Treg-Therapy Allows Mixed Chimerism and Transplantation Tolerance Without Cytoreductive Conditioning

Pilat, Nina; Baranyi, Ulrike; Klaus, Christoph; Jaeckel, Elmar; Mpofu, Nonsikelelo; Wrba, Fritz; Golshayan, Déla; Muehlbacher, Ferdinand; Wekerle, Thomas

doi:10.1111/j.1600-6143.2010.03018.x

Cited by 125 publications

(167 citation statements)

References 51 publications

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“…Our results show that allogeneic stimulation of naive T cells in the presence of RA consistently induced the de novo differentiation of Treg cells with an unbiased homing potential, presenting effective in vivo suppressive abilities in a skin allograft model. Several protocols have been developed to generate Treg cells; some are designed to produce polyclonal Treg cells by stimulating naive T cells with anti-CD3 in anti-inflammatory conditions [55,56], while others have expanded selected thymus-derived Treg cells [29,30]. Although these Treg cells can be used to produce tolerance to a transplanted tissue, they cannot be used for cellular therapy in humans due to the lack of specificity.…”

Section: Discussionmentioning

confidence: 99%

Alloreactive regulatory T cells generated with retinoic acid prevent skin allograft rejection

et al. 2014

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CD4 + CD25 + Foxp3 + regulatory T (Treg) cells mediate immunological self-tolerance and suppress immune responses. Retinoic acid (RA), a natural metabolite of vitamin A, has been reported to enhance the differentiation of Treg cells in the presence of TGF-β. In this study, we show that the co-culture of naive T cells from C57BL/6 mice with allogeneic antigen-presenting cells (APCs) from BALB/c mice in the presence of TGF-β, RA, and IL-2 resulted in a striking enrichment of Foxp3 + T cells. These RA in vitro-induced regulatory T (RA-iTreg) cells did not secrete Th1-, Th2-, or Th17-related cytokines, showed a nonbiased homing potential, and expressed several cell surface molecules related to Treg-cell suppressive potential. Accordingly, these RA-iTreg cells suppressed T-cell proliferation and inhibited cytokine production by T cells in in vitro assays. Moreover, following adoptive transfer, RA-iTreg cells maintained Foxp3 expression and their suppressive capacity. Finally, RA-iTreg cells showed alloantigen-specific immunosuppressive capacity in a skin allograft model in immunodeficient mice. Altogether, these data indicate that functional and stable allogeneic-specific Treg cells may be generated using TGF-β, RA, and IL-2. Thus, RA-iTreg cells may have a potential use in the development of more effective cellular therapies in clinical transplantation. Keywords: Allogeneic regulatory T cells r Homing r Retinoic acid r Tolerance r TransplantationAdditional supporting information may be found in the online version of this article at the publisher's web-site IntroductionRegulatory T (Treg) cells are responsible for inducing and maintaining peripheral tolerance [1]. Treg cells are classified into two Correspondence: Dr. Daniela Sauma e-mail: dsauma@u.uchile.cl major subpopulations: thymus-derived Treg cells, which are generated in the thymus and circulate in the periphery as functional mature Treg cells [2][3][4], and peripherally derived Treg cells, which are generated in the periphery from CD4 + CD25 − naive * These authors contributed equally to this work.C 2014 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim www.eji-journal.eu Eur. J. Immunol. 2015. 45: 452-463 Immunomodulation 453T cells [5][6][7]. Treg cells target effector T cells and dendritic cells (DCs) by modulating their maturation and function through several mechanisms that suppress immune responses [8][9][10]; these include secretion of inhibitory cytokines (IL-10, IL-35, and TGF-β), granzyme/perforin-dependent mediated cytolysis, metabolic disruption [11][12][13][14][15], and the expression of LAG3 and CTLA4, which alter DC function [16,17]. In addition to the aforementioned mechanisms, Treg-cell suppressive capacity is dependent on Treg-cell migration and retention in the microenvironment where regulation is required. Differential expression patterns of chemokine receptors (such as CCR4, CCR5, and CCR9), integrins (α4β7), and selectins (CD62L) contribute to selective retention and trafficking of Treg cells and allow their appropriate localization during ...

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Section: Discussionmentioning

confidence: 99%

Alloreactive regulatory T cells generated with retinoic acid prevent skin allograft rejection

et al. 2014

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“…Skin graft (Chai et al, 2005) Foxp3 transduced expression in naïve CD4 + CD25 _ Skin graft (Banuelos et al, 2004) DST and anti-CD154 in CD4, CD8, or CD25 depleted skin and islet graft recipients Skin graft (Sanchez-Fueyo et al, 2007) Wt or Class II -mice Skin graft Mixed chimerism (Pilat et al, 2010) Rapamyacin and costimulation blockade;…”

