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Article: A Mixed-chimerism Protocol Utilizing Thymoglobulin and Belatacept Did Not Induce Lung Allograft Tolerance, Despite Previous Success in Renal Allotransplantation.

Sommer, Wiebke / O, Jane M / Pruner, Kurt B / Dehnadi, Abbas / Ha Huh, Kyu / Robinson, Kortney A / Hanekamp, Isabel / Rosales, Ivy / Bean, Alison S / Paster, Josh / Oura, Tetsu / Neal Smith, Rex / Colvin, Robert / Benichou, Gilles / Kawai, Tatsuo / Madsen, Joren C / Allan, James S

Transplantation direct

2021  Volume 7, Issue 6, Page(s) e705

Abstract: Background: In kidney transplantation, long-term allograft acceptance in cynomolgus macaques was achieved using a mixed-chimerism protocol based on the clinically available reagents, rabbit anti-thymocyte globulin (ATG), and belatacept. Here, we have ... ...

Abstract Background: In kidney transplantation, long-term allograft acceptance in cynomolgus macaques was achieved using a mixed-chimerism protocol based on the clinically available reagents, rabbit anti-thymocyte globulin (ATG), and belatacept. Here, we have tested the same protocol in cynomolgus macaques transplanted with fully allogeneic lung grafts.
Methods: Five cynomolgus macaques underwent left orthotopic lung transplantation. Initial immunosuppression included equine ATG and anti-IL6RmAb induction, followed by triple-drug immunosuppression for 4 mo. Post-transplant, a nonmyeloablative conditioning regimen was applied, including total body and thymic irradiation. Rabbit ATG, belatacept, anti-IL6RmAb, and donor bone marrow transplantation (DBMT) were given, in addition to a 28-d course of cyclosporine. All immunosuppressant drugs were stopped on day 29 after DBMT.
Results: One monkey rejected its lung before DBMT due to AMR, after developing donor-specific antibodies. Two monkeys developed fatal post-transplant lymphoproliferative disorder, and both monkeys had signs of cellular rejection in their allografts upon autopsy. The remaining 2 monkeys showed severe cellular rejection on days 42 and 70 post-DBMT. Cytokine analysis suggested higher levels of pro-inflammatory markers in the lung transplant cohort, as compared to kidney recipients.
Conclusion: Although the clinically applicable protocol showed success in kidney transplantation, the study did not show long-term survival in a lung transplant model, highlighting the organ-specific differences in tolerance induction.
Language English
Publishing date 2021-05-25
Publishing country United States
Document type Journal Article
ISSN 2373-8731
ISSN 2373-8731
DOI 10.1097/TXD.0000000000001150
Database MEDical Literature Analysis and Retrieval System OnLINE

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