Publication
Title
Combined positivity for HLA DQ2/DQ8 and IA-2 antibodies defines population at high risk of developing type 1 diabetes
Author
Institution/Organisation
Belgian Diabet Registry
Abstract
Aims/hypothesis: Prevention trials in first-degree relatives of type 1 diabetic patients are hampered by large interindividual differences in progression rate to diabetes. We investigated whether specific combinations of immune and genetic markers can identify subgroups with more homogeneous progression to clinical onset. Methods: Antibodies against islet cell cytoplasm (ICA), insulin (IAA), glutamate decarboxylase (GADA) and IA-2 protein (IA2A) were measured in 790 non-diabetic control subjects and 4,589 first-degree relatives under age 40. Results: On first sampling, 11.1% of the siblings presented at least one antibody type ( p< 0.001 vs other relatives). During follow-up ( median 52 months) 43 subjects developed type 1 diabetes ( 31 siblings, ten offspring of a diabetic father, two offspring of a diabetic mother). Using Kaplan - Meier survival analysis and Cox regression, IA-2A conferred the highest 5-year diabetes risk (> 50%) irrespective of the number of antibodies present. In initially IA-2A-positive relatives (n = 58) progression to hyperglycaemia depended more on HLA DQ status than on type of kinship (84% progression in the presence of DQ2/DQ8 vs 32% in its absence; p< 0.003). In IA-2A-negative relatives (n = 4,531) 5-year progression to diabetes increased with the number of other antibodies (ICA, GADA and/or IAA) ( p< 0.001) but overall did not exceed 10% even for two or more antibodies. Among relatives initially positive for one or more antibody type other than IA-2A (n = 315), there was significantly more progression to diabetes ( overall still < 10%) in carriers of DQ2 ( p< 0.001 vs no DQ2), regardless of DQ8 status. Conclusions/interpretation: These observations suggest that the HLA-DQ-inferred risk of diabetes can proceed through two distinct pathways distinguished by IA-2A status. Combined positivity for DQ2/DQ8 and IA-2A defines a more homogeneous high-risk population for prevention trials than those used so far.
Language
English
Source (journal)
Diabetologia / European Association for the Study of Diabetes. - Berlin, 1965, currens
Publication
Berlin : 2005
ISSN
0012-186X [print]
1432-0428 [online]
Volume/pages
48:4(2005), p. 687-694
ISI
000228515900014
Full text (Publisher's DOI)
Full text (publisher's version - intranet only)
UAntwerpen
Faculty/Department
Research group
Publication type
Subject
Affiliation
Publications with a UAntwerp address
External links
Web of Science
Record
Identification
Creation 03.01.2013
Last edited 20.09.2017
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