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TCR affinity for p/MHC formed by tumor antigens that are self-proteins: impact on efficacy and toxicity.


ABSTRACT: Recent studies have shown that the range of affinities of T cell receptors (TCRs) against non-mutated cancer peptide/class I complexes are lower than TCR affinities for foreign antigens. Raising the affinity of TCRs for optimal activity of CD8 T cells, and for recruitment of CD4 T cell activity against a class I antigen, provides opportunities for more robust adoptive T cell therapies. However, TCRs with enhanced affinities also risk increased reactivity with structurally related self-peptides, and off-target toxicities. Careful selection of tumor peptide antigens, in silico proteome screens, and in vitro peptide specificity assays will be important in the development of the most effective, safe TCR-based adoptive therapies.

SUBMITTER: Stone JD 

PROVIDER: S-EPMC4920053 | biostudies-literature | 2015 Apr

REPOSITORIES: biostudies-literature

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TCR affinity for p/MHC formed by tumor antigens that are self-proteins: impact on efficacy and toxicity.

Stone Jennifer D JD   Harris Daniel T DT   Kranz David M DM  

Current opinion in immunology 20150122


Recent studies have shown that the range of affinities of T cell receptors (TCRs) against non-mutated cancer peptide/class I complexes are lower than TCR affinities for foreign antigens. Raising the affinity of TCRs for optimal activity of CD8 T cells, and for recruitment of CD4 T cell activity against a class I antigen, provides opportunities for more robust adoptive T cell therapies. However, TCRs with enhanced affinities also risk increased reactivity with structurally related self-peptides,  ...[more]

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