CD28 costimulation is essential for human T regulatory expansion and function

TN Golovina, T Mikheeva, MM Suhoski… - The Journal of …, 2008 - journals.aai.org
TN Golovina, T Mikheeva, MM Suhoski, NA Aqui, VC Tai, X Shan, R Liu, RR Balcarcel…
The Journal of Immunology, 2008journals.aai.org
The costimulatory requirements required for peripheral blood T regulatory cells (Tregs) are
unclear. Using cell-based artificial APCs we found that CD28 but not ICOS, OX40, 4-1BB,
CD27, or CD40 ligand costimulation maintained high levels of Foxp3 expression and in vitro
suppressive function. Only CD28 costimulation in the presence of rapamycin consistently
generated Tregs that consistently suppressed xenogeneic graft-vs-host disease in
immunodeficient mice. Restimulation of Tregs after 8–12 days of culture with CD28 …
Abstract
The costimulatory requirements required for peripheral blood T regulatory cells (Tregs) are unclear. Using cell-based artificial APCs we found that CD28 but not ICOS, OX40, 4-1BB, CD27, or CD40 ligand costimulation maintained high levels of Foxp3 expression and in vitro suppressive function. Only CD28 costimulation in the presence of rapamycin consistently generated Tregs that consistently suppressed xenogeneic graft-vs-host disease in immunodeficient mice. Restimulation of Tregs after 8–12 days of culture with CD28 costimulation in the presence of rapamycin resulted in> 1000-fold expansion of Tregs in< 3 wk. Next, we determined whether other costimulatory pathways could augment the replicative potential of CD28-costimulated Tregs. We observed that while OX40 costimulation augmented the proliferative capacity of CD28-costimulated Tregs, Foxp3 expression and suppressive function were diminished. These studies indicate that the costimulatory requirements for expanding Tregs differ from those for T effector cells and, furthermore, they extend findings from mouse Tregs to demonstrate that human postthymic Tregs require CD28 costimulation to expand and maintain potent suppressive function in vivo.
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