S Jurcevic1, P Chandler, S H Sacks, E Simpson. 1. Department of Nephrology & Transplantation, King's College, Guy's, King's and St. Thomas' Medical School, Guy's Hospital, London SE1 9RT, UK. stipo.jurcevic@kcl.ac.uk.
Abstract
BACKGROUND: At present, it is not clear whether xenogeneic MHC molecules are recognized by T cells directly or indirectly through self-MHC-restricted presentation in a transplantation setting. METHODS: We have transplanted skin from HLA-A2 transgenic (B6.A2) to nontransgenic C57BL/6 (B6) mice and investigated the subsequent mouse T-cell responses to HLA molecules, in vivo and in vitro. RESULTS: Skin transplanted from transgenic B6.A2 to B6 mice was rejected rapidly, in 12-16 days. Although naive B6 mice did not respond to B6.A2 splenocytes in vitro, spleen cells from mice that underwent transplantation showed strong proliferative responses. An anti-B6.A2 T-cell line from mice that underwent transplantation made proliferative responses to B6.A2 splenocytes but did not recognize HLA-A2 on human cells or transfected allogeneic mouse cells. The indirect, self-H-2-restricted recognition of HLA-A2 implied by this was confirmed by the finding that lysates of HLA-A2-positive, but not HLA-A2-negative, human B cells were stimulatory when pulsed onto syngeneic antigen-presenting cells and by inhibition of anti-B6.A2 proliferation with both anti-mouse MHC class I and class II antibodies. CONCLUSION: Our results suggest that indirect recognition of xenogeneic MHC antigen plays a predominant role in graft rejection.
BACKGROUND: At present, it is not clear whether xenogeneic MHC molecules are recognized by T cells directly or indirectly through self-MHC-restricted presentation in a transplantation setting. METHODS: We have transplanted skin from HLA-A2 transgenic (B6.A2) to nontransgenic C57BL/6 (B6) mice and investigated the subsequent mouse T-cell responses to HLA molecules, in vivo and in vitro. RESULTS: Skin transplanted from transgenic B6.A2 to B6 mice was rejected rapidly, in 12-16 days. Although naive B6 mice did not respond to B6.A2 splenocytes in vitro, spleen cells from mice that underwent transplantation showed strong proliferative responses. An anti-B6.A2 T-cell line from mice that underwent transplantation made proliferative responses to B6.A2 splenocytes but did not recognize HLA-A2 on human cells or transfected allogeneic mouse cells. The indirect, self-H-2-restricted recognition of HLA-A2 implied by this was confirmed by the finding that lysates of HLA-A2-positive, but not HLA-A2-negative, human B cells were stimulatory when pulsed onto syngeneic antigen-presenting cells and by inhibition of anti-B6.A2 proliferation with both anti-mouse MHC class I and class II antibodies. CONCLUSION: Our results suggest that indirect recognition of xenogeneic MHC antigen plays a predominant role in graft rejection.
Authors: Hideyoshi Toyokawa; Atsunori Nakao; Robert J Bailey; Michael A Nalesnik; Takashi Kaizu; Jerome L Lemoine; Atsushi Ikeda; Koji Tomiyama; Glenn D Papworth; Leaf Huang; Anthony J Demetris; Thomas E Starzl; Noriko Murase Journal: Liver Transpl Date: 2008-03 Impact factor: 5.799