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Original Articles

Organ-Specific Autoimmunity and HLA-DR Antigens as Markers for β-Cell Destruction in Patients With Type II Diabetes

  1. Leif Groop,
  2. Aaro Miettinen,
  3. Per-Henrik Groop,
  4. Seppo Meri,
  5. Saija Koskimies and
  6. Gian Franco Bottazzo
  1. Fourth Department of Medicine, Helsinki University Central Hospital London, United Kingdom
  2. Department of Bacteriology and Immunology, University of Helsinki London, United Kingdom
  3. Finnish Red Cross Blood Transfusion Service Helsinki, Finland
  4. Department of Immunology, Middlesex Hospital Medical School London, United Kingdom
  1. Address correspondence and reprint requests to Leif C. Groop, MD, Fourth Department of Medicine, Helsinki University Central Hospital, Unioninkatu 38, SF-00170 Helsinki, Finland.
Diabetes 1988 Jan; 37(1): 99-103. https://doi.org/10.2337/diab.37.1.99
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Abstract

Islet cell antibodies (ICAs), thyrogastric antibodies, and HLA-DR antigens were determined in 204 patients with type II (non-insulin-dependent) diabetes controlled with diet and/or oral hypoglycemic agents (NIR) and in 108 age-matched patients who required insulin to control their hyperglycemia (IR). β-Cell function measured as C-peptide response to glucagon was evaluated in relation to the presence of ICAs and HLA-DR antigens. The IR patients differed from the NIR patients with respect to higher frequency of ICAs (P < .001), thyroid antibodies (P < .02), and the HLA antigen DR4 (P < .02). The highest frequency of ICAs and thyroid antibodies was observed in female insulin-treated subjects (51.2 and 46.4%). Patients who were heterozygous for HLA-DR3/DR4 showed significantly higher frequency of ICAs (P < .01) and complement-fixing ICAs (P < .001) than patients without the heterozygous form DR3/DR4. Neither the presence of ICA alone nor DR3/DR4 alone was associated with a significant impairment of β-cell function. However, when both ICA and DR3/DR4 were present in a diabetic individual, β-cell function was markedly impaired (P < .001), suggesting that both genetic and autoimmune factors are necessary to facilitate the process leading to β-cell destruction of the patients. Our findings suggest that type II diabetes is a heterogeneous disorder including at least two major subgroups, which can be further characterized by HLA-DR antigens and organ-specific antibodies

  • Received January 15, 1987.
  • Revision received May 18, 1987.
  • Accepted May 18, 1987.
  • Copyright © 1988 by the American Diabetes Association

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January 1988, 37(1)
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Organ-Specific Autoimmunity and HLA-DR Antigens as Markers for β-Cell Destruction in Patients With Type II Diabetes
Leif Groop, Aaro Miettinen, Per-Henrik Groop, Seppo Meri, Saija Koskimies, Gian Franco Bottazzo
Diabetes Jan 1988, 37 (1) 99-103; DOI: 10.2337/diab.37.1.99

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Organ-Specific Autoimmunity and HLA-DR Antigens as Markers for β-Cell Destruction in Patients With Type II Diabetes
Leif Groop, Aaro Miettinen, Per-Henrik Groop, Seppo Meri, Saija Koskimies, Gian Franco Bottazzo
Diabetes Jan 1988, 37 (1) 99-103; DOI: 10.2337/diab.37.1.99
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