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Contributions of the N-terminal flanking residues of an antigenic peptide from the Japanese cedar pollen allergen Cry j 1 to the T-cell activation by HLA-DP5.

Authors :
Kusano, Seisuke
Ueda, Sho
Oryoji, Daisuke
Toyoumi, Aya
Hashimoto-Tane, Akiko
Kishi, Hiroyuki
Hamana, Hiroshi
Muraguchi, Atsushi
Jin, Hui
Arase, Hisashi
Miyadera, Hiroko
Kishikawa, Reiko
Yoshikai, Yasunobu
Yamada, Hisakata
Yamamoto, Ken
Nishimura, Yasuharu
Saito, Takashi
Sasazuki, Takehiko
Yokoyama, Shigeyuki
Source :
International Immunology. Sep2023, Vol. 35 Issue 9, p447-458. 12p.
Publication Year :
2023

Abstract

Cry j 1 is a major allergen present in Japanese cedar (Cryptomeria japonica) pollens. Peptides with the core sequence of KVTVAFNQF from Cry j 1 ('pCj1') bind to HLA-DP5 and activate Th2 cells. In this study, we noticed that Ser and Lys at positions −2 and −3, respectively, in the N-terminal flanking (NF) region to pCj1 are conserved well in HLA-DP5-binding allergen peptides. A competitive binding assay showed that the double mutation of Ser(–2) and Lys(–3) to Glu [S(P–2)E/K(P–3)E] in a 13-residue Cry j 1 peptide (NF-pCj1) decreased its affinity for HLA-DP5 by about 2-fold. Similarly, this double mutation reduced, by about 2-fold, the amount of NF-pCj1 presented on the surface of mouse antigen-presenting dendritic cell line 1 (mDC1) cells stably expressing HLA-DP5. We established NF-pCj1-specific and HLA-DP5-restricted CD4+ T-cell clones from HLA-DP5 positive cedar pollinosis (CP) patients, and analyzed their IL-2 production due to the activation of mouse TG40 cells expressing the cloned T-cell receptor by the NF-pCj1-presenting mDC1 cells. The T-cell activation was actually decreased by the S(P–2)E/K(P–3)E mutation, corresponding to the reduction in the peptide presentation by this mutation. In contrast, the affinity of NF-pCj1·HLA-DP5 for the T-cell receptor was not affected by the S(P–2)E/K(P–3)E mutation, as analyzed by surface plasmon resonance. Considering the positional and side-chain differences of these NF residues from previously reported T-cell activating sequences, the mechanisms of enhanced T-cell activation by Ser(–2) and Lys(–3) of NF-pCj1 may be novel. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
09538178
Volume :
35
Issue :
9
Database :
Academic Search Index
Journal :
International Immunology
Publication Type :
Academic Journal
Accession number :
171918968
Full Text :
https://doi.org/10.1093/intimm/dxad024