Minor Antigen H60-Mediated Aplastic Anemia Is Ameliorated by Immunosuppression and the Infusion of Regulatory T Cells

Chen, Jichun; Ellison, Felicia M.; Eckhaus, Michael; Smith, Aleah; Keyvanfar, Keyvan; Calado, Rodrigo T.; Young, Neal S.

doi:10.4049/jimmunol.178.7.4159

Cited by 69 publications

(83 citation statements)

References 48 publications

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“…25,26,34 At 10 days after LN injection, the proportion of IL-17A positive CD4 ϩ cells in B6 LN-cellinfused animals (15.0% Ϯ 1.1%) was significantly higher (P Ͻ .01) than that in TBI-only controls (6.5% Ϯ 1.3%). Almost no IL-17A positive CD4 ϩ cells were detectable in untreated animals ( Figure 4A upper panels).…”

Section: Dynamics Of Th1 and Th17 Immune Responses In A Mouse Model Omentioning

confidence: 99%

Th17 immune responses contribute to the pathophysiology of aplastic anemia

Latour

Visconte

Takaku

et al. 2010

Blood

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T helper type 17 (Th17) cells have been characterized based on production of interleukin-17 (IL-17) and association with autoimmune diseases. We studied the role of Th17 cells in aplastic anemia (AA) by isolating Th17 cells from patients blood (n ‫؍‬ 41) and bone marrow (BM) mononuclear cells (n ‫؍‬ 7). The frequency and total number of CD3 ؉ CD4 ؉ IL-17-producing T cells were increased in AA patients at presentation compared with healthy controls (P ‫؍‬ .0007 and .02, respectively) and IntroductionTh17 cells have been characterized recently in mice as a novel subset of CD4 ϩ T cells that produce interleukin-17A (IL-17A), IL-17-F, and IL-22, 1,2 and serve as immune effectors in various settings, including inflammation, infection, and autoimmunity. 3,4 Th17 cells produce a large amount of IL-17A, a cytokine that coordinates tissue inflammation by inducing the expression of proinflammatory cytokines (such as IL-6 and tumor necrosis factor [TNF]), chemokines (such as KC, MCP-1, and MIP-2), and matrix metalloproteases that mediate tissue infiltration and tissue destruction. 5 In mice, the differentiation program of Th17 cells from naive CD4 ϩ T cells requires the activation of the transcription factor, orphan nuclear receptor ROR␥t, 6 and the presence of IL-6 and transforming growth factor-␤ (TGF-␤). 7,8 In humans, Th17 differentiation is under the control of IL-1␤, 10 Several studies have reported the association of IL-17 with inflammatory disorders, such as rheumatoid arthritis, asthma, multiple sclerosis, and lupus, 11 as well as hematologic disorders, such as myelodysplastic syndrome 12,13 and acute myeloid leukemia. 14 Aplastic anemia (AA), a disease characterized by peripheral blood pancytopenia and bone marrow (BM) hypoplasia, 15 is an immunemediated disorder in most cases with active destruction of hematopoietic cells by effector T lymphocytes. 16 Recovery of autologous hematopoiesis in patients who failed to engraft after conditioning and stem cell transplantation, 17 and responsiveness of patients to immunosuppressive therapies, 18 provided powerful evidence for the pivotal role of the immune system in the disease pathophysiology. Immoderate production of interferon-␥ (IFN-␥), TNF-␣, and IL-2 from patients'T cells suggests that the hematopoietic cells are destroyed through a Th1 response, [19][20][21] as illustrated by the up-regulation of the transcription factor T-bet in patient T cells. 22 The description of nonrandom skewing of the V␤ chain families of the T-cell receptor in patient peripheral blood (PB) revealed that expanded oligoclonal or monoclonal specific V␤ subfamilies selectively induced apoptosis of hematopoietic progenitor cells. 23 Regulatory T cells (Tregs), which control and suppress autoreactive T cells, are decreased at disease presentation in almost all patients. 24 We have developed murine models for immune-mediated BM failure by the infusion of allogeneic lymph node (LN) cells into sublethally irradiated recipients for which treatment with limited number of Treg cells, 25 or anti-IFN...

