Anti‐GAD65 autoantibody in Taiwanese patients with insulin‐dependent diabetes mellitus: effect of HLA on anti‐GAD65 positivity and clinical characteristics

Abstract

OBJECTIVE Anti-GAD₆₅ antibody has been studied widely in patients with insulin-dependent diabetes mellitus (IDDM) in many different populations. However, the prevalence of GAD₆₅ autoantibody has not been assessed in Taiwanese patients with IDDM. We therefore characterized GAD₆₅ antibody and investigated the effect of HLA-DR phenotypes on GAD₆₅ autoimmunity and other clinical characteristics in Taiwanese subjects with IDDM. SUBJECTS AND MEASUREMENTS Two hundred and twenty-five patients (male 102, female 123) with IDDM were recruited. The diagnostic criteria for IDDM were age of onset before 30 years, presence of diabetic ketoacidosis, and insulin-dependency within 3 years of onset. We employed a radioligand method to detect GAD₆₅ antibody. HLA-DR typing was performed by the PCR-SSO techniques. Plasma C-peptide and antithyroid microsomal antibody were also measured. RESULTS The prevalence of GAD₆₅ antibody according to duration of disease were 50/91 (54.9%), 37/95 (38.9%), 8/24 (33%), and 3/15 (20%) among the groups of duration ≤5, 6–10, 11–15, and >15 years, respectively (p = 0.0011). There were no significant differences between GAD(+) and GAD(−) patients in age of onset (11.5 ± 6.5 and 11.6 ± 13.4 years, respectively), gender distribution (male:female 39:59 and 58:69, respectively) and percentage with residual β cell function (38.8% and 29.1%, respectively). Multiple regression analysis revealed that duration of IDDM correlated inversely with residual β cell function. Earlier onset of IDDM correlated with a loss of β cell function and a HLA-DR phenotype containing DR3/4, DR3/3 or DR3/9. CONCLUSIONS Prevalence of GAD₆₅ autoantibody among Taiwanese subjects with IDDM was negatively correlated with duration of disease. Different determinants in the HLA-DR locus contributed to the clinical onset of IDDM but not to GAD autoimmunity.