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儿童糖尿病中胰岛细胞胞浆抗体的临床病程及特征

Clinical time-course and characteristics of islet cell cytoplasmatic antibodies in childhood diabetes.

作者信息

Bruining G J, Molenaar J, Tuk C W, Lindeman J, Bruining H A, Marner B

出版信息

Diabetologia. 1984 Jan;26(1):24-9. doi: 10.1007/BF00252258.

Abstract

Circulating islet cell antibodies (ICA) were present in high frequency (80%) early after diagnosis and decreased in the time course of childhood diabetes mellitus. The complement fixing ability of islet cell antibodies (CF-ICA) in the course of the disease appeared to depend on the titre of ICA: the coefficient of correlation between ICA and CF-ICA titres was 0.79 and all ICA's with a titre over 16 were complement-fixing. Incubating fresh frozen human pancreatic sections thrice rather than once with the children's sera, increased the detectability of complement fixation by a factor 1.4 in all ICA-positive sera. Thus tested, the detection of complement fixation per se did not appear to have a separate pathogenic significance, as the fraction of complement fixing ICA's was almost constant throughout the clinical course. The presence of ICA-IgG subclasses also was dependent on the ICA titre: above a titre of 16 mostly all four subclasses could be detected. Incubating the pancreatic tissue thrice rather than once with ICA-positive sera resulted in enhanced detectability of ICA-IgG1. Early in the course of childhood diabetes, including two prediabetic children, most of the IgG subclasses could be detected in ICA, but after a duration of one year IgG1 alone was mainly seen. In two other children, having a family history of insulin-dependency, restriction to the IgG2 subclass was found.

摘要

循环胰岛细胞抗体(ICA)在诊断后早期出现的频率较高(80%),并在儿童糖尿病病程中逐渐减少。胰岛细胞抗体的补体结合能力(CF-ICA)在疾病过程中似乎取决于ICA的滴度:ICA与CF-ICA滴度之间的相关系数为0.79,所有滴度超过16的ICA均具有补体结合能力。用患儿血清对新鲜冷冻的人胰腺切片进行三次而非一次孵育,可使所有ICA阳性血清中补体结合的可检测性提高1.4倍。经如此检测,补体结合本身的检测似乎没有独立的致病意义,因为在整个临床过程中,具有补体结合能力的ICA比例几乎恒定。ICA-IgG亚类的存在也取决于ICA滴度:滴度高于16时,大多可检测到所有四个亚类。用ICA阳性血清对胰腺组织进行三次而非一次孵育,可提高ICA-IgG1的可检测性。在儿童糖尿病病程早期,包括两名糖尿病前期儿童,在ICA中大多可检测到大部分IgG亚类,但病程一年后,主要只能见到IgG1。在另外两名有胰岛素依赖家族史的儿童中,发现仅局限于IgG2亚类。

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