Differential Immunogenetic Determinants of Polyclonal Insulin Autoimmune Syndrome (Hirata's Disease) and Monoclonal Insulin Autoimmune Syndrome

Author:

Uchigata Yasuko1,Tokunaga Katsushi2,Nepom Gerald3,Bannai Makoto4,Kuwata Shoji5,Dozio Nicoletta6,Benson Edward A7,Ronningen Kjersti S8,Spinas Glatgen A9,Tadokoro Kenji2,Hirata Yukimasa1,Juji Takeo2,Omori Yasue1

Affiliation:

1. Diabetes Center, Tokyo Women's Medical College, University of Tokyo Tokyo, Japan

2. Department of Research, Japanese Red Cross Central Blood Center, University of Tokyo Tokyo, Japan

3. Virginia Mason Research Center Seattle, Washington

4. Department of Research, Japanese Red Cross Tokyo Metropolitan Blood Center, University of Tokyo Tokyo, Japan

5. Department of Transfusion, Medicine and Immunohematology, Faculty of Medicine, University of Tokyo Tokyo, Japan

6. Department of Internal Medicine, Scientific Institute H San Raffaele Milan, Italy

7. Department of Medicine, Virginia Mason Clinic Seattle, Washington

8. Institute of Transplantation Immunology, The National Hospital Oslo, Norway

9. Division of Endocrinology and Metabolism, University Hospital Zurich, Switzerland

Abstract

The insulin autoimmune syndrome (IAS), or Hirata's disease, is characterized by the combination of fasting hypoglycemia, high concentration of total serum immunoreactive insulin, and presence of autoantibodies to native human insulin in serum. Autoantibody production is classified as monoclonal or polyclonal, with the majority of IAS cases classified as polyclonal. Previously, we observed a striking association between the human leukocyte antigen (HLA) class II alleles DRB1*0406/DQA1* 0301/DQB1*0302 and Japanese IAS patients with polyclonal insulin autoantibodies (IAAs) and T-cell recognition of human insulin in the context of DRB1*0406 molecules. Because of such a strong HLA association in IAS, we performed intra- and interethnic studies on IAS-associated DRB1 alleles and searched for the critical amino acid residue(s) for IAS pathogenesis. Glutamate at position 74 in the HLA-DR4 β1-chain was presumed to be essential to the production of polyclonal IAA in IAS, whereas alanine at the same position of the HLA-DR β1-chain might be important in the production of monoclonal IAA.

Publisher

American Diabetes Association

Subject

Endocrinology, Diabetes and Metabolism,Internal Medicine

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