethylation region within the FOXP3 gene and highly expressed of FOXP3, HELIOS, and CTLA4. A minority of the expanded nTregs produced IL-10, IL-2, IFN-γ, and TNF-α, but few IL-17–producing nTregs were found. Next-generation sequencing of mRNA of moDC-expanded nTregs revealed a strong induction of Treg-associated mRNAs. Human allogeneic mature moDCs are highly efficient stimulator cells, in the presence of exogenous IL-15, for expansion of stable alloantigen-specific nTregs with superior suppressive function.

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Direct Expansion of Human Allospecific FoxP3+CD4+ Regulatory T Cells with Allogeneic B Cells for Therapeutic Application

Cited by 66 publications

References 66 publications

Constitutive Nuclear Localization of NFAT in Foxp3+ Regulatory T Cells Independent of Calcineurin Activity

Constitutive Nuclear Localization of NFAT in Foxp3+ Regulatory T Cells Independent of Calcineurin Activity

Adenosine production by human B cells and B cell–mediated suppression of activated T cells

Allogeneic Mature Human Dendritic Cells Generate Superior Alloreactive Regulatory T Cells in the Presence of IL-15

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