Basu Ananda, Service F John, Yu Liping, Heser Don, Ferries Laura M, Eisenbarth George
Division of Endocrinology, Department of Internal Medicine, Mayo Clinic, Rochester, Minnesota 55905, USA.
Endocr Pract. 2005 Mar-Apr;11(2):97-103. doi: 10.4158/EP.11.2.97.
To report the clinical, biochemical, and immunologic characteristics of 7 white patients with the rare disorder of hyperinsulinemic hypoglycemia in association with spontaneously generated high titers of antibodies to human insulin.
We reviewed the clinical data, history, and symptoms of the 7 study patients and summarized the biochemical findings during a spontaneous episode of hypoglycemia. Insulin antibody binding was measured in all patients, and antibody affinity, capacity, and clonality were analyzed in 4. A mixed meal study was conducted in 2 patients. A potential mechanism for postprandial hypoglycemia is presented.
In all 7 patients (6 women and 1 man), symptoms were neuroglycopenic, occurring primarily postprandially but during fasting in some patients. During hypoglycemia, concentrations of insulin, proinsulin, and, in most patients, C peptide considerably exceeded those observed in patients with insulinoma. These concentrations were spuriously elevated as a result of interference by the autoantibodies in the immunoassays. No patient had evidence of an insulinoma on various radiologic localization procedures directed at the pancreas. Insulin antibodies showed a high percentage of binding to human insulin--50 to 90%. Heterogeneity of antibodies regarding clonality and antibody binding sites was noted; some patients had polyclonal and some had monoclonal IgG class antibodies. Most patients had two categories of binding sites: high affinity/low capacity and low capacity/high affinity. Although the mechanism for postprandial hypoglycemia remains conjectural, prolonged elevations of postprandial concentrations of total and free insulin are consistent with the putative mechanism of a buffering effect of insulin antibodies.
Insulin autoimmune hypoglycemia, although rare in any racial group and especially in white subjects, can be readily detected by high titers of insulin antibodies. Such a determination should be done in all patients undergoing evaluation for hypoglycemia.
报告7例患有高胰岛素血症性低血糖罕见疾病并伴有自发产生高滴度人胰岛素抗体的白人患者的临床、生化和免疫学特征。
我们回顾了7例研究患者的临床资料、病史和症状,并总结了低血糖自发发作期间的生化检查结果。对所有患者测量胰岛素抗体结合情况,对4例患者分析抗体亲和力、容量和克隆性。对2例患者进行了混合餐试验。提出了餐后低血糖的一种潜在机制。
所有7例患者(6例女性和1例男性)均有神经低血糖症状,主要发生在餐后,但部分患者在空腹时也会出现。低血糖期间,胰岛素、胰岛素原浓度,以及大多数患者的C肽浓度大大超过胰岛素瘤患者中观察到的浓度。由于自身抗体在免疫测定中的干扰,这些浓度被假性升高。在针对胰腺的各种放射学定位检查中,没有患者有胰岛素瘤的证据。胰岛素抗体与人胰岛素的结合率很高,为50%至90%。注意到抗体在克隆性和抗体结合位点方面存在异质性;一些患者有多克隆IgG类抗体,一些患者有单克隆IgG类抗体。大多数患者有两类结合位点:高亲和力/低容量和低容量/高亲和力。虽然餐后低血糖的机制仍属推测,但餐后总胰岛素和游离胰岛素浓度的长期升高与胰岛素抗体缓冲作用的假定机制一致。
胰岛素自身免疫性低血糖在任何种族群体中都很罕见,在白人中尤为罕见,但通过高滴度的胰岛素抗体很容易检测到。对所有接受低血糖评估的患者都应进行这样的检测。
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