Islet Autoimmunity and HLA Markers of Presymptomatic and Clinical Type 1 Diabetes: Joint Analyses of Prospective Cohort Studies in Finland, Germany, Sweden, and the U.S.

Author:

Anand Vibha1ORCID,Li Ying1,Liu Bin1,Ghalwash Mohamed12,Koski Eileen1,Ng Kenney1,Dunne Jessica L.3,Jönsson Josefine4,Winkler Christiane567,Knip Mikael891011ORCID,Toppari Jorma12,Ilonen Jorma13,Killian Michael B.14,Frohnert Brigitte I.15ORCID,Lundgren Markus5,Ziegler Anette-Gabriele567ORCID,Hagopian William14ORCID,Veijola Riitta16,Rewers Marian15

Affiliation:

1. Center for Computational Health, IBM T.J. Watson Research Center

2. Ain Shams University, Cairo, Egypt

3. JDRF, New York, NY

4. Department of Clinical Sciences Malmö, Lund University/CRC, Skåne University Hospital, Malmö

5. Institute of Diabetes Research, Helmholtz Zentrum München German Research Center for Environmental Health, Munich-Neuherberg, Germany

6. Forschergruppe Diabetes e.V. am Helmholtz Zentrum München, Munich, Germany

7. Forschergruppe Diabetes, Technical University Munich, Germany

8. Tampere Center for Child Health Research, Tampere University Hospital, Tampere, Finland

9. Pediatric Research Center, Children's Hospital, University of Helsinki and Helsinki University Hospital, Helsinki, Finland

10. Research Program for Clinical and Molecular Metabolism, Faculty of Medicine, University of Helsinki, Helsinki, Finland

11. Folkhälsan Research Center, Helsinki, Finland

12. Institute of Biomedicine and Population Research Centre, University of Turku, and Department of Pediatrics, Turku University Hospital, Turku, Finland

13. Immunogenetics Laboratory, Institute of Biomedicine, University of Turku, and Clinical Microbiology, Turku University Hospital, Turku, Finland

14. Pacific Northwest Research Institute, Seattle, WA

15. Barbara Davis Center for Diabetes, University of Colorado, Denver, CO

16. PEDEGO Research Unit, Department of Pediatrics, University of Oulu and Oulu University Hospital, Oulu, Finland

Abstract

OBJECTIVE To combine prospective cohort studies, by including HLA harmonization, and estimate risk of islet autoimmunity and progression to clinical diabetes. RESEARCH DESIGN AND METHODS For prospective cohorts in Finland, Germany, Sweden, and the U.S., 24,662 children at increased genetic risk for development of islet autoantibodies and type 1 diabetes have been followed. Following harmonization, the outcomes were analyzed in 16,709 infants-toddlers enrolled by age 2.5 years. RESULTS In the infant-toddler cohort, 1,413 (8.5%) developed at least one autoantibody confirmed at two or more consecutive visits (seroconversion), 865 (5%) developed multiple autoantibodies, and 655 (4%) progressed to diabetes. The 15-year cumulative incidence of diabetes varied in children with one, two, or three autoantibodies at seroconversion: 45% (95% CI 40–52), 85% (78–90), and 92% (85–97), respectively. Among those with a single autoantibody, status 2 years after seroconversion predicted diabetes risk: 12% (10–25) if reverting to autoantibody negative, 30% (20–40) if retaining a single autoantibody, and 82% (80–95) if developing multiple autoantibodies. HLA-DR-DQ affected the risk of confirmed seroconversion and progression to diabetes in children with stable single-autoantibody status. Their 15-year diabetes incidence for higher- versus lower-risk genotypes was 40% (28–50) vs. 12% (5–38). The rate of progression to diabetes was inversely related to age at development of multiple autoantibodies, ranging from 20% per year to 6% per year in children developing multipositivity in ≤2 years or >7.4 years, respectively. CONCLUSIONS The number of islet autoantibodies at seroconversion reliably predicts 15-year type 1 diabetes risk. In children retaining a single autoantibody, HLA-DR-DQ genotypes can further refine risk of progression.

Publisher

American Diabetes Association

Subject

Advanced and Specialized Nursing,Endocrinology, Diabetes and Metabolism,Internal Medicine

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