Section: Graft or Target Authors Methods Of Inductionmentioning

confidence: 99%

Immunological Considerations for Inducing Skin Graft Tolerance

Gordon¹

2011

Skin Grafts - Indications, Applications and Current Research

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“…Recently, two methods have been reported to successfully eliminate myelosuppression from recipient conditioning. One involves the coupling of Treg-cell therapy with the mixed chimerism strategy [40]. Studies from our group established that the administration of polyclonal recipient Treg cells at the time of transplantation of a conventional dose of fully allogeneic donor BM induces multilineage mixed chimerism in murine recipients conditioned solely with a short course of costimulation blockers (CTLA4Ig, anti-CD40L) and an mTOR inhibitor (rapamycin) ( Fig.…”

Section: Noncytoreductive Conditioning Protocolsmentioning

confidence: 99%

“…Along these lines, regulation is critical in the NHP setting and in clinical trials (see below) in which permanent mixed chimerism (which is a prerequisite for maintaining continuous central deletion) is not achieved [69]. Combining Treg-cell therapy with noncytoreductive BMT actively has been shown to potentiate regulatory mechanisms [40,41]. Clonal deletion has been shown with such a Treg-cell chimerism regimen, but is less pronounced, while regulation is predominant throughout follow up.…”

Section: Regulatory Mechanismsmentioning

confidence: 99%

“…Studies from our group established that the administration of polyclonal recipient Treg cells at the time of transplantation of a conventional dose of fully allogeneic donor BM induces multilineage mixed chimerism in murine recipients conditioned solely with a short course of costimulation blockers (CTLA4Ig, anti-CD40L) and an mTOR inhibitor (rapamycin) ( Fig. 1) [40]. Relatively low chimerism levels were observed with this protocol, but transplantation of BM retrieved from chimeras into secondary BMT recipients demonstrated that HSC engraftment had been achieved in the primary BMT recipients [40].…”

Section: Noncytoreductive Conditioning Protocolsmentioning

confidence: 99%

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Deletional and regulatory mechanisms coalesce to drive transplantation tolerance through mixed chimerism

et al. 2015

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Establishing donor-specific immunological tolerance could improve long-term outcome by obviating the need for immunosuppressive drug therapy, which is currently required to control alloreactivity after organ transplantation. Mixed chimerism is defined as the engraftment of donor hematopoietic stem cells in the recipient, leading to viable coexistence of both donor and recipient leukocytes. In numerous experimental models, cotransplantation of donor bone marrow (BM) into preconditioned (e.g., through irradiation or cytotoxic drugs) recipients leads to transplantation tolerance through (mixed) chimerism. Mixed chimerism offers immunological advantages for clinical translation; pilot trials have established proof of concept by deliberately inducing tolerance in humans.Widespread clinical application is prevented, however, by the harsh preconditioning currently necessary for permitting BM engraftment. Recently, the immunological mechanisms inducing and maintaining tolerance in experimental mixed chimerism have been defined, revealing a more prominent role for regulation than historically assumed. The evidence from murine models suggests that both deletional and regulatory mechanisms are critical in promoting complete tolerance, encompassing also the minor histocompatibility antigens. Here, we review the current understanding of tolerance through mixed chimerism and provide an outlook on how to realize widespread clinical translation based on mechanistic insights gained from chimerism protocols, including cell therapy with polyclonal regulatory T cells. Keywords: Clonal deletion Mixed chimerism Nonmyeloablative conditioning Transplantation tolerance Treg cells IntroductionLong-term outcome after organ transplantation has improved little in the past few decades and remains suboptimal [1]. Grafts are still lost to immunological damage that is not prevented by current immunosuppressive drug regimens [2], which in addition cause severe adverse effects, including increased risks of malignancy and infection. Therefore, immunological tolerance -i.e., a state of specific nonresponsiveness to donor antigens -remains the "Holy Grail" in clinical organ transplantation. Among the Correspondence: Dr. Thomas Wekerle e-mail: Thomas.Wekerle@meduniwien.ac.at numerous strategies that have been tested over time, chimerismbased tolerance induction appears particularly promising [3,4]. This concept is based on the cotransplantation of donor hematopoietic stem cells (HSCs) (contained in bone marrow (BM) or mobilized peripheral blood stem cells (mPBSCs)) into the organ transplant recipient who has been sufficiently preconditioned, either with radiation or cytotoxic drugs, to permit HSC engraftment. If engraftment is achieved, multilineage chimerism ensues, which is termed "mixed" chimerism if donor representation is clearly detectable (by flow cytometry, for instance) but is less than 100% (which would constitute "full" chimerism) and can be achieved with less extensive recipient conditioning.In 1945 Ray Owen described a naturally occur...

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Treg-Therapy Allows Mixed Chimerism and Transplantation Tolerance Without Cytoreductive Conditioning

Cited by 125 publications

References 51 publications

Alloreactive regulatory T cells generated with retinoic acid prevent skin allograft rejection

Alloreactive regulatory T cells generated with retinoic acid prevent skin allograft rejection

Immunological Considerations for Inducing Skin Graft Tolerance

Deletional and regulatory mechanisms coalesce to drive transplantation tolerance through mixed chimerism

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