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器官特异性自身免疫病患者的胰岛细胞抗体和胰岛素自身抗体。它们对1型(胰岛素依赖型)糖尿病发生发展的表现及预测价值。一项10年随访研究。

Islet cell and insulin autoantibodies in organ-specific autoimmune patients. Their behaviour and predictive value for the development of type 1 (insulin-dependent) diabetes mellitus. A 10-year follow-up study.

作者信息

Betterle C, Presotto F, Pedini B, Moro L, Slack R S, Zanette F, Zanchetta R

出版信息

Diabetologia. 1987 May;30(5):292-7. doi: 10.1007/BF00299020.

Abstract

To evaluate the behaviour and predictive value of islet cell and insulin autoantibodies in patients with organ-specific autoimmune diseases, we followed 21 non-diabetic subjects for a mean period of 84 +/- 27 months. Ten patients were persistently seropositive for complement-fixing islet cell antibodies and high titres of immunoglobulin G islet cell antibodies (greater than or equal to 1:8). The prevalence of persistent insulin autoantibodies in this group was 67%. Seven patients (70%) developed Type 1 (insulin-dependent) diabetes mellitus after a latency period of 2-60 months. The predictive value of complement-fixing islet cell antibodies was 65%, and in the presence of both complement-fixing islet cell and insulin autoantibodies the predictive value rose to 76%. Eleven patients were seronegative for complement-fixing islet cell antibodies and had low immunoglobulin G islet cell antibodies titres (less than 1:8) that were either persistent or transient, or that fluctuated during follow-up. The prevalence of persistent insulin autoantibodies in this group was 45%; only one subject developed Type 1 diabetes. The predictive value of persistent islet cell antibodies (complement-fixing positive/negative) was 54%, and it rose to 70% when both islet cell and insulin autoantibodies were present. Individuals with only insulin autoantibodies or immunoglobulin G islet cell antibodies did not develop diabetes mellitus. A high frequency of HLA-DR3 and/or DR4 was found in patients who developed diabetes mellitus. Thus, the presence of both islet cell and insulin autoantibodies in patients with organ-specific autoimmune disease appears to confer the highest risk of progression toward Type 1 diabetes.

摘要

为评估器官特异性自身免疫性疾病患者中胰岛细胞抗体和胰岛素自身抗体的行为及预测价值,我们对21名非糖尿病受试者进行了平均84±27个月的随访。10名患者补体结合胰岛细胞抗体和高滴度免疫球蛋白G胰岛细胞抗体(≥1:8)持续呈血清阳性。该组中持续性胰岛素自身抗体的患病率为67%。7名患者(70%)在2至60个月的潜伏期后发生了1型(胰岛素依赖型)糖尿病。补体结合胰岛细胞抗体的预测价值为65%,当同时存在补体结合胰岛细胞抗体和胰岛素自身抗体时,预测价值升至76%。11名患者补体结合胰岛细胞抗体呈血清阴性,免疫球蛋白G胰岛细胞抗体滴度较低(<1:8),这些滴度要么持续存在、要么短暂存在,要么在随访期间波动。该组中持续性胰岛素自身抗体的患病率为45%;只有1名受试者发生了1型糖尿病。持续性胰岛细胞抗体(补体结合阳性/阴性)的预测价值为54%,当同时存在胰岛细胞抗体和胰岛素自身抗体时,预测价值升至70%。仅具有胰岛素自身抗体或免疫球蛋白G胰岛细胞抗体的个体未发生糖尿病。在发生糖尿病的患者中发现HLA-DR3和/或DR4的频率较高。因此,器官特异性自身免疫性疾病患者中同时存在胰岛细胞抗体和胰岛素自身抗体似乎赋予了向1型糖尿病进展的最高风险。

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