International Journal of Molecular Sciences (May 2017)

TRAV7-2*02 Expressing CD8+ T Cells Are Responsible for Palladium Allergy

  • Yuri Takeda,
  • Yoshiko Suto,
  • Koyu Ito,
  • Wataru Hashimoto,
  • Tadashi Nishiya,
  • Kyosuke Ueda,
  • Takayuki Narushima,
  • Tetsu Takahashi,
  • Kouetsu Ogasawara

DOI
https://doi.org/10.3390/ijms18061162
Journal volume & issue
Vol. 18, no. 6
p. 1162

Abstract

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While metallic biomaterials have led to an improvement in the quality of life, metal allergies, especially to palladium (Pd), has caused a recent increase in allergic patients. Metal allergy is known to be a T cell-mediated delayed-type hypersensitivity (DTH); however, the pathogenic T cell subsets and the specific T cell receptor (TCR) have not been identified. Therefore, we attempted to identify the pathogenic T cells responsible for Pd allergy. We found that activating CD8+ T cells significantly increased and that the TRAV (TCRα variable) 7-2*02 chain skewed in Pd allergic mice. Furthermore, adoptive transfer experiments revealed that in vitro-cultured Pd-stimulated antigen presenting cells (APCs) function as memory APCs with recipient mice developing Pd allergy and that the frequency of TRAV7-2*02 increases the same as conventional Pd allergic mice. In contrast, neither proliferation of CD8+ T cells nor increasing of TRAV7-2*02 was observed in major histocompatibility complex I (MHC I)-deficient Pd-APCs transferred to mice. Taken together, we revealed that TRAV7-2*02-expressing CD8+ T cells are the pathogenic T cells for the development of Pd allergy. We also identified the CDR3 consensus motif of pathogenic TCRs as CAAXSGSWQLIF in TRAV7-2*02/TRAJ (TCRα junction)22*01 positive cells. These results suggest that the specific TCRs represent novel targets for the development of diagnostics and treatments for metal allergy.

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