Long-term Persistence of CD4 super(+) but Rapid Disappearance of CD8 super(+) T Cells Expressing an MHC Class I-restricted TCR of Nanomolar Affinity

Most T cells have T cell receptors (TCR) of micromolar affinity for peptide-major histocompatibility complex (MHC) ligands, but genetic engineering can generate TCRs of nanomolar affinity. The affinity of the TCR used, m33, for its cognate non-self peptide-MHC-I complex (SIYRYYGL-K super(b)) is 1,00...

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Bibliographic Details
Published in:Molecular therapy 2012-03, Vol.20 (3), p.652-660
Main Authors: Engels, Boris, Chervin, Adam S, Sant, Andrea J, Kranz, David M, Schreiber, Hans
Format: Article
Language:English
Online Access:Get full text
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Summary:Most T cells have T cell receptors (TCR) of micromolar affinity for peptide-major histocompatibility complex (MHC) ligands, but genetic engineering can generate TCRs of nanomolar affinity. The affinity of the TCR used, m33, for its cognate non-self peptide-MHC-I complex (SIYRYYGL-K super(b)) is 1,000-fold higher than of the wild-type TCR 2C. The affinity of m33 for the self-peptide dEV-8 on K super(b) is only twofold higher. Mouse CD8 super(+) T cells transduced with an m33-encoding retrovirus showed binding of SIY-K super(b) and potent function in vitro, but in vivo these T cells disappeared within hours after transfer into syngeneic hosts without causing graft-versus-host disease (GVHD). Accordingly, in cases where such CD8-dependent self-reactivity might occur in human adoptive T cell therapies, our results show that a peripheral T-cell deletion mechanism could operate to avoid reactions with the host. In contrast to CD8 super(+) T cells, we show that CD4 super(+) T cells expressing m33 survived for months in vivo. Furthermore, the m33-transduced CD4 super(+) T cells were able to mediate antigen-specific rejection of 6-day-old tumors. Together, we show that CD8 super(+) T cell expressing a MHC class I-restricted high-affinity TCR were rapidly deleted whereas CD4 super(+) T cells expressing the same TCR survived and provided function while being directed against a class I-restricted antigen.
ISSN:1525-0016
1525-0024
DOI:10.1038/mt.2011.286