Naive and memory T cells induce different types of graft-versus-host disease

S Dutt, D Tseng, J Ermann, TI George… - The Journal of …, 2007 - journals.aai.org
S Dutt, D Tseng, J Ermann, TI George, YP Liu, CR Davis, CG Fathman, S Strober
The Journal of Immunology, 2007journals.aai.org
The goal of this study was to compare the ability of donor naive and alloantigen-primed
effector memory T cells to induce graft-vs-host disease after bone marrow transplantation in
MHC-mismatched irradiated host mice. Purified CD4+ naive (CD62L high CD44 low) T cells
and CD4+ effector memory (CD62L low CD44 high) T cells obtained from unprimed donors
and donors primed to host alloantigens, respectively, were injected into host mice, and the
rapidity, severity, and pattern of tissue injury of graft-vs-host disease was assessed …
Abstract
The goal of this study was to compare the ability of donor naive and alloantigen-primed effector memory T cells to induce graft-vs-host disease after bone marrow transplantation in MHC-mismatched irradiated host mice. Purified CD4+ naive (CD62L high CD44 low) T cells and CD4+ effector memory (CD62L low CD44 high) T cells obtained from unprimed donors and donors primed to host alloantigens, respectively, were injected into host mice, and the rapidity, severity, and pattern of tissue injury of graft-vs-host disease was assessed. Unexpectedly, the naive T cells induced a more acute and severe colitis than the primed memory cells. Whereas the naive T cells expressing CD62L and CCR7 lymph node homing receptors vigorously expanded in mesenteric lymph nodes and colon by day 6 after transplantation, the primed memory T cells without these receptors had 20-to 100-fold lower accumulation at this early time point. These differences were reflected in the significantly more rapid decline in survival and weight loss induced by naive T cells. The primed memory T cells had a greater capacity to induce chronic colitis and liver injury and secrete IL-2 and IFN-γ in response to alloantigenic stimulation compared with memory T cells from unprimed donors. Nevertheless, the expected increase in potency as compared with naive T cells was not observed due to differences in the pattern and kinetics of tissue injury.
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