Lung transplant acceptance is facilitated by early events in the graft and is associated with lymphoid neogenesis |
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Authors: | Li W Bribriesco A C Nava R G Brescia A A Ibricevic A Spahn J H Brody S L Ritter J H Gelman A E Krupnick A S Miller M J Kreisel D |
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Affiliation: | 1] Department of Surgery, Washington University in St Louis, St Louis, Missouri, USA [2] The first two authors contributed equally to this work. |
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Abstract: | Early immune responses are important in shaping long-term outcomes of human lung transplants. To examine the role of early immune responses in lung rejection and acceptance, we developed a method to retransplant mouse lungs. Retransplantation into T-cell-deficient hosts showed that for lungs and hearts alloimmune responses occurring within 72 h of transplantation are reversible. In contrast to hearts, a 72-h period of immunosuppression with costimulation blockade in primary allogeneic recipients suffices to prevent rejection of lungs upon retransplantation into untreated allogeneic hosts. Long-term lung acceptance is associated with induction of bronchus-associated lymphoid tissue, where Foxp3+ cells accumulate and recipient T cells interact with CD11c+ dendritic cells. Acceptance of retransplanted lung allografts is abrogated by treatment of immunosuppressed primary recipients with anti-CD25 antibodies. Thus, events contributing to lung transplant acceptance are established early in the graft and induction of bronchus-associated lymphoid tissue can be associated with an immune quiescent state. |
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