Only the CD45RA+ subpopulation of CD4+CD25high T cells gives rise to homogeneous regulatory T-cell lines upon in vitro expansion

Hoffmann, Petra; Eder, Ruediger; Boeld, Tina J.; Doser, Kristina; Piseshka, Biserka; Andreesen, Reinhard; Edinger, Matthias

doi:10.1182/blood-2006-06-027409

Cited by 374 publications

(364 citation statements)

References 65 publications

(80 reference statements)

Supporting

Mentioning

337

Contrasting

Order By: Relevance

“…This happened although reproducibly more than 90% of the sorted cells expressed FOXP3 on the day of isolation ( [16] and H. and M. E. unpublished data). Possible explanations for the observed heterogeneity could be either contamination of the starting population with CD25 1 , non-regulatory Tconv that preferentially expand in culture over time, or, alternatively, the presence of a substantial number of ''converted'' or ''induced'' Treg that only transiently express FOXP3 after recent in vivo activation [22,23] and that re-convert to effector T cells during in vitro culture.…”

Section: Discussionmentioning

confidence: 92%

“…We previously showed that the heterogeneity in FOXP3 expression observed after prolonged in vitro expansion of bulk CD4 1 CD25 high T cells was predominantly caused by the emergence of FOXP3 À cells in the CD45RA À subfraction of the initial cell population [16]. Because at that time we had not included CD127 in our sorting strategy, we could not formally rule out contamination of the starting population with activated Tconv cells (which would be expected to reside primarily among CD45RA À memory cells).…”

Section: Epigenetic Changes In the Foxp3 Gene Locus Upon In Vitro Expmentioning

confidence: 99%

“…We previously demonstrated that these CD45RA 1 CD4 1 CD25 high T cells (RA 1 Treg) homogeneously maintain their Treg cell phenotype and function upon in vitro expansion, whereas CD4 1 T cells selected solely for CD25 high expression were highly variable with respect to FOXP3 expression (50.5 to 72.8% FOXP3 1 cells) after long-term culture [16]. Based on these findings, we proposed that the selection of CD45RA 1 naïve Treg is the best strategy for the generation of homogeneous Treg cell products for future clinical trials.…”

Section: Introductionmentioning

confidence: 99%

“…3). Thus, epigenetic DNA modifications in the FOXP3 gene locus indicate that CD127 À Treg partially lose their lineage-specific signature during in vitro expansion, whereas this is not the case for RA 1 Treg isolated from the same donors.Heterogeneity of CD127 À Treg cultures is caused by CD45RA À Treg in the starting populationWe previously showed that the heterogeneity in FOXP3 expression observed after prolonged in vitro expansion of bulk CD4 1 CD25 high T cells was predominantly caused by the emergence of FOXP3 À cells in the CD45RA À subfraction of the initial cell population [16]. Because at that time we had not included CD127 in our sorting strategy, we could not formally rule out contamination of the starting population with activated Tconv cells (which would be expected to reside primarily among CD45RA À memory cells).…”

mentioning

confidence: 99%

“…For this purpose, RA 1 and CD127 À Treg were isolated from the same leukapheresis products by high-speed flow cytometric cell sorting (FACS). Both cell populations showed 498% purity with regard to the applied sort gates: RA 1 Treg were isolated according to their particular expression levels of CD25 (expression level above that of CD4 À PBMC) and CD45RA (only CD45RA high cells), as described previously [16] and detailed in Fig. 1A Fig.…”

