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糖尿病患者中的胰岛素抗体与低血糖。抗体结合的定量分析能否预测低血糖风险?

Insulin antibodies and hypoglycemia in diabetic patients. Can a quantitative analysis of antibody binding predict the risk of hypoglycemia?

作者信息

Kim M R, Sheeler L R, Mansharamani N, Haug M T, Faiman C, Gupta M K

机构信息

Department of Endocrinology, Cleveland Clinic Foundation, OH, USA.

出版信息

Endocrine. 1997 Jun;6(3):285-91. doi: 10.1007/BF02820505.

Abstract

We report a noninsulin-dependent diabetes mellitus (NIDDM) patient with spontaneous, severe hypoglycemic reactions and the presence of insulin antibodies. He had a remote antecedent history of beef-pork insulin therapy as well as exposure to hydralazine. Detailed insulin binding kinetic studies were performed in this patient as well as in six other insulin-treated diabetic patients with anti-insulin antibodies (three with and three without an obvious cause of hypoglycemia). Sera from the current patient and five of the six other diabetic patients (one NIDDM, four IDDM) revealed two types of binding sites: high-affinity with low capacity (Kd, 0.4-12.4 x 10(-9) mol/L; binding capacity, 0.6-659 mU/L) and low-affinity with high capacity (Kd, 0.3 to 35.7 x 10(-7) mol/L; binding capacity; 202-113,680 mU/L). One NIDDM patient had only high-affinity antibodies (Kd, 22.9 x 10(-9) mol/L; binding capacity of 78 mU/L). Type of diabetes mellitus, insulin antibody titers or their binding capacities, insulin levels (total, bound, or free), and bioavailable insulin were not related to hypoglycemic reactions. Two calculated values by the method described tended to discriminate patients with and without hypoglycemia. The calculated amount of low-affinity antibody bound insulin ranged from 69.4-2090 mU/L vs < 4-70.6 mU/L in patients with and without hypoglycemia, respectively. The best discrimination was afford by the percent saturation of low-affinity binding sites; values were clearly higher in the patients with hypoglycemia (2.5-34.4%) than in those without hypoglycemia (not detectable, 0.06, 0.15%). Consideration of the possible drug-associated insulin antibody formation in insulin-treated diabetics and the novel quantitative analysis of the antibody binding kinetics should prove helpful in evaluating patients with high insulin antibody titers and assessing the risk of hypoglycemia.

摘要

我们报告了一名非胰岛素依赖型糖尿病(NIDDM)患者,该患者出现自发性严重低血糖反应且存在胰岛素抗体。他既往有使用牛-猪胰岛素治疗以及接触肼苯哒嗪的病史。对该患者以及另外六名接受胰岛素治疗且伴有抗胰岛素抗体的糖尿病患者(三名有低血糖明显病因,三名无)进行了详细的胰岛素结合动力学研究。该患者以及另外六名糖尿病患者中的五名(一名NIDDM,四名IDDM)的血清显示出两种结合位点:高亲和力低容量(解离常数Kd,0.4 - 12.4×10⁻⁹mol/L;结合容量,0.6 - 659mU/L)和低亲和力高容量(Kd,0.3至35.7×10⁻⁷mol/L;结合容量;202 - 113,680mU/L)。一名NIDDM患者仅具有高亲和力抗体(Kd,22.9×10⁻⁹mol/L;结合容量为78mU/L)。糖尿病类型、胰岛素抗体滴度或其结合容量、胰岛素水平(总胰岛素、结合胰岛素或游离胰岛素)以及生物可利用胰岛素与低血糖反应无关。通过所述方法计算的两个值倾向于区分有和无低血糖的患者。有和无低血糖患者中,低亲和力抗体结合胰岛素的计算量分别为69.4 - 2090mU/L和<4 - 70.6mU/L。低亲和力结合位点的饱和百分比提供了最佳区分度;低血糖患者的值(2.5 - 34.4%)明显高于无低血糖患者(未检测到、0.06、0.15%)。考虑胰岛素治疗的糖尿病患者中可能与药物相关的胰岛素抗体形成以及抗体结合动力学的新型定量分析,应有助于评估胰岛素抗体滴度高的患者并评估低血糖风险。

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