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根据诊断时的年龄和 1 型糖尿病的病程,可检测到 C-肽的流行率。

Prevalence of detectable C-Peptide according to age at diagnosis and duration of type 1 diabetes.

机构信息

Benaroya Research Institute, Seattle, WA

Jaeb Center for Health Research, Tampa, FL.

出版信息

Diabetes Care. 2015 Mar;38(3):476-81. doi: 10.2337/dc14-1952. Epub 2014 Dec 17.

Abstract

OBJECTIVE

It is generally accepted that complete β-cell destruction eventually occurs in individuals with type 1 diabetes, which has implications for treatment approaches and insurance coverage. The frequency of residual insulin secretion in a large cohort of individuals at varying ages of diagnosis and type 1 diabetes duration is unknown.

RESEARCH DESIGN AND METHODS

The frequency of residual insulin secretion was determined by measurement of nonfasting serum C-peptide concentration in 919 individuals with type 1 diabetes according to prespecified groups based on age at diagnosis and duration of disease (from 3 to 81 years' duration). Stimulated C-peptide was measured in those with detectable nonfasting values and a group of those with undetectable values as control.

RESULTS

The overall frequency of detectable nonfasting C-peptide was 29%, decreasing with time from diagnosis regardless of age at diagnosis. In all duration groups, the frequency of C-peptide was higher with diagnosis age >18 years compared with ≤18 years. Nineteen percent of those with undetectable nonfasting C-peptide were C-peptide positive upon stimulation testing.

CONCLUSIONS

The American Diabetes Association's definition of type 1 diabetes as "usually leading to absolute insulin deficiency" results in clinicians often considering the presence of residual insulin secretion as unexpected in this population. However, our data suggest that residual secretion is present in almost one out of three individuals 3 or more years from type 1 diabetes diagnosis. The frequency of residual C-peptide decreases with time from diagnosis regardless of age at diagnosis, yet at all durations of disease, diagnosis during adulthood is associated with greater frequency and higher values of C-peptide.

摘要

目的

人们普遍认为,1 型糖尿病患者最终会出现完全的β细胞破坏,这对治疗方法和保险覆盖范围有影响。在不同诊断年龄和 1 型糖尿病病程的大人群中,残余胰岛素分泌的频率尚不清楚。

研究设计和方法

根据诊断年龄和疾病持续时间(3 至 81 年)的预设分组,通过测量 919 名 1 型糖尿病患者的非空腹血清 C 肽浓度,确定残余胰岛素分泌的频率。在那些可检测到非空腹值的患者中以及一组不可检测值的患者中测量刺激 C 肽作为对照。

结果

总体上,可检测到的非空腹 C 肽的频率为 29%,无论诊断时的年龄如何,其频率均随时间的推移而降低。在所有持续时间组中,与≤18 岁相比,诊断年龄>18 岁的患者 C 肽阳性率更高。19%的非空腹 C 肽不可检测者在刺激试验时 C 肽阳性。

结论

美国糖尿病协会将 1 型糖尿病定义为“通常导致绝对胰岛素缺乏”,这导致临床医生通常认为在该人群中,残余胰岛素分泌是出乎意料的。然而,我们的数据表明,在确诊 1 型糖尿病 3 年以上的患者中,近三分之一的患者存在残余分泌。无论诊断时的年龄如何,从诊断到现在的时间流逝都会导致残余 C 肽的频率降低,但在所有疾病持续时间中,成年期诊断与更高频率和更高的 C 肽值相关。

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