Fluorine substitutions in an antigenic peptide selectively modulate T-cell receptor binding in a minimally perturbing manner

Piepenbrink, Kurt H; Borbulevych, Oleg Y; Sommese, Ruth F; Clemens, John; Armstrong, Kathryn M; Desmond, Clare; Do, Priscilla; Baker, Brian M

doi:10.1042/BJ20090732

Title: Fluorine substitutions in an antigenic peptide selectively modulate T-cell receptor binding in a minimally perturbing manner

Journal Article · Tue Aug 17 00:00:00 EDT 2010 · Biochem. J.

DOI:https://doi.org/10.1042/BJ20090732· OSTI ID:1006136

Piepenbrink, Kurt H; Borbulevych, Oleg Y; Sommese, Ruth F; Clemens, John; Armstrong, Kathryn M; Desmond, Clare; Do, Priscilla; Baker, Brian M

TCR (T-cell receptor) recognition of antigenic peptides bound and presented by MHC (major histocompatibility complex) molecules forms the basis of the cellular immune response to pathogens and cancer. TCRs bind peptide - MHC complexes weakly and with fast kinetics, features which have hindered detailed biophysical studies of these interactions. Modified peptides resulting in enhanced TCR binding could help overcome these challenges. Furthermore, there is considerable interest in using modified peptides with enhanced TCR binding as the basis for clinical vaccines. In the present study, we examined how fluorine substitutions in an antigenic peptide can selectively impact TCR recognition. Using a structure-guided design approach, we found that fluorination of the Tax peptide [HTLV (human T-cell lymphotropic virus)-1 Tax] enhanced binding by the Tax-specific TCR A6, yet weakened binding by the Tax-specific TCR B7. The changes in affinity were consistent with crystallographic structures and fluorine chemistry, and with the A6 TCR independent of other substitutions in the interface. Peptide fluorination thus provides a means to selectively modulate TCR binding affinity without significantly perturbing peptide composition or structure. Lastly, we probed the mechanism of fluorine's effect on TCR binding and we conclude that our results were most consistent with a 'polar hydrophobicity' mechanism, rather than a purely hydrophobic- or electrostatic-based mechanism. This finding should have an impact on other attempts to alter molecular recognition with fluorine.

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Research Organization:: Argonne National Lab. (ANL), Argonne, IL (United States)

Sponsoring Organization:: USDOE

OSTI ID:: 1006136

Journal Information:: Biochem. J., Vol. 423, Issue 2009; ISSN 0006-2936

Country of Publication:: United States

Language:: ENGLISH

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59 BASIC BIOLOGICAL SCIENCES
99 GENERAL AND MISCELLANEOUS//MATHEMATICS, COMPUTING, AND INFORMATION SCIENCE
AFFINITY
CHEMISTRY
DESIGN
FLUORINATION
FLUORINE
HISTOCOMPATIBILITY COMPLEX
KINETICS
NEOPLASMS
PATHOGENS
PEPTIDES
VACCINES

Title: Fluorine substitutions in an antigenic peptide selectively modulate T-cell receptor binding in a minimally perturbing manner

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