Autoantibodies Directed Toward a Novel IA-2 Variant Protein Enhance Prediction of Type 1 Diabetes
Author(s) -
Maria Acevedo-Calado,
Susan L. Pietropaolo,
Michael P. Morran,
Santiago Schnell,
Andrew D. Vonberg,
Charles F. Verge,
Roberto Gianani,
Dorothy J. Becker,
Shuai Huang,
Carla J. Greenbaum,
Liping Yu,
Howard W. Davidson,
Aaron W. Michels,
Stephen S. Rich,
Massimo Pietropaolo
Publication year - 2019
Publication title -
diabetes
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.219
H-Index - 330
eISSN - 1939-327X
pISSN - 0012-1797
DOI - 10.2337/db18-1351
Subject(s) - autoantibody , type 2 diabetes , medicine , diabetes mellitus , type 1 diabetes , computational biology , immunology , antibody , biology , endocrinology
We identified autoantibodies (AAb) reacting with a variant IA-2 molecule (IA-2var) that has three amino acid substitutions (Cys 27 , Gly 608 , and Pro 671 ) within the full-length molecule. We examined IA-2var AAb in first-degree relatives of type 1 diabetes (T1D) probands from the TrialNet Pathway to Prevention Study. The presence of IA-2var-specific AAb in relatives was associated with accelerated progression to T1D in those positive for AAb to GAD65 and/or insulin but negative in the standard test for IA-2 AAb. Furthermore, relatives with single islet AAb (by traditional assays) and carrying both IA-2var AAb and the high-risk HLA-DRB1*04-DQB1*03:02 haplotype progress rapidly to onset of T1D. Molecular modeling of IA-2var predicts that the genomic variation that alters the three amino acids induces changes in the three-dimensional structure of the molecule, which may lead to epitope unmasking in the IA-2 extracellular domain. Our observations suggest that the presence of AAb to IA-2var would identify high-risk subjects who would benefit from participation in prevention trials who have one islet antibody by traditional testing and otherwise would be misclassified as "low risk" relatives.
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