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1型糖尿病患者β细胞存活预测因素的前瞻性研究。

Prospective study of predictors of beta-cell survival in type I diabetes.

作者信息

Schiffrin A, Suissa S, Poussier P, Guttmann R, Weitzner G

机构信息

Department of Pediatrics, Montreal Children's Hospital-McGill University Research Institute, Quebec, Canada.

出版信息

Diabetes. 1988 Jul;37(7):920-5. doi: 10.2337/diab.37.7.920.

Abstract

We conducted a prospective study to describe the course of the pancreatic beta-cell function from the time of clinical diagnosis of insulin-dependent (type I) diabetes to determine whether DR type, presence of islet cell antibodies (ICA), presence of insulin antibodies (IA), age at onset, and sex could help in the prediction of residual endogenous insulin secretion. A cohort of 68 children was followed for 18 mo after diagnosis of type I diabetes. The outcome variables selected for analysis were 1) serum C-peptide peak concentration after a Sustacal meal, 2) time of disappearance of the serum C-peptide response, and 3) time after diagnosis at which the maximal serum C-peptide response was observed. After institution of insulin therapy, serum C-peptide peak concentrations rose temporarily for 1-6 mo and declined thereafter. Multivariate analysis of the data showed that DR type (P = .2488) and presence of IA (P = .1604) had no effect on serum C-peptide over time, but sex (P = .0146), age at onset (P = .0002), and presence of ICA (P = .0147) significantly contributed to the variation of serum C-peptide over time. Furthermore, age at onset, presence of ICA, and sex were also the only significant predictors of the time of disappearance of the beta-cell function. The relative risks of beta-cell-function disappearance were 0.87 (P = .0015), 9.43 (P = .0181), and 2.25 (P = .0468), respectively. In conclusion, there are distinct variations in the natural course of the beta-cell function in type I diabetes. beta-Cell-function survival is significantly shortened the younger the subject is at disease onset, if ICA are present at diagnosis, and if the subject is male.

摘要

我们进行了一项前瞻性研究,以描述从胰岛素依赖型(I型)糖尿病临床诊断时起胰腺β细胞功能的变化过程,从而确定糖尿病视网膜病变(DR)类型、胰岛细胞抗体(ICA)的存在、胰岛素抗体(IA)的存在、发病年龄和性别是否有助于预测残余内源性胰岛素分泌。68名儿童在被诊断为I型糖尿病后随访了18个月。选择用于分析的结局变量为:1)服用苏达卡尔餐(Sustacal meal)后血清C肽峰值浓度;2)血清C肽反应消失时间;3)诊断后观察到最大血清C肽反应的时间。开始胰岛素治疗后,血清C肽峰值浓度暂时升高1 - 6个月,此后下降。对数据的多变量分析表明,DR类型(P = 0.2488)和IA的存在(P = 0.1604)对血清C肽随时间的变化没有影响,但性别(P = 0.0146)、发病年龄(P = 0.0002)和ICA的存在(P = 0.0147)对血清C肽随时间的变化有显著影响。此外,发病年龄、ICA的存在和性别也是β细胞功能消失时间的唯一显著预测因素。β细胞功能消失的相对风险分别为0.87(P = 0.0015)、9.43(P = 0.0181)和2.25(P = 0.0468)。总之,I型糖尿病β细胞功能的自然病程存在明显差异。如果发病时年龄较小、诊断时存在ICA以及受试者为男性,β细胞功能的存活时间会显著缩短。

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