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Thomas Stratmann, Natalia Martin-Orozco, Valérie Mallet-Designe, Laurent Poirot, Dorian McGavern, Grigoriy Losyev, Cathleen M. Dobbs, Michael B.A. Oldstone, Kenji Yoshida, Hitoshi Kikutani, Diane Mathis, Christophe Benoist, Kathryn Haskins, Luc Teyton
Published in Volume 112, Issue 6
J Clin Invest. 2003; 112(6):902–914 doi:10.1172/JCI18337
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Figure 8

Ag7 is sufficient to select 2.5mi+CD4+ T cells. (a) Thymocytes, inguinal LNs (ILNs), and PLNs from young adult NOD mice, NOR mice, C57BL/6 mice congenic for H-2g7 (B6.H2g7), and C57BL/6 (B6) mice were stained for CD4, CD8, CD3, and Ag7/2.5mi tetramer. The percentage of Ag7/2.5mi+CD4+CD3hi T cells was electronically calculated from the rectangle gate of each profile. (b) 2.5mi+ T cells accumulate in PLNs of mice that do not get insulitis or diabetes but share Ag7. Average representation (percent) of 2.5mi+CD4+ T cells from NOD, NOR, and B6.H2g7 mice (five to seven mice per group) was measured in four independent experiments. (c) 2.5mi+ T cells are activated in PLNs of mice that do not get insulitis or diabetes but share Ag7. The percentage of CD44hiCD4+Ag7/2.5mi+ T cells in ILNs, PLNs, and MLNs of NOD, NOR, and B6.H2g7 mice (five to seven mice per group) was measured in four independent experiments.