Frontiers in Immunology (Sep 2019)

Hepatitis E Virus (HEV)-Specific T Cell Receptor Cross-Recognition: Implications for Immunotherapy

  • Chai Fen Soon,
  • Chai Fen Soon,
  • Shihong Zhang,
  • Pothakamuri Venkata Suneetha,
  • Dinler Amaral Antunes,
  • Michael Peter Manns,
  • Michael Peter Manns,
  • Solaiman Raha,
  • Christian Schultze-Florey,
  • Christian Schultze-Florey,
  • Immo Prinz,
  • Immo Prinz,
  • Heiner Wedemeyer,
  • Heiner Wedemeyer,
  • Heiner Wedemeyer,
  • Margaret Sällberg Chen,
  • Margaret Sällberg Chen,
  • Markus Cornberg,
  • Markus Cornberg,
  • Markus Cornberg,
  • Markus Cornberg,
  • Markus Cornberg

DOI
https://doi.org/10.3389/fimmu.2019.02076
Journal volume & issue
Vol. 10

Abstract

Read online

T cell immunotherapy is a concept developed for the treatment of cancer and infectious diseases, based on cytotoxic T lymphocytes to target tumor- or pathogen-specific antigens. Antigen-specificity of the T cell receptors (TCRs) is an important selection criterion in the developmental design of immunotherapy. However, off-target specificity is a possible autoimmunity concern if the engineered antigen-specific T cells are cross-reacting to self-peptides in-vivo. In our recent work, we identified several hepatitis E virus (HEV)-specific TCRs as potential candidates to be developed into T cell therapy to treat chronic hepatitis E. One of the identified TCRs, targeting a HLA-A2-restricted epitope at the RNA-dependent RNA polymerase (HEV-1527: LLWNTVWNM), possessed a unique multiple glycine motif in the TCR-β CDR3, which might be a factor inducing cross-reactivity. The aim of our study was to explore if this TCR could cross-recognize self-peptides to underlay autoimmunity. Indeed, we found that this HEV-1527-specific TCR could also cross-recognize an apoptosis-related epitope, Nonmuscle Myosin Heavy Chain 9 (MYH9-478: QLFNHTMFI). While this TCR had dual specificities to both viral epitope and a self-antigen by double Dextramer binding, it was selectively functional against HEV-1527 but not activated against MYH9-478. The consecutive glycine motif in β chain may be the reason promoting TCR binding promiscuity to recognize a secondary target, thereby facilitating cross-recognition. In conclusion, candidate TCRs for immunotherapy development should be screened for autoimmune potential, especially when the TCRs exhibit unique sequence pattern.

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