The systemic and SmD183-119-autoantigen-specific cytokine memory of Th cells in SLE patients

doi:10.1093/rheumatology/kel180

Rheumatology Advance Access originally published online on July 31, 2006
Rheumatology 2007 46(2):238-245; doi:10.1093/rheumatology/kel180

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The systemic and SmD1^83–119–autoantigen-specific cytokine memory of Th cells in SLE patients

S. Langer¹, D. Langnickel¹, P. Enghard¹, R. Undeutsch¹, G. R. Burmester¹, F. Hiepe¹^,2, A. Radbruch² and G. Riemekasten¹

¹Department of Rheumatology and Clinical Immunology, Charité University Hospital, Humboldt University of Berlin and ²German Rheumatism Research Center, D-10117 Berlin, Germany

Correspondence to: G. Riemekasten, MD, Department of Rheumatology and Clinical Immunology, Charité University Hospital, Schumannstr. 20/21, D-10117 Berlin, Germany. E-mail: gabriela.riemekasten{at}charite.de

Abstract

Objectives. The aim of the study was to analyse the cytokinememory of T-cells derived from systemic lupus erythematosus(SLE) patients and healthy donors enriched for autoantigen-specificT-cells by in vitro stimulation with SmD1^83–119, a commonautoantigen in SLE.

Methods. Autoreactive CD3+ T-cells derived from 37 SLE patientsand 14 healthy donors were enriched by repetitive ex vivo stimulationof peripheral blood mononuclear cells (PBMCs) with SmD1^83–119.For control, PBMCs were stimulated only with interleukin-2 (IL-2).After two rounds of antigenic stimulation, cultures were stimulatedwith PMA/ionomycin to probe the cytokine memory by intracellularcytokine staining. Frequencies of cytokine-expressing T-cellswere analysed and, in SLE patients, compared with disease activitiesand autoantibody levels.

Results. Comparing the cytokine memory in the cultures, SLEpatients displayed higher frequencies of tumour necrosis factor- ${alpha}$ (TNF- ${alpha}$ )+ T-cells than healthy donors and the frequencies correlatedwith disease activity. Frequencies of SmD1^83–119-specificTNF- ${alpha}$ + T-cells and of memory T-cells expressing interferon- ${gamma}$ (IFN- ${gamma}$ )correlated with serum anti-dsDNA antibody levels. The frequenciesof IL-10 expressing SmD1^83–119-specific T-cells were loweramong PBMCs of SLE patients. Relatively higher frequencies ofIL-10+ T-cells in SLE patients correlated with low disease activities,and low anti-dsDNA and anti-SmD1^83–119 antibody concentrationsin culture supernatants.

Conclusions. The memory of autoreactive SmD1^83–119-specificand unspecific stimulated peripheral Th cells for re-expressionof cytokines is shifted towards more cells expressing TNF- ${alpha}$ andless IL-10+ cells, when compared SLE patients with normal donors.This shift towards proinflammatory memory effector Th cellscorrelates with disease severity and humoral autoimmunity.

KEY WORDS: SLE, T-cell cytokines, Cytokine memory, IL-10+ T-cells, Autoantigens

Submitted 8 August 2005; revised version accepted 21 April 2006.
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Rheumatology

The systemic and SmD183–119–autoantigen-specific cytokine memory of Th cells in SLE patients

The systemic and SmD1^83–119–autoantigen-specific cytokine memory of Th cells in SLE patients