Induced Regulatory T Cells Promote Tolerance When Stabilized by Rapamycin and IL-2 In Vivo

Zhang, Ping; Tey, Siok-Keen; Koyama, Motoko; Kuns, Rachel D.; Olver, Stuart D.; Lineburg, Katie E.; Lor, Mary; Teal, Bianca E.; Raffelt, Neil C.; Raju, Jyothy; Lévêque, Lucie; Markey, Kate A.; Varelias, Antiopi; Clouston, Andrew D.; Lane, Steven; MacDonald, Kelli P. A.; Hill, Geoffrey R.

doi:10.4049/jimmunol.1301181

Cited by 105 publications

(112 citation statements)

References 57 publications

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“…122 Treg number or function perturbations lead to the development of autoimmune diseases and are thought to contribute to aGVHD and cGVHD pathology. 8,10,123 Both preclinical and clinical studies demonstrate that donor graft Treg number inversely correlates with aGVHD, [124][125][126][127][128] and cGVHD is associated with decreased numbers of circulating Tregs. 21,[129][130][131] Factors contributing to diminished Treg numbers in cGVHD recipients remain to be fully elucidated although there are multiple candidates including diminished thymic production, reduced proliferative capacity of naive Tregs, 132 and a failure in memory Treg survival due to their increased susceptibility to apoptosis.…”

Section: Immune Regulators Of Cgvhdmentioning

confidence: 99%

Chronic graft-versus-host disease: biological insights from preclinical and clinical studies

MacDonald¹,

Hill

Blazar

2017

Blood

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219

212

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With the increasing use of mismatched, unrelated, and granulocyte colony-stimulating factor–mobilized peripheral blood stem cell donor grafts and successful treatment of older recipients, chronic graft-versus-host disease (cGVHD) has emerged as the major cause of nonrelapse mortality and morbidity. cGVHD is characterized by lichenoid changes and fibrosis that affects a multitude of tissues, compromising organ function. Beyond steroids, effective treatment options are limited. Thus, new strategies to both prevent and treat disease are urgently required. Over the last 5 years, our understanding of cGVHD pathogenesis and basic biology, born out of a combination of mouse models and correlative clinical studies, has radically improved. We now understand that cGVHD is initiated by naive T cells, differentiating predominantly within highly inflammatory T-helper 17/T-cytotoxic 17 and T-follicular helper paradigms with consequent thymic damage and impaired donor antigen presentation in the periphery. This leads to aberrant T- and B-cell activation and differentiation, which cooperate to generate antibody-secreting cells that cause the deposition of antibodies to polymorphic recipient antigens (ie, alloantibody) or nonpolymorphic antigens common to both recipient and donor (ie, autoantibody). It is now clear that alloantibody can, in concert with colony-stimulating factor 1 (CSF-1)-dependent donor macrophages, induce a transforming growth factor β–high environment locally within target tissue that results in scleroderma and bronchiolitis obliterans, diagnostic features of cGVHD. These findings have yielded a raft of potential new therapeutics, centered on naive T-cell depletion, interleukin-17/21 inhibition, kinase inhibition, regulatory T-cell restoration, and CSF-1 inhibition. This new understanding of cGVHD finally gives hope that effective therapies are imminent for this devastating transplant complication.

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Section: Immune Regulators Of Cgvhdmentioning

confidence: 99%

Chronic graft-versus-host disease: biological insights from preclinical and clinical studies

MacDonald¹,

Hill

Blazar

2017

Blood

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219

212

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“…9 These complexes preferentially bind to CD25 hi cells, which results in Treg expansion in a variety of disease models. [9][10][11] As a result, IL-2/mAb complexes may be superior to IL-2 for Treg expansion in cGVHD. Treg infusions also increase Treg numbers, and, unlike IL-2-based therapies, only a single dose may be required.…”

Section: Introductionmentioning

confidence: 99%

Therapeutic regulatory T-cell adoptive transfer ameliorates established murine chronic GVHD in a CXCR5-dependent manner

