Global Natural Regulatory T Cell Depletion in Active Systemic Lupus Erythematosus

122

Objective. To define the phenotype and function of CD4؉,CD25؉ regulatory T cells (Treg) in patients with cutaneous lupus erythematosus (CLE), a heterogeneous autoimmune disease characterized primarily by inflammatory skin lesions.Methods. The number of Treg in skin specimens obtained from patients with various subtypes of CLE was investigated by immunohistochemical analysis, using anti-Foxp3 and anti-CD4 monoclonal antibodies. Furthermore, characterization of peripheral blood CD4؉,CD25؉ Treg from normal healthy donors and patients with CLE was carried out by flow cytometry, analyzing the expression of Foxp3 and Treg subpopulations. We also purified CD4؉,CD25 high Treg obtained from patients with CLE and tested the sensitivity of these cells to CD95L-mediated apoptosis.Results. Quantitative analysis of CD4؉ T cells in skin lesions from patients with CLE revealed that the number was similar to that in lesions from patients with other chronic inflammatory diseases, but the number of Foxp3؉ Treg in CLE was significantly reduced. There was no correlation between disease subtype and the frequency of Foxp3؉ Treg in the skin of patients with CLE. In peripheral blood, no significant differences were observed in the number and phenotype of CD4؉,CD25؉ Treg or in the sensitivity to apoptosis of CD4؉,CD25 high Treg derived from patients with CLE and those derived from normal healthy donors.Conclusion. These data suggest that an organspecific abnormality of Treg in the skin underscores the importance of analyzing Treg in the affected tissue. Such a local process might give insight into the pathogenic mechanisms of CLE and differs from a global peripheral dysfunction as reported for patients with a systemic manifestation of the disease.

Section: Discussionmentioning

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Section: Cd4؉foxp3؉ T Cells In the Skin Of Patients With Clementioning

confidence: 91%

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confidence: 99%

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Low number of regulatory T cells in skin lesions of patients with cutaneous lupus erythematosus

Franz¹,

Fritzsching²,

Riehl³

et al. 2007

122

Functional defect of circulating regulatory CD4+ T cells in patients with Wegener's granulomatosis in remission

Abdulahad¹,

Stegeman²,

Geld³

et al. 2007

157

117

Objective. Accumulating data support the role of regulatory T cells, a subset of CD4؉ T cells that expresses CD25high and the transcription factor forkhead box P3 (FoxP3), in controlling and preventing autoimmunity. In Wegener's granulomatosis (WG), an autoimmune vasculitis, up-regulation of CD25 on circulating CD4؉ T cells has been observed, even in patients in remission. The objective of this study was to test whether the frequency and/or function of Treg cells from WG patients in remission are disturbed.Methods. Peripheral blood mononuclear cells were freshly isolated from 52 WG patients in remission and from 27 age-and sex-matched healthy control subjects. The proportion of circulating Treg cells was assessed by flow cytometry using CD4, CD25, FoxP3, and CD45RO markers. Anergy and suppressive function of CD25 high ,CD4؉ T cells were determined using polyclonal stimulants and coculture assay in 10 WG patients in remission and in 10 age-and sex-matched healthy controls.Results. In WG patients, a significant increase was observed in the percentage of circulating

Dysfunctional CD4+,CD25+ regulatory T cells in untreated active systemic lupus erythematosus secondary to interferon‐α–producing antigen‐presenting cells

Yan¹,

Ye²,

Chen³

et al. 2008

164

129

Objective. To explore whether there are extrinsic factors that impair the suppressive function of CD4؉,CD25؉ regulatory T cells in patients with untreated active systemic lupus erythematosus (SLE).Methods. We studied 15 patients with untreated active SLE, 10 patients with SLE in remission, and 15 healthy control subjects. Percentages of CD4؉,CD25؉, FoxP3؉ Treg cells and levels of forkhead box P3 (FoxP3) protein were analyzed by flow cytometry. Expression of messenger RNA (mRNA) for FoxP3 in purified Treg cell populations was assessed by real-time polymerase chain reaction analysis. Experiments examining Treg cell function in SLE were designed to distinguish primary from secondary T cell dysfunction. Levels of interferon-␣ (IFN␣) in supernatants from the function assays were determined with an IFN-stimulated response element-luciferase reporter assay.Results. The percentage of CD4؉,CD25؉, FoxP3؉ cells in peripheral blood was significantly increased in SLE patients as compared with controls (mean ؎ SEM 9.11 ؎ 0.73% versus 4.78 ؎ 0.43%; P < 0.0001). We found no difference in FoxP3 expression at either the mRNA or protein level in any CD4؉,CD25؉ T cell subset from SLE patients as compared with controls. Antigen-presenting cells (APCs) from SLE patients were responsible for decreased Treg cell activity and could also render dysfunctional Treg cells from healthy control subjects. CD4؉,CD25؉ Treg cells from SLE patients exhibited normal suppressive activity when cultured with APCs from healthy controls. A partial Treg cell blockade effect was induced by the high levels of IFN␣ derived from SLE patient APCs.Conclusion. We suggest that blockade of Treg cell-mediated suppression by IFN␣-producing APCs in SLE patients may contribute to a pathogenic loss of peripheral tolerance in this disease.