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Stefan Lüth, Samuel Huber, Christoph Schramm, Thorsten Buch, Stefan Zander, Christine Stadelmann, Wolfgang Brück, David C. Wraith, Johannes Herkel, Ansgar W. Lohse
Published in Volume 118, Issue 10
J Clin Invest. 2008; 118(10):3403–3410 doi:10.1172/JCI32132
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Figure 5
Selective expansion of autoantigen-specific Tregs in mice expressing the autoantigen ectopically in the liver.

Conventional CD25CD4+ effector T cells (Teff) from Tg4 mice were labeled with CFSE and activated in the absence or presence of CD25+CD4+ Tregs from CRP-MBP or nontransgenic mice at the indicated ratios. (A) Tregs of CRP-MBP and nontransgenic mice showed an equal capacity to suppress after nonspecific stimulation with antibody to CD3. (B) Tregs from CRP-MBP mice showed greatly increased efficacy to suppress after being stimulated with Ac1–9 compared with Tregs from nontransgenic mice, indicating selective expansion of MBP-specific Tregs in CRP-MBP mice. Percentages indicate the proportion of cells that did not proliferate (black peaks).