Islet xenotransplantation using gal-deficient neonatal donors improves engraftment and function.
Published
Journal Article
Significant deficiencies in understanding of xenospecific immunity have impeded the success of preclinical trials in xenoislet transplantation. Although galactose-α1,3-galactose, the gal epitope, has emerged as the principal target of rejection in pig-to-primate models of solid organ transplant, the importance of gal-specific immunity in islet xenotransplant models has yet to be clearly demonstrated. Here, we directly compare the immunogenicity, survival and function of neonatal porcine islets (NPIs) from gal-expressing wild-type (WT) or gal-deficient galactosyl transferase knockout (GTKO) donors. Paired diabetic rhesus macaques were transplanted with either WT (n = 5) or GTKO (n = 5) NPIs. Recipient blood glucose, transaminase and serum xenoantibody levels were used to monitor response to transplant. Four of five GTKO versus one of five WT recipients achieved insulin-independent normoglycemia; transplantation of WT islets resulted in significantly greater transaminitis. The WT NPIs were more susceptible to antibody and complement binding and destruction in vitro. Our results confirm that gal is an important variable in xenoislet transplantation. The GTKO NPI recipients have improved rates of normoglycemia, likely due to decreased susceptibility of xenografts to innate immunity mediated by complement and preformed xenoantibody. Therefore, the use of GTKO donors is an important step toward improved consistency and interpretability of results in future xenoislet studies.
Full Text
Duke Authors
Cited Authors
- Thompson, P; Badell, IR; Lowe, M; Cano, J; Song, M; Leopardi, F; Avila, J; Ruhil, R; Strobert, E; Korbutt, G; Rayat, G; Rajotte, R; Iwakoshi, N; Larsen, CP; Kirk, AD
Published Date
- December 2011
Published In
Volume / Issue
- 11 / 12
Start / End Page
- 2593 - 2602
PubMed ID
- 21883917
Pubmed Central ID
- 21883917
Electronic International Standard Serial Number (EISSN)
- 1600-6143
Digital Object Identifier (DOI)
- 10.1111/j.1600-6143.2011.03720.x
Language
- eng
Conference Location
- United States