In vivo Treg expansion under costimulation blockade targets early rejection and improves long-term outcome

Schwarz, Christoph; Mahr, Benedikt; Muckenhuber, Moritz; Weijler, Anna Marianne; Unger, Lukas; Pilat, Nina; Latus, Michaela; Regele, Heinz; Wekerle, Thomas

doi:10.1111/ajt.16724

Cited by 12 publications

(18 citation statements)

References 30 publications

(64 reference statements)

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“…Next, we aimed at increasing Treg numbers through IL-2 complexes (IL-2 cplxs). Thereby, we could successfully increase the number of regulatory T cells but also showed a synergistic effect of IL-2 cplxs and CTLA4Ig in reducing the expression of B7 molecules on dendritic cells (34).…”

Section: Figurementioning

confidence: 89%

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Costimulation blockade and Tregs in solid organ transplantation

2022

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Regulatory T cells (Tregs) play a critical role in maintaining self-tolerance and in containing allo-immune responses in the context of transplantation. Recent advances yielded the approval of the first pharmaceutical costimulation blockers (abatacept and belatacept), with more of them in the pipeline. These costimulation blockers inhibit effector cells with high clinical efficacy to control disease activity, but might inadvertently also affect Tregs. Treg homeostasis is controlled by a complex network of costimulatory and coinhibitory signals, including CD28, the main target of abatacept/belatacept, and CTLA4, PD-1 and ICOS. This review shall give an overview on what effects the therapeutic manipulation of costimulation has on Treg function in transplantation.

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Section: Figurementioning

confidence: 89%

“…In addition to PD-1, Tregs also upregulated ICOS and CTLA4 upon stimulation with IL-2 complexes (52). Together with CTLA4Ig these in vivo expanded Tregs facilitated long-term survival of fully mismatched cardiac allografts in mice (34).…”

Section: Homeostatic Control Of Tregsmentioning

confidence: 94%

Costimulation blockade and Tregs in solid organ transplantation

2022

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“…Our findings highlight again the potency of dual costimulation blockade, but also the need for further investigation of the mechanisms behind the “partial efficacy” and observed costimulation blockade resistant rejection. In this context, regulatory T-cells (Tregs) represent an attractive therapeutic target as their in-vivo expansion with IL-2 complexes (that allow for a more targeted delivery of IL-2 to Tregs than conventional IL-2) successfully prevented rejection under CTLA4-Ig in murine cardiac transplantation ( 32 ). The biggest advantage of combined costimulatory pathway blockade including CD40-CD40L is certainly the superior control over humoral allo-immunity, as CD40-CD40L is the main signaling pathway responsible for B cell activation and immunoglobulin class switch ( 33 ).…”

Section: Discussionmentioning

confidence: 99%

Chronic CD40L blockade is required for long-term cardiac allograft survival with a clinically relevant CTLA4-Ig dosing regimen

et al. 2022

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IntroductionIn de-novo kidney transplantation, the CTLA4-Ig fusion protein belatacept is associated with improved graft function but also an increased risk of acute rejection compared to calcineurin inhibitor therapy. The combination with a second costimulation blocker could potentially improve outcome while avoiding calcineurin inhibitor toxicity. The aim of this study was to define the conditions under which the combination of CTLA4-Ig and CD40L blockade leads to rejection-free permanent graft survival in a stringent murine heart transplantation model.MethodsNaïve wild-type or CD40L (CD154) knock-out mice received a fully mismatched BALB/c cardiac allograft. Selected induction and maintenance protocols for CTLA4-Ig and blocking αCD40L monoclonal antibodies (mAB) were investigated. Graft survival, rejection severity and donor-specific antibody (DSA) formation were assessed during a 100-day follow-up period.Results and DiscussionAdministering αCD40L mAb as monotherapy at the time of transplantation significantly prolonged heart allograft survival but did not further improve the outcome when given in addition to chronic CTLA4-Ig therapy (which prolongs graft survival to a median of 22 days). Likewise, chronic αCD40L mAb therapy (0.5mg) combined with perioperative CTLA4-Ig led to rejection in a proportion of mice and extensive histological damage, despite abrogating DSA formation. Only the permanent interruption of CD40-CD40L signaling by using CD40L-/- recipient mice or by chronic αCD40L administration synergized with chronic CTLA4-Ig to achieve long-term allograft survival with preserved histological graft integrity in all recipients without DSA formation. The combination of α-CD40L and CTLA4-Ig works most effectively when both therapeutics are administered chronically.

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“…CTLA4‐Ig impairs Treg generation and survival through inhibition of signaling via CD28 and has been shown to abrogate Treg‐dependent graft acceptance in animal models 153,154 . Conversely, in vivo Treg expansion using IL‐2 prior to transplant reversed CTLA‐Ig‐mediated decline on Tregs and prolonged allograft survival 155 . Finally, treatment of IL‐6‐deficient mice with CTLA4‐Ig resulted in graft infiltration with Tregs and prolonged graft acceptance, 156 suggesting that IL‐6 inhibition can synergize with costimulation blockade, and potentially mitigate the early risk of acute T cell‐mediated rejection associated with belatacept‐based immunosuppression.…”

Section: Impact Of Il‐6 Inhibition On Tregsmentioning

confidence: 99%

“…153,154 Conversely, in vivo Treg expansion using IL-2 prior to transplant reversed CTLA-Ig-mediated decline on Tregs and prolonged allograft survival. 155 Finally, treatment of IL-6-deficient mice with CTLA4-Ig resulted in graft infiltration with Tregs and prolonged graft acceptance, 156 suggesting that IL-6 inhibition can synergize with costimulation blockade, and potentially mitigate the early risk of acute T cell-mediated rejection associated with belatacept-based immunosuppression. This strategy is currently being tested in a pilot trial of living donor kidney transplant recipients who receive tocilizumab for 6 months, in combination with lulizumab for the first 3 months and belatacept for the next 3 months, following which patients are maintained on belatacept in combination with everolimus and prednisone (NCT04066114).…”

Section: Impac T Of Il-6 Inhib Iti On On Treg Smentioning

confidence: 99%

Impact of interleukin-6 on T cells in kidney transplant recipients

Chandran

Tang

2022

American Journal of Transplantation

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Interleukin-6 (IL-6), a multifunctional proinflammatory cytokine, plays a key role in T cell activation, survival, and differentiation. Acting as a switch that induces the differentiation of naïve T cells into Th17 cells and inhibits their development into regulatory T cells, IL-6 promotes rejection and abrogates tolerance. Therapies that target IL-6 signaling include antibodies to IL-6 and the IL-6 receptor and inhibitors of janus kinases; several of these therapeutics have demonstrated robust clinical efficacy in autoimmune and inflammatory diseases. Clinical trials of IL-6 inhibition in kidney transplantation have focused primarily on its effects on B cells, plasma cells, and HLA antibodies. In this review, we summarize the impact of IL-6 on T cells in experimental models of transplant and describe the effects of IL-6 inhibition on the T cell compartment in kidney transplant recipients.

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In vivo Treg expansion under costimulation blockade targets early rejection and improves long-term outcome

Abstract: This is an open access article under the terms of the Creat ive Commo ns Attri bution License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

Cited by 12 publications

References 30 publications

Costimulation blockade and Tregs in solid organ transplantation

Costimulation blockade and Tregs in solid organ transplantation

Chronic CD40L blockade is required for long-term cardiac allograft survival with a clinically relevant CTLA4-Ig dosing regimen

Impact of interleukin-6 on T cells in kidney transplant recipients

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