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Characterizations of a neutralizing antibody broadly reactive to multiple gluten peptide:HLA-DQ2.5 complexes in the context of celiac disease

Authors :
Yuu Okura
Yuri Ikawa-Teranishi
Akihiko Mizoroki
Noriyuki Takahashi
Takashi Tsushima
Machiko Irie
Zulkarnain Harfuddin
Momoko Miura-Okuda
Shunsuke Ito
Genki Nakamura
Hiroaki Takesue
Yui Ozono
Masamichi Nishihara
Kenta Yamada
Siok Wan Gan
Akira Hayasaka
Shinya Ishii
Tetsuya Wakabayashi
Masaru Muraoka
Nishiki Nagaya
Hiroshi Hino
Takayuki Nemoto
Taichi Kuramochi
Takuya Torizawa
Hideaki Shimada
Takehisa Kitazawa
Makoto Okazaki
Junichi Nezu
Ludvig M. Sollid
Tomoyuki Igawa
Source :
Nature Communications, Vol 14, Iss 1, Pp 1-15 (2023)
Publication Year :
2023
Publisher :
Nature Portfolio, 2023.

Abstract

Abstract In human celiac disease (CeD) HLA-DQ2.5 presents gluten peptides to antigen-specific CD4+ T cells, thereby instigating immune activation and enteropathy. Targeting HLA-DQ2.5 with neutralizing antibody for treating CeD may be plausible, yet using pan-HLA-DQ antibody risks affecting systemic immunity, while targeting selected gluten peptide:HLA-DQ2.5 complex (pHLA-DQ2.5) may be insufficient. Here we generate a TCR-like, neutralizing antibody (DONQ52) that broadly recognizes more than twenty-five distinct gluten pHLA-DQ2.5 through rabbit immunization with multi-epitope gluten pHLA-DQ2.5 and multidimensional optimization. Structural analyses show that the proline-rich and glutamine-rich motif of gluten epitopes critical for pathogenesis is flexibly recognized by multiple tyrosine residues present in the antibody paratope, implicating the mechanisms for the broad reactivity. In HLA-DQ2.5 transgenic mice, DONQ52 demonstrates favorable pharmacokinetics with high subcutaneous bioavailability, and blocks immunity to gluten while not affecting systemic immunity. Our results thus provide a rationale for clinical testing of DONQ52 in CeD.

Subjects

Subjects :
Science

Details

Language :
English
ISSN :
20411723
Volume :
14
Issue :
1
Database :
Directory of Open Access Journals
Journal :
Nature Communications
Publication Type :
Academic Journal
Accession number :
edsdoj.bd4902c569894da788e57ae0094f2b7a
Document Type :
article
Full Text :
https://doi.org/10.1038/s41467-023-44083-4
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