iScience (Feb 2021)

Healthy cells functionally present TAP-independent SSR1 peptides: implications for selection of clinically relevant antigens

  • Antonius A. de Waard,
  • Tamara Verkerk,
  • Kelly Hoefakker,
  • Dirk M. van der Steen,
  • Marlieke L.M. Jongsma,
  • Dganit Melamed Kadosh,
  • Sophie Bliss,
  • Arnoud H. de Ru,
  • Arie Admon,
  • Peter A. van Veelen,
  • Marieke Griffioen,
  • Mirjam H.M. Heemskerk,
  • Robbert M. Spaapen

Journal volume & issue
Vol. 24, no. 2
p. 102051

Abstract

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Summary: Tumors with an impaired transporter associated with antigen processing (TAP) present several endoplasmic reticulum-derived self-antigens on HLA class I (HLA-I) which are absent on healthy cells. Selection of such TAP-independent antigens for T cell-based immunotherapy should include analysis of their expression on healthy cells to prevent therapy-induced adverse toxicities. However, it is unknown how the absence of clinically relevant antigens on healthy cells needs to be validated. Here, we monitored TAP-independent antigen presentation on various healthy cells after establishing a T cell tool recognizing a TAP-independent signal sequence receptor 1-derived antigen. We found that most but not all healthy cells present this antigen under normal and inflammatory conditions, indicating that TAP-independent antigen presentation is a variable phenomenon. Our data emphasize the necessity of extensive testing of a wide variety of healthy cell types to define clinically relevant TAP-independent antigens that can be safely targeted by immunotherapy.

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