Immunomodulation Induced By a Novel Immunosuppressant, NK026680 Plus Donor Specific Transfusion Permits a Long-Term Cardiac Allograft Survival in Mice.

Abstract

Background: We have recently demonstrated that a novel triazolopylimidine derivative, NK026680 (NK), inhibits T cell proliferation and prolongs rat cardiac allograft survival. In this study, we examined the immunomodulatory effect of NK in combination with donor specific transfusion (DST) in mice. Methods: A fully MHC incompatible BALB/c-to-C57BL/6 mouse heart transplantation was performed on day 0. DST, 20x106 donor-splenocytes, was given intravenously on day -7. NK (40 mg/kg/day) was orally administered from day -7 to day +6. Recipient-splenocytes were cocultured with irradiated donor-splenocytes, and T cell proliferation (3H-thymidine incorporation), IFN-g production (ELISPOT) and cell phenotypes (FACS) were assessed. Results: Untreated mice promptly rejected cardiac allograft at a graft median survival time (gMST) of 6.5 days. DST or NK monotherapy prolonged gMST to 24.5 and 25.5 days, respectively. In a sharp contrast, NK plus DST treatment (NK+DST) markedly prolonged gMST to 75.5 days. (A). In the NK+DST group, both proliferation and IFN-g production against donorantigens transiently increased on day 0, while they were both significantly suppressed on day 7 (p<0.05, vs. Untreated). Following in vivo antigen-challenge by infusing 20x106 donor-splenocytes on day 0, the splenic Foxp3+CD4+ T cells increased[Figure 1](B); however, CD69+ effector T cells were abolished.Figure: No Caption available.(C and D) in the NK+DST group. Conclusion:NK together with DST induces a potent immunomodulatory effect by shifting immune-balance towards a regulatory milieu, and markedly prolongs cardiac allograft survival in mice. DISCLOSURES:Saiga, K.: Employee, salary.