作者
Mubarak Almutairi, Adam Lister, Qing Zhao, James Line, Kareena Adair, Arun Tailor, James Waddington, Elsie Clarke, Joshua Gardner, Paul Thomson, Nicolas Harper, Yonghu Sun, Lele Sun, David A Ostrov, Hong Liu, David J MacEwan, Munir Pirmohamed, Xiaoli Meng, Furen Zhang, Dean J Naisbitt
发表日期
2023/4/15
期刊
The Journal of Immunology
卷号
210
期号
8
页码范围
1031-1042
出版商
AAI
简介
Previous studies have shown that cysteine-reactive drug metabolites bind covalently with protein to activate patient T cells. However, the nature of the antigenic determinants that interact with HLA and whether T cell stimulatory peptides contain the bound drug metabolite has not been defined. Because susceptibility to dapsone hypersensitivity is associated with the expression of HLA-B*13:01, we have designed and synthesized nitroso dapsone–modified, HLA-B*13:01 binding peptides and explored their immunogenicity using T cells from hypersensitive human patients. Cysteine-containing 9-mer peptides with high binding affinity to HLA-B*13:01 were designed (AQDCEAAAL [Pep1], AQDACEAAL [Pep2], and AQDAEACAL [Pep3]), and the cysteine residue was modified with nitroso dapsone. CD8+ T cell clones were generated and characterized in terms of phenotype, function, and cross-reactivity …
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