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儿童1型糖尿病诊断后第一年预测残余β细胞功能的因素。

Factors predicting residual beta-cell function in the first year after diagnosis of childhood type 1 diabetes.

作者信息

Couper J J, Hudson I, Werther G A, Warne G L, Court J M, Harrison L C

机构信息

Department of Endocrinology and Diabetes, Royal Children's Hospital, Parkville, Victoria, Australia.

出版信息

Diabetes Res Clin Pract. 1991 Jan;11(1):9-16. doi: 10.1016/0168-8227(91)90135-z.

Abstract

Twenty-five children aged 2-14 years (mean age 8.39 +/- 0.78 years) were studied prospectively during the first year after the diagnosis of type 1 diabetes. Of their clinical and metabolic features at diagnosis, only age showed a significant independent relationship with endogenous C-peptide production during the first year. Age was correlated with higher values for basal and stimulated plasma C-peptide at 7-14 days after diagnosis, at 6 months and at 12 months. At diagnosis, age was also associated with a higher value for HbA1c and a lower prevalence of insulin antibodies. C-peptide production peaked at 3 months and thereafter declined. Mean HbA1c and insulin requirement were both minimal at 6 months. At diagnosis, there were significant inverse relationships between basal C-peptide production and both insulin dose and HbA1c and between stimulated C-peptide production and HbA1c. Basal and stimulated C-peptide production were inversely related to insulin dose at 6 and 12 months. Stimulated C-peptide was higher at 12 months in children retaining islet cell antibodies. These findings confirm the importance of age as a predictor of residual beta-cell function in type 1 diabetes and indicate that older children present clinically following a slower course of beta cell destruction.

摘要

对25名年龄在2至14岁(平均年龄8.39±0.78岁)的儿童在1型糖尿病确诊后的第一年进行了前瞻性研究。在确诊时的临床和代谢特征中,只有年龄与第一年的内源性C肽产生存在显著的独立关系。年龄与确诊后7至14天、6个月和12个月时基础和刺激后血浆C肽的较高值相关。确诊时,年龄还与较高的糖化血红蛋白(HbA1c)值和较低的胰岛素抗体患病率相关。C肽产生在3个月时达到峰值,此后下降。平均HbA1c和胰岛素需求量在6个月时均最低。确诊时,基础C肽产生与胰岛素剂量和HbA1c之间以及刺激后C肽产生与HbA1c之间均存在显著的负相关。基础和刺激后C肽产生在6个月和12个月时与胰岛素剂量呈负相关。在保留胰岛细胞抗体的儿童中,12个月时刺激后C肽较高。这些发现证实了年龄作为1型糖尿病残余β细胞功能预测指标的重要性,并表明年龄较大的儿童在临床上β细胞破坏进程较慢。

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