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Computationally driven deletion of broadly distributed T cell epitopes in a biotherapeutic candidate.

Cell Mol Life Sci.. 2014-06; 
Salvat RS, Parker AS, Guilliams A, Choi Y, Bailey-Kellogg C, Griswold KE. Thayer School of Engineering, Dartmouth College, 14 Engineering Dr., Hanover, NH, 03755, USA.
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摘要

Biotherapeutics are subject to immune surveillance within the body, and anti-biotherapeutic immune responses can compromise drug efficacy and patient safety. Initial development of targeted antidrug immune memory is coordinated by T cell recognition of immunogenic subsequences, termed "T cell epitopes." Biotherapeutics may therefore be deimmunized by mutating key residues within cognate epitopes, but there exist complex trade-offs between immunogenicity, mutational load, and protein structure-function. Here, a protein deimmunization algorithm has been applied to P99 beta-lactamase, a component of antibody-directed enzyme prodrug therapies. The algorithm, integer programming for immunogenic proteins, s... More

关键词

Biotherapeutics; Protein engineering; Immunogenicity; Deimmunization; Epitope deletion; Computational protein design