Computational and Structural Biotechnology Journal (Jan 2022)

A computational algorithm to assess the physiochemical determinants of T cell receptor dissociation kinetics

  • Zachary A. Rollins,
  • Jun Huang,
  • Ilias Tagkopoulos,
  • Roland Faller,
  • Steven C. George

Journal volume & issue
Vol. 20
pp. 3473 – 3481

Abstract

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The rational design of T Cell Receptors (TCRs) for immunotherapy has stagnated due to a limited understanding of the dynamic physiochemical features of the TCR that elicit an immunogenic response. The physiochemical features of the TCR-peptide major histocompatibility complex (pMHC) bond dictate bond lifetime which, in turn, correlates with immunogenicity. Here, we: i) characterize the force-dependent dissociation kinetics of the bond between a TCR and a set of pMHC ligands using Steered Molecular Dynamics (SMD); and ii) implement a machine learning algorithm to identify which physiochemical features of the TCR govern dissociation kinetics. Our results demonstrate that the total number of hydrogen bonds between the CDR2β-MHC⍺(β), CDR1α-Peptide, and CDR3β-Peptide are critical features that determine bond lifetime.

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