TY - JOUR
T1 - Anti-TCRβ mAb induces long-term allograft survival by reducing antigen-reactive T cells and sparing regulatory T cells
AU - Miyahara, Y.
AU - Khattar, M.
AU - Schroder, P. M.
AU - Mierzejewska, B.
AU - Deng, R.
AU - Han, R.
AU - Hancock, W. W.
AU - Chen, W.
AU - Stepkowski, S. M.
N1 - Copyright:
Copyright 2012 Elsevier B.V., All rights reserved.
PY - 2012/6
Y1 - 2012/6
N2 - TCR specific antibodies may modulate the TCR engagement with antigen-MHC complexes, and in turn regulate in vivo T cell responses to alloantigens. Herein, we found that in vivo administration of mAbs specific for mouse TCRβ (H57-597), TCRα or CD3 promptly reduced the number of CD4 + and CD8 + T cells in normal mice, but H57-597 mAb most potently increased the frequency of CD4 +Foxp3 + Treg cells. When mice were injected with staphylococcal enterotoxin B (SEB) superantigen and H57-597 mAb, the expansion of SEB-reactive Vβ8 + T cells was completely abrogated while SEB-nonreactive Vβ2 + T cells remained unaffected. More importantly, transient H57-597 mAb treatment exerted long-lasting effect in preventing T cell responses to alloantigens, and produced long-term cardiac allograft survival (>100 days) in 10 out of 11 recipients. While Treg cells were involved in maintaining donor-specific long-term graft survival, T cell homeostasis recovered over time and immunity was retained against third party allografts. Moreover, transient H57-597 mAb treatment significantly prolonged survival of skin allografts in naïve recipients as well as heart allografts in skin-sensitized recipients. Thus, transient modulation of the TCRβ chain by H57-597 mAb exhibits potent, long-lasting therapeutic effects to control alloimmune responses. This study shows that peri-transplant therapy with a T cell receptor-specific antibody induces long-term allograft survival in mice by selective reduction of antigen-reactive T cells while sparing regulatory CD4+Foxp3+ T cells.
AB - TCR specific antibodies may modulate the TCR engagement with antigen-MHC complexes, and in turn regulate in vivo T cell responses to alloantigens. Herein, we found that in vivo administration of mAbs specific for mouse TCRβ (H57-597), TCRα or CD3 promptly reduced the number of CD4 + and CD8 + T cells in normal mice, but H57-597 mAb most potently increased the frequency of CD4 +Foxp3 + Treg cells. When mice were injected with staphylococcal enterotoxin B (SEB) superantigen and H57-597 mAb, the expansion of SEB-reactive Vβ8 + T cells was completely abrogated while SEB-nonreactive Vβ2 + T cells remained unaffected. More importantly, transient H57-597 mAb treatment exerted long-lasting effect in preventing T cell responses to alloantigens, and produced long-term cardiac allograft survival (>100 days) in 10 out of 11 recipients. While Treg cells were involved in maintaining donor-specific long-term graft survival, T cell homeostasis recovered over time and immunity was retained against third party allografts. Moreover, transient H57-597 mAb treatment significantly prolonged survival of skin allografts in naïve recipients as well as heart allografts in skin-sensitized recipients. Thus, transient modulation of the TCRβ chain by H57-597 mAb exhibits potent, long-lasting therapeutic effects to control alloimmune responses. This study shows that peri-transplant therapy with a T cell receptor-specific antibody induces long-term allograft survival in mice by selective reduction of antigen-reactive T cells while sparing regulatory CD4+Foxp3+ T cells.
KW - Allograft survival
KW - T cell receptor
KW - T regulatory cells
KW - tolerance
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U2 - 10.1111/j.1600-6143.2012.04006.x
DO - 10.1111/j.1600-6143.2012.04006.x
M3 - Review article
C2 - 22420295
AN - SCOPUS:84862832381
SN - 1600-6135
VL - 12
SP - 1409
EP - 1418
JO - American Journal of Transplantation
JF - American Journal of Transplantation
IS - 6
ER -