Title of article
Structural Engineering of pMHC Reagents for T Cell Vaccines and Diagnostics Original Research Article
Author/Authors
Vesselin Mitaksov، نويسنده , , Steven M. Truscott، نويسنده , , Lonnie Lybarger، نويسنده , , Janet M. Connolly، نويسنده , , Ted H. Hansen، نويسنده , , Daved H. Fremont، نويسنده ,
Issue Information
ماهنامه با شماره پیاپی سال 2007
Pages
14
From page
909
To page
922
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.
Journal title
Chemistry and Biology
Serial Year
2007
Journal title
Chemistry and Biology
Record number
1159412
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