The relationships between genetic markers and disease-associated autoantibodies were studied in an unselected population of 701 siblings of children with type 1 diabetes, and the predictive characteristics of these markers over a period of 9 years were determined. Increased prevalences of all the antibodies were closely associated with HLA identity to the index case, the DR4 and DQB1*0302 alleles, and the DR3/4 phenotype and the DQB1*02/0302 genotype. Antibodies to GAD (GADA) were also associated with the DR3 and DQB1*02 alleles. Siblings carrying the protective DR2 and DQB1*0602-3 alleles were characterized by lower frequencies of islet cell antibodies (ICA), antibodies to IA-2 (IA-2A), and GADA. Higher levels of ICA were related to HLA identity, the DR4 and DQB1*0302 alleles, and the susceptible DQB1 genotypes, while no significant differences were observed in the levels of IA-2A, GADA, or insulin autoantibodies among siblings with different HLA risk markers. The DR2 or DQB1*0602-3 alleles were not related to the levels of any antibody specificity. A combination of the genetic markers and autoantibodies increased the positive predictive values of all autoantibodies substantially, which may have clinical implications when evaluating the risk of developing type 1 diabetes at the individual level or when recruiting high-risk individuals for intervention trials. However, because such combinations also resulted in reduced sensitivity, autoantibodies alone rather than in combination with genetic markers are recommended as the first-line screening in siblings. Finally, not all siblings with a broad humoral autoimmune response or high-risk genetic markers present with type 1 diabetes, while some with a low genetic risk and weak initial signs of humoral autoimmunity may progress to disease.
Abstract|
January 01 2000
Genetic markers, humoral autoimmunity, and prediction of type 1 diabetes in siblings of affected children. Childhood Diabetes in Finland Study Group.
P Kulmala;
P Kulmala
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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K Savola;
K Savola
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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H Reijonen;
H Reijonen
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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R Veijola;
R Veijola
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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P Vähäsalo;
P Vähäsalo
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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J Karjalainen;
J Karjalainen
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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E Tuomilehto-Wolf;
E Tuomilehto-Wolf
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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J Ilonen;
J Ilonen
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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J Tuomilehto;
J Tuomilehto
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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H K Akerblom;
H K Akerblom
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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M Knip
M Knip
Department of Pediatrics, University of Oulu, Finland. petri.kulmala@oulu.fi
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Citation
P Kulmala, K Savola, H Reijonen, R Veijola, P Vähäsalo, J Karjalainen, E Tuomilehto-Wolf, J Ilonen, J Tuomilehto, H K Akerblom, M Knip; Genetic markers, humoral autoimmunity, and prediction of type 1 diabetes in siblings of affected children. Childhood Diabetes in Finland Study Group.. Diabetes 1 January 2000; 49 (1): 48–58. https://doi.org/10.2337/diabetes.49.1.48
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