McDonald-Hyman

Flynn

Panoskaltsis‐Mortari

et al. 2016

Blood

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Key Points• IL-2/mAb complexes expand Tregs and treat established murine cGVHD, but concurrent T-effector cell expansion can reduce their therapeutic index.• Prophylactic Treg infusions can prevent cGVHD, whereas therapeutic efficacy requires homing to and inhibition of the GC reaction.Chronic graft-versus-host disease (cGVHD) is a major complication of allogeneic hematopoietic stem cell transplantation. In cGVHD, alloreactive T cells and germinal center (GC) B cells often participate in GC reactions to produce pathogenic antibodies. Although regulatory T cells (Tregs) can inhibit GC reactions, Treg numbers are reduced in cGVHD, contributing to cGVHD pathogenesis. Here, we explored 2 means to increase Tregs in cGVHD: interleukin-2/monoclonal antibody (IL-2/mAb) complexes and donor Treg infusions. IL-2/mAb complexes given over 1 month were efficacious in expanding Tregs and treating established cGVHD in a multi-organ-system disease mouse model characterized by GC reactions, antibody deposition, and lung dysfunction. In an acute GVHD (aGVHD) model, IL-2/mAb complexes given for only 4 days resulted in rapid mortality, indicating IL-2/mAb complexes can drive conventional T-cell (Tcon)-mediated injury. In contrast, Treg infusions, which uniformly suppress aGVHD, increased Treg frequency and were effective in preventing the onset of, and treating, established cGVHD. Efficacy was dependent upon CXCR5-sufficient Tregs homing to, and inhibiting, GC reactions. These studies indicate that the infusion of Tregs, especially ones enriched for GC homing, may be desirable for cGVHD therapy. Although IL-2/mAb complexes can be efficacious in cGVHD, a cautious approach needs to be taken in settings in which aGVHD elements, and associated Tcon, are present. (Blood. 2016;128(7):1013-1017

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“…The administration of IL-2/anti-IL-2 mAb (clone JES6-1) complexes in vivo has been shown to increase polyclonal Treg numbers in lymphoid organs (29). It has also been reported that the mammalian target of rapamycin inhibitor rapamycin can selectively inhibit proliferation of CD4 + effector T cells, enhance the expansion of Tregs (30,31), and maintain the stability of expanded Tregs (32,33). Therefore, we hypothesized that a combined treatment comprising an islet Ag (BDC2.5 cognate mimetope), IL-2/IL-2 mAb complexes, and rapamycin could act in synergy to expand Ag-specific Tregs in lymphoid organs.…”

mentioning

confidence: 99%

Combination Therapy Using IL-2/IL-2 Monoclonal Antibody Complexes, Rapamycin, and Islet Autoantigen Peptides Increases Regulatory T Cell Frequency and Protects against Spontaneous and Induced Type 1 Diabetes in Nonobese Diabetic Mice

Manirarora

Wei

2015

The Journal of Immunology

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Regulatory T cells (Treg) play a crucial role in the maintenance of self-tolerance. In this study, we sought to expand Ag-specific Tregs in vivo and investigate whether the expanded Tregs can prevent or delay the development of type 1 diabetes (T1D) in the NOD mouse model. NOD mice were treated with a combination of IL-2/anti–IL-2 Ab complex, islet Ag peptide, and rapamycin. After the combined treatment, CD4+CD25+Foxp3+ Tregs were significantly expanded in vivo, they expressed classical Treg markers, exerted enhanced suppressive functions in vitro, and protected against spontaneous development of T1D in NOD mice. Moreover, treated mice were almost completely protected from the adoptively transferred, aggressive form of T1D caused by in vitro–activated cytotoxic islet Ag-specific CD8 T cells. Protection from T1D was transferrable by Tregs and could be attributed to reduced islet infiltration of immune cells as well as the skewing of the immune response toward a Th2 cytokine profile. This new method of peripheral immune regulation could potentially contribute to development of novel immunotherapeutic strategies to prevent the development of T1D or to promote tolerance to islet transplants without using immunosuppressive drugs for long terms.

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Induced Regulatory T Cells Promote Tolerance When Stabilized by Rapamycin and IL-2 In Vivo

Cited by 105 publications

References 57 publications

Chronic graft-versus-host disease: biological insights from preclinical and clinical studies

Chronic graft-versus-host disease: biological insights from preclinical and clinical studies

Therapeutic regulatory T-cell adoptive transfer ameliorates established murine chronic GVHD in a CXCR5-dependent manner

Combination Therapy Using IL-2/IL-2 Monoclonal Antibody Complexes, Rapamycin, and Islet Autoantigen Peptides Increases Regulatory T Cell Frequency and Protects against Spontaneous and Induced Type 1 Diabetes in Nonobese Diabetic Mice

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