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Structural engineering of pMHC reagents for T cell vaccines and diagnostics.


ABSTRACT: MHC class I peptide complexes (pMHC) are routinely used to enumerate T cell populations and are currently being evaluated as vaccines to tumors and specific pathogens. Herein, we describe the structures of three generations of single-chain pMHC progressively designed for the optimal presentation of covalently associated epitopes. Our ultimate design employs a versatile disulfide trap between an invariant MHC residue and a short C-terminal peptide extension. This general strategy is nondisruptive of native pMHC conformation and T cell receptor engagement. Indeed, cell-surface-expressed MHC complexes with disulfide-trapped epitopes are refractory to peptide exchange, suggesting they will make safe and effective vaccines. Furthermore, we find that disulfide-trap stabilized, recombinant pMHC reagents reliably detect polyclonal CD8 T cell populations as proficiently as conventional reagents and are thus well suited to monitor or modulate immune responses during pathogenesis.

SUBMITTER: Mitaksov V 

PROVIDER: S-EPMC3601489 | biostudies-literature | 2007 Aug

REPOSITORIES: biostudies-literature

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Structural engineering of pMHC reagents for T cell vaccines and diagnostics.

Mitaksov Vesselin V   Truscott Steven M SM   Lybarger Lonnie L   Connolly Janet M JM   Hansen Ted H TH   Fremont Daved H DH  

Chemistry & biology 20070801 8


MHC class I peptide complexes (pMHC) are routinely used to enumerate T cell populations and are currently being evaluated as vaccines to tumors and specific pathogens. Herein, we describe the structures of three generations of single-chain pMHC progressively designed for the optimal presentation of covalently associated epitopes. Our ultimate design employs a versatile disulfide trap between an invariant MHC residue and a short C-terminal peptide extension. This general strategy is nondisruptive  ...[more]

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