Altered balance between effector T cells and FOXP3<sup>+</sup>HELIOS<sup>+</sup>regulatory T cells after thymoglobulin induction in kidney transplant recipients

Tang, Qizhi; Leung, Joey; Melli, Kristin; Lay, Kimberly; Chuu, Emmeline L.; Liu, Weihong; Bluestone, Jeffrey A.; Kang, ⋅Sang-Mo; Peddi, V. Ram; Vincenti, Flavio

doi:10.1111/j.1432-2277.2012.01565.x

Cited by 41 publications

(36 citation statements)

References 37 publications

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“…This is in line with earlier studies showing that anti-CD3 mAbs may induce Helios expression in Tregs, and that the Helios + Tregs produce less IFN-γ and IL2 [27]. Interestingly, it has been shown in kidney transplant recipients receiving ATG at the time of transplantation that depletion of CD4 + Helios + Foxp3 + T cells was less pronounced compared to CD4 + Foxp3 - T cells [28]. In kidney transplant patients, Bouvy et al found [29] an increase of the percentages of Tregs 6 months following ATG treatment in comparison with Basiliximab (anti-CD25 antibody) therapy.…”

Section: Discussionsupporting

confidence: 89%

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

et al. 2017

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Thymoglobulin (ATG) is a polyclonal rabbit antibody against human thymocytes used as a T cell-depleting agent to prevent or treat allotransplant rejection. The aim of the present study was to investigate the effect of low dose ATG treatment exclusively on T cells using a humanized BALB/c human CD3Ɛ transgenic mouse model expressing both human and murine T cell receptors (TCR). Mice received a single intravenous (i.v.) injection of ATG. Blood and peripheral lymphoid organs were obtained after different time points. We found a significant T cell depletion in this mouse model. In addition, regulatory T cells (Tregs) proved to be less sensitive to depletion than the rest of T cells and the Treg:non-Treg ratio was therefore increased. Finally, we also investigated the effect of ATG in a heterotopic allogenic murine model of heart transplantation. Survival and transplant function were significantly prolonged in ATG-treated mice. In conclusion, we showed (a) an immunosuppressive effect of ATG in this humanized mouse model which is exclusively mediated by reactivity against human CD3Ɛ; (b) provided evidence for a relative resistance of Tregs against this regimen; and (c) demonstrated the immunomodulatory effect of ATG under these experimental circumstances by prolongation of heart allograft survival.

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Section: Discussionsupporting

confidence: 89%

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

et al. 2017

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“…ATG induction therapy in vivo reduces the absolute number of Treg, but less than that for Tconvs, favorably altering the Treg/Tconv ratio 29,32,33 . Furthermore, Treg recover faster during immune reconstitution following ATG treatment, contributing to the sustained elevation of Treg/Tconv ratio 34 .…”

Section: Impact Of Approved Immunosuppressive Drugs On Tregmentioning

confidence: 99%

Impact of Immune-Modulatory Drugs on Regulatory T Cell

2016

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Immunosuppression strategies that selectively inhibit effector T cells while preserving and even enhancing CD4+FOXP3+ regulatory T cells (Treg) permit immune self-regulation and may allow minimization of immunosuppression and associated toxicities. Many immunosuppressive drugs were developed before the identity and function of Treg were appreciated. A good understanding of the interactions between Treg and immunosuppressive agents will be valuable to the effective design of more tolerable immunosuppression regimens. This review will discuss preclinical and clinical evidence regarding the influence of current and emerging immunosuppressive drugs on Treg homeostasis, stability, and function as a guideline for the selection and development of Treg-friendly immunosuppressive regimens.

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“…Elkord et al observed that there was an increased frequency of Helios + Tregs in the peripheral blood of patients with renal cell carcinoma, particularly after IL2 treatment (27). Another study revealed that there was a selective preservation of the Helios + Tregs in kidney transplant recipients that received thymoglobulin induction and a reduction in control patients (28). Similarly, others have noted an expansion of Helios + Tregs in patients with active systemic lupus erythematosus (29).…”

Section: Phenotypic Markersmentioning

confidence: 99%

Peripheral and Thymic Foxp3+ Regulatory T Cells in Search of Origin, Distinction, and Function

et al. 2013

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Over the past decade, much has been learnt and much more to discover about Foxp3+ regulatory T cells (Tregs). Initially, it was thought that Tregs were a unique entity that originates in the thymus. It is now recognized that there is a fraternal twin sibling that is generated in the periphery. The difficulty is in the distinction between these two subsets. The ability to detect, monitor, and analyze these two subsets in health and disease will provide invaluable insights into their functions and purposes. The plasticity and mechanisms of action can be unique and not overlapping within these subsets. Therefore, the therapeutic targeting of a particular subset of Tregs might be more efficacious. In the past couple of years, a vast amount of data have provided a better understanding of the cellular and molecular components essential for their development and stability. Many studies are implicating their preferential involvement in certain diseases and immunologic tolerance. However, it remains controversial as to whether any phenotypic markers have been identified that can differentiate thymic versus peripheral Tregs. This review will address the validity and controversy regarding Helios, Lap/Garp and Neuropilin-1 as markers of thymic Tregs. It also will discuss updated information on distinguishing features of these two subsets and their critical roles in maternal-fetal tolerance and transplantation.

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Altered balance between effector T cells and FOXP3⁺HELIOS⁺regulatory T cells after thymoglobulin induction in kidney transplant recipients

Cited by 41 publications

References 37 publications

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

Impact of Immune-Modulatory Drugs on Regulatory T Cell

Peripheral and Thymic Foxp3+ Regulatory T Cells in Search of Origin, Distinction, and Function

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Altered balance between effector T cells and FOXP3+HELIOS+regulatory T cells after thymoglobulin induction in kidney transplant recipients

Cited by 41 publications

References 37 publications

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

Differential depletion of total T cells and regulatory T cells and prolonged allotransplant survival in CD3Ɛ humanized mice treated with polyclonal anti human thymocyte globulin

Impact of Immune-Modulatory Drugs on Regulatory T Cell

Peripheral and Thymic Foxp3+ Regulatory T Cells in Search of Origin, Distinction, and Function

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Altered balance between effector T cells and FOXP3⁺HELIOS⁺regulatory T cells after thymoglobulin induction in kidney transplant recipients