Grants Funded

Abstract
Currently described regimens based on costimulation blockade for the induction of tolerance have been developed utilizing experimental models of organ transplantation. A nerve allograft differs from an organ allograft because it acts as a temporary conduit to guide nerve regeneration whereas an organ allograft is permanent. Once the host peripheral nerve has regenerated through the allograft and the donor cells have been replaced, immunosuppression is no longer necessary. Anti-CD40 ligand costimulation blocking antibody is able to induce an extended period of immune unresponsiveness without additional dosing following antibody administration. We hypothesize that a single dose of costimulation-blocking antibody(s) is sufficient for successful regeneration in the murine peripheral nerve allograft model. The dosage may be further reduced by combination with additional treatments such as T-cell depletion and donor bone marrow transplantation. Anti-CD40L antibody has been used in clinical trials for bone marrow transplantation and is potentially an essential part of strategies that will be used clinically for organ transplantation. The findings of this study will determine the ability for successful clinical nerve transplantation using lower doses and shorter courses of antibody therapy than are required for organ transplantation.