Autoimmune Diabetes Onset Results From Qualitative Rather Than Quantitative Age-Dependent Changes in Pathogenic T-Cells

Sylvaine You(Délégation Paris 5), Mériam Belghith(Délégation Paris 5), Stephen Cobbold, Marie‐Alexandra Alyanakian(Délégation Paris 5), Christine Gouarin(Délégation Paris 5), Samia Barriot(Délégation Paris 5), Corinne Garcia(Délégation Paris 5), Herman Waldmann, Jean‐François Bach(Délégation Paris 5), Lucienne Chatenoud(Délégation Paris 5)
Diabetes
May 1, 2005
Cited by 206Open Access
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Abstract

Diabetogenic T-cells can be detected in pre-diabetic nonobese diabetic (NOD) mice after transfer in NOD-SCID recipients. Here we demonstrate that 6-week-old pre-diabetic NOD mice, >2 months before disease onset, already harbor pathogenic T-cells in equal numbers to overtly diabetic animals. The delay in diabetes appearance is explained by the presence of regulatory CD4+ CD25+ T-cells that control diabetogenic effectors and that are, in our hands, transforming growth factor (TGF)-beta-dependent. Our present results suggest, however, that diabetes onset is only partly explained by a decline in this regulatory T-cell activity. Another major factor appears to be the progressive resistance of diabetogenic cells to TGF-beta-dependent mediated inhibition. We propose that progression to overt disease correlates with the pathogenic T-cell's escape from TGF-beta-dependent T-cell-mediated regulation.


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