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Section: Dynamics Of Th1 and Th17 Immune Responses In A Mouse Model Omentioning

confidence: 99%

Th17 immune responses contribute to the pathophysiology of aplastic anemia

Latour

Visconte

Takaku

et al. 2010

Blood

Self Cite

158

139

View full text Add to dashboard Cite

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“…Although numerous mechanisms have been proposed to explain the suppressive function of Tregs, none appears to be unifying, and the development of immunomodulating pharmacotherapies has been limited. 9 In mouse models, adoptive immunotherapy with Tregs has been shown to be effective in the prevention of experimental autoimmune encephalomyelitis, 10 type 1 diabetes, 11 SLE,12 autoimmune gastritis, 13 inflammatory bowel disease, 14 aplastic anemia, 15 graft rejection, 16 and GVHD. 17 It is likely that CD4 ϩ FOXP3 ϩ Tregs represent a mixture of thymic-derived and FOXP3 ϩ Tregs that are generated at peripheral sites.…”

Section: Introductionmentioning

confidence: 99%

Selective expression of latency-associated peptide (LAP) and IL-1 receptor type I/II (CD121a/CD121b) on activated human FOXP3+ regulatory T cells allows for their purification from expansion cultures

Tran

Andersson

Hardwick

et al. 2009

Blood

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Although adoptive transfer of regulatory T cells (Foxp3 ؉ Tregs) has proven to be efficacious in the prevention and treatment of autoimmune diseases and graftversus-host disease in rodents, a major obstacle for the use of Treg immunotherapy in humans is the difficulty of obtaining a highly purified preparation after ex vivo expansion. We have identi- IntroductionRegulatory T cells (CD4 ϩ FOXP3 ϩ , Tregs) are central to the maintenance of self-tolerance and the control of immune homeostasis. 1 A diminished frequency or dysfunction of Tregs has been reported in many human diseases, including systemic lupus erythematosus (SLE), 2 type 1 diabetes, 3 multiple sclerosis, 4 aplastic anemia, 5 idiopathic thrombocytopenic purpura, 6 graft-versushost disease (GVHD) 7 and transplant rejection. 8 A detailed cellular and molecular understanding of the mechanisms of action of Tregs should provide a strong foundation for pharmacologic and therapeutic manipulation of their functions. Although numerous mechanisms have been proposed to explain the suppressive function of Tregs, none appears to be unifying, and the development of immunomodulating pharmacotherapies has been limited. 9 In mouse models, adoptive immunotherapy with Tregs has been shown to be effective in the prevention of experimental autoimmune encephalomyelitis, 10 type 1 diabetes, 11 SLE, 12 autoimmune gastritis, 13 inflammatory bowel disease, 14 aplastic anemia, 15 graft rejection, 16 and GVHD. 17 It is likely that CD4 ϩ FOXP3 ϩ Tregs represent a mixture of thymic-derived and FOXP3 ϩ Tregs that are generated at peripheral sites. 18 Human Tregs can be expanded ex vivo, 19,20 and their use for the cell-based tolerogenic therapy of autoimmune diseases, graft rejection, or GVHD has been advocated. 21,22 The major obstacle for the use of human Tregs in cell-based therapy is the difficulty of obtaining a highly pure population after ex vivo expansion. A CD4 ϩ FOXP3 ϩ population of greater than 90% purity can be isolated by fluorescence-activated cell sorting (FACS) of the top 2% to 4% of CD4 ϩ T cells with high CD25 expression (CD25 hi ) from peripheral blood, but frequently the percentage of FOXP3 ϩ T cells decreases to 75% after 1 week and to 50% after 2 weeks of expansion by stimulation with anti-CD3/CD28 and IL-2. 23 A more complex problem is the validity of FOXP3 as a bona fide marker of human Tregs. We have recently shown that expression of FOXP3 can be induced by T-cell receptor (TCR) stimulation of human CD4 ϩ CD25 Ϫ FOXP3 Ϫ T cells in the presence of TGF␤, but the induced cells lack all the functional properties of Tregs. 24 Because TGF␤ is present in the serum used for cultures, a similar induction of FOXP3 expression in contaminating FOXP3 Ϫ T cells may occur during expansion cultures of partially purified Tregs. Although the expanded population might appear to be highly enriched in FOXP3 ϩ cells, many of these cells may be induced FOXP3 ϩ cells that lack Treg functions.We have identified 3 unique cell-surface markers, latencyassociated peptide (LAP) and IL-...

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“…According to the widely-accepted model of acquired aplastic anemia (AA), cytotoxic T lymphocytes (CTLs) recognize auto-antigens that are presented on hematopoietic stem cells (HSCs) through their class I human leukocyte antigen (HLA) molecules, playing an important role in initiation of the autoimmune reactions that lead to bone marrow (BM) failure [1][2][3]. Several indirect pieces of evidence have been reported in previous studies, such as the accumulation of T cells with particular clonotypes as demonstrated by T-cell receptor analyses [2,4,5], as well as the presence of T-cell clones capable of killing myeloid leukemia cell lines within the BM [6,7].…”

Section: Introductionmentioning

confidence: 99%

“…Several indirect pieces of evidence have been reported in previous studies, such as the accumulation of T cells with particular clonotypes as demonstrated by T-cell receptor analyses [2,4,5], as well as the presence of T-cell clones capable of killing myeloid leukemia cell lines within the BM [6,7]. However, it is entirely unknown what kind of cells the antigen-specific T cells attack and how these T cells diminish HSCs…”

Section: Introductionmentioning

confidence: 99%