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Structure-Based Rational and General Strategy for Stabilizing Single-Chain T-Cell Receptors to Enhance Affinity. | LitMetric

Structure-Based Rational and General Strategy for Stabilizing Single-Chain T-Cell Receptors to Enhance Affinity.

J Med Chem

Lab of Computational Chemistry and Drug Design, State Key Laboratory of Chemical Oncogenomics, Peking University Shenzhen Graduate School, Shenzhen 518055, China.

Published: May 2024

AI Article Synopsis

  • The study focuses on improving the stability and solubility of single-chain T-cell receptors (scTCRs) for therapeutic use, addressing their limitations in research and manufacturing.
  • Researchers identified key structural motifs in TCR variable domains and developed a strategy to stabilize scTCRs by modifying specific amino acid residues.
  • The optimized scTCRs maintain high binding affinities similar to traditional TCRs, showcasing their potential for enhanced TCR-related therapies.

Article Abstract

The T-cell receptor (TCR) is a crucial molecule in cellular immunity. The single-chain T-cell receptor (scTCR) is a potential format in TCR therapeutics because it eliminates the possibility of αβ-TCR mispairing. However, its poor stability and solubility impede the in vitro study and manufacturing of therapeutic applications. In this study, some conserved structural motifs are identified in variable domains regardless of germlines and species. Theoretical analysis helps to identify those unfavored factors and leads to a general strategy for stabilizing scTCRs by substituting residues at exact IMGT positions with beneficial propensities on the consensus sequence of germlines. Several representative scTCRs are displayed to achieve stability optimization and retain comparable binding affinities with the corresponding αβ-TCRs in the range of μM to pM. These results demonstrate that our strategies for scTCR engineering are capable of providing the affinity-enhanced and specificity-retained format, which are of great value in facilitating the development of TCR-related therapeutics.

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Source
http://dx.doi.org/10.1021/acs.jmedchem.4c00503DOI Listing

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