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Acute rejection of vascular heart allografts by perforin-deficient mice
Authors:Manfred Schulz,Henk-Jan Schuurman,Joanne Joergensen,Carolina Steiner,Timo Meerloo,David K  gi,Hans Hengartner,Rolf M. Zinkernagel,Max H. Schreier,Kurt Bü  rki,Birgit Ledermann
Affiliation:Manfred Schulz,Henk-Jan Schuurman,Joanne Joergensen,Carolina Steiner,Timo Meerloo,David Kägi,Hans Hengartner,Rolf M. Zinkernagel,Max H. Schreier,Kurt Bürki,Birgit Ledermann
Abstract:To study the role of perforin in cell-mediated graft rejection, vascularized hearts were grafted to perforin-deficient C57BL/6 and control C57BL/6 recipient mice. Fully allogeneic heart grafts (BALB/c) were acutely rejected by both recipients within 6 days. Peritoneal exudate lymphocytes from control mice but not from perforin-deficient mice exhibit a strong alloreactive cytotoxic activity in vitro. Histological analysis of the rejected tissues demonstrated extensive mononuclear cell infiltrates in both recipients. Flow cytometry analysis and immunohistology of graft-infiltrating cells showed similar proportions of lymphocyte subsets (CD8 ≧ CD4). Collectively, these data indicate that perforin is not essential in the cell-mediated acute rejection of a fully mismatched heart allograft. However, perforin-dependent effector mechanisms appeared to be limiting in the T cellmediated rejection of heart allografts differing only at a single major histocompatibility complex class I antigen (bm1), because these grafts survived longer (mean 87.8 days) in perforin-deficient than in control mice (mean 31.5 days).
Keywords:Perforin  Graft rejection  Mice
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