mentioning

confidence: 99%

See 4 more Smart Citations

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation

et al. 2009

Self Cite

View full text Add to dashboard Cite

The adoptive transfer of CD4 1 CD25 1 natural regulatory T cells (Treg) is a promising strategy for the treatment of autoimmune diseases and the prevention of alloresponses after transplantation. Clinical trials exploring this strategy require efficient in vitro expansion of this rare cell population. Protocols developed thus far rely on high-grade purification of Treg prior to culture initiation, a process still hampered by the lack of Treg cell-specific surface markers. Depletion of CD127 1 cells was shown to separate activated conventional T cells from natural Treg cell populations allowing the isolation of highly enriched FOXP3 1 cells with all functional and molecular characteristics of natural Treg. Here, we demonstrate that upon in vitro expansion, CpG methylation in a conserved region within the FOXP3 gene locus increased in CD4 1 CD25 1 CD127 low Treg, correlating with loss of FOXP3 expression and emergence of pro-inflammatory cytokines. Further analysis identified CD45RA À FOXP3 1 memory-type Treg as the main source of converting cells, whereas CD45RA 1 FOXP3 1 Treg from the same donors showed no conversion within 3 wk of in vitro expansion. Thus, Treg cell lineage differentiation does not seem to represent a final fate decision, as natural Treg can lose their cell-type-specific characteristics after repetitive TCR stimulation.Key words: Cellular therapy . Immune regulation . Treg Supporting Information available online Introduction CD4 1 CD25 1 Treg are pivotal for the maintenance of peripheral self-tolerance and imbalances in this T-cell compartment have been shown to contribute to various autoimmune diseases [1]. In murine disease models, adoptively transferred Treg prevent, and in some cases, even cure autoimmunity [2,3]. In addition, they protect from graft rejection after allogeneic organ transplantation [4] as well as from graft-versus-host disease after MHCmismatched stem cell transplantation [5][6][7][8]. Recently, a limited number of Phase I clinical trials exploring the adoptive transfer of Treg have been initiated and several additional trials in various clinical settings are in preparation [9,10]. Prerequisites for the initiation of such trials are (i) the availability of efficient in vitro expansion protocols for this rare cell population and (ii) the ability to unequivocally identify Treg to avoid contamination of 1088Treg cultures with potentially harmful conventional effector T cells (Tconv). While efficient cell culture protocols have recently been established by us and others for the polyclonal as well as antigen-specific Treg cell expansion [11][12][13], the search for an exclusive surface marker for Treg is still ongoing.Contrary to earlier reports, human CD4 1 CD25 high Treg in adult peripheral blood have recently been shown to comprise not only (self-)antigen-experienced, CD45RA À central and effector memory cells, but also a subpopulation of CD45RA 1 naïve recent thymic emigrants [14,15]. We previously demonstrated that these CD45RA 1 CD4 1 CD25 high T cells (RA 1 Treg) homogen...

show abstract

Section: Discussionmentioning

confidence: 92%

Section: Epigenetic Changes In the Foxp3 Gene Locus Upon In Vitro Expmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

See 3 more Smart Citations

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation

et al. 2009

Self Cite

View full text Add to dashboard Cite

show abstract

Immune Regulation in Hematopoietic Cell Transplantation

Negrin¹,

Ritz²

2015

Thomas’ Hematopoietic Cell Transplantation

View full text Add to dashboard Cite

BATF is Required for Treg Homeostasis and Stability to Prevent Autoimmune Pathology

Khatun,

Wu,

et al. 2023

Advanced Science

View full text Add to dashboard Cite

Regulatory T (Treg) cells are inevitable to prevent deleterious immune responses to self and commensal microorganisms. Treg function requires continuous expression of the transcription factor (TF) FOXP3 and is divided into two major subsets: resting (rTregs) and activated (aTregs). Continuous T cell receptor (TCR) signaling plays a vital role in the differentiation of aTregs from their resting state, and in their immune homeostasis. The process by which Tregs differentiate, adapt tissue specificity, and maintain stable phenotypic expression at the transcriptional level is still inconclusivei. In this work, the role of BATF is investigated, which is induced in response to TCR stimulation in naïve T cells and during aTreg differentiation. Mice lacking BATF in Tregs developed multiorgan autoimmune pathology. As a transcriptional regulator, BATF is required for Treg differentiation, homeostasis, and stabilization of FOXP3 expression in different lymphoid and non‐lymphoid tissues. Epigenetically, BATF showed direct regulation of Treg‐specific genes involved in differentiation, maturation, and tissue accumulation. Most importantly, FOXP3 expression and Treg stability require continuous BATF expression in Tregs, as it regulates demethylation and accessibility of the CNS2 region of the Foxp3 locus. Considering its role in Treg stability, BATF should be considered an important therapeutic target in autoimmune disease.

show abstract

Only the CD45RA+ subpopulation of CD4+CD25high T cells gives rise to homogeneous regulatory T-cell lines upon in vitro expansion

Cited by 374 publications

References 65 publications

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation

Immune Regulation in Hematopoietic Cell Transplantation

BATF is Required for Treg Homeostasis and Stability to Prevent Autoimmune Pathology

Contact Info

Product

Resources

About

Only the CD45RA+ subpopulation of CD4+CD25high T cells gives rise to homogeneous regulatory T-cell lines upon in vitro expansion

Cited by 374 publications

References 65 publications

Loss of FOXP3 expression in natural human CD4+CD25+ regulatory T cells upon repetitive in vitro stimulation

Loss of FOXP3 expression in natural human CD4+CD25+ regulatory T cells upon repetitive in vitro stimulation

Immune Regulation in Hematopoietic Cell Transplantation

BATF is Required for Treg Homeostasis and Stability to Prevent Autoimmune Pathology

Contact Info

Product

Resources

About

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation

Loss of FOXP3 expression in natural human CD4⁺CD25⁺ regulatory T cells upon repetitive in vitro stimulation