Reference Database

YearReference
2021
The self-peptide repertoire plays a critical role in transplant tolerance induction.
Son, Eric T
Faridi, Pouya
Paul-Heng, Moumita
Leong, Mario L
English, Kieran
Ramarathinam, Sri H
Braun, Asolina
Dudek, Nadine L
Alexander, Ian E
Lisowski, Leszek
Bertolino, Patrick
Bowen, David G
Purcell, Anthony W
Mifsud, Nicole A
Sharland, Alexandra F
The Journal of clinical investigation 2021 Nov 01;131(21): e146771
Abstract

While direct allorecognition underpins both solid organ allograft rejection and tolerance induction, the specific molecular targets of most directly alloreactive CD8+ T cells have not been defined. In this study, we used a combination of genetically engineered major histocompatibility complex class I (MHC I) constructs, mice with a hepatocyte-specific mutation in the class I antigen-presentation pathway, and immunopeptidomic analysis to provide definitive evidence for the contribution of the peptide cargo of allogeneic MHC I molecules to transplant tolerance induction. We established a systematic approach for the discovery of directly recognized pMHC epitopes and identified 17 strongly immunogenic H-2Kb-associated peptides recognized by CD8+ T cells from B10.BR (H-2k) mice, 13 of which were also recognized by BALB/c (H-2d) mice. As few as 5 different tetramers used together were able to identify a high proportion of alloreactive T cells within a polyclonal population, suggesting that there are immunodominant allogeneic MHC-peptide complexes that can account for a large component of the alloresponse.

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