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初发未受影响的学龄儿童中自身抗体的稳定性及其与1型糖尿病遗传和代谢标志物的关系。

Stability of autoantibodies and their relation to genetic and metabolic markers of Type I diabetes in initially unaffected schoolchildren.

作者信息

Kulmala P, Rahko J, Savola K, Vähäsalo P, Veijola R, Sjöroos M, Reunanen A, Ilonen J, Knip M

机构信息

Department of Paediatrics, University of Oulu, Finland.

出版信息

Diabetologia. 2000 Apr;43(4):457-64. doi: 10.1007/s001250051329.

Abstract

AIMS/HYPOTHESIS: To study temporal changes in positivity for autoantibodies associated with Type I (insulin-dependent) diabetes mellitus and the relations between these antibodies, HLA-DQB1-risk markers and first-phase insulin response (FPIR) in non-diabetic schoolchildren.

METHODS

The stability of the antibody status over 2 years was assessed in 104 schoolchildren initially positive for islet cell antibodies (ICA) or antibodies to the 65,000 M(r) isoform of the glutamic acid decarboxylase (GADA) or both and in 104 antibody-negative control children matched for sex, age and place of residence. All children were also studied for their first-phase insulin response and HLA-DQB1 alleles on the second occasion.

RESULTS

On the second occasion 3 of the 98 initially ICA-positive children, 3/13 of those positive for antibodies to the IA-2 protein (IA-2A), 1/17 GADA-positive and 2/7 of those positive for insulin autoantibodies (IAA) tested negative for these antibodies. Children with IA-2A, GADA, IAA and multiple (> or = 2) antibodies had significantly lower first-phase insulin responses than the control children. In contrast, these responses did not differ between subjects with and without specific HLA-DQB1-risk alleles or genotypes. Of the six subjects with a considerably reduced first-phase insulin response three had multiple antibodies on both occasions but none of them had a DQB1 genotype conferring increased diabetes risk. Two subjects progressed to Type I diabetes within 3.4 years of follow-up, both of them having multiple antibodies and a considerably reduced first-phase insulin response but neither of them having a DQB1-risk genotype.

CONCLUSIONS/INTERPRETATION: Positivity for diabetes-associated autoantibodies is a relatively stable phenomenon in unaffected schoolchildren, although conversion to seronegativity can occur occasionally. Our observations also indicate that DQB1 alleles associated with decreased susceptibility to Type I diabetes do not protect from impaired beta-cell function or from progression to overt disease in initially unaffected schoolchildren.

摘要

目的/假设:研究与Ⅰ型(胰岛素依赖型)糖尿病相关的自身抗体阳性率随时间的变化,以及这些抗体、HLA - DQB1风险标志物与非糖尿病学龄儿童的第一相胰岛素反应(FPIR)之间的关系。

方法

对104名最初胰岛细胞抗体(ICA)或谷氨酸脱羧酶65000 M(r)异构体抗体(GADA)或两者均呈阳性的学龄儿童以及104名性别、年龄和居住地点相匹配的抗体阴性对照儿童进行了为期2年的抗体状态稳定性评估。第二次检查时,还对所有儿童进行了第一相胰岛素反应和HLA - DQB1等位基因研究。

结果

第二次检查时,98名最初ICA阳性儿童中有3名、IA - 2蛋白抗体(IA - 2A)阳性儿童中有3/13、GADA阳性儿童中有1/17以及胰岛素自身抗体(IAA)阳性儿童中有2/7这些抗体检测呈阴性。IA - 2A、GADA、IAA及多种(≥2种)抗体阳性的儿童第一相胰岛素反应显著低于对照儿童。相比之下,具有或不具有特定HLA - DQB1风险等位基因或基因型的受试者之间这些反应无差异。在6名第一相胰岛素反应明显降低的受试者中,3名在两次检查时均有多种抗体,但他们均无增加糖尿病风险的DQB1基因型。两名受试者在随访3.4年内进展为Ⅰ型糖尿病,他们均有多种抗体且第一相胰岛素反应明显降低,但均无DQB1风险基因型。

结论/解读:在未患病的学龄儿童中,与糖尿病相关的自身抗体阳性是一种相对稳定的现象,尽管偶尔可能会转为血清阴性。我们的观察结果还表明,与Ⅰ型糖尿病易感性降低相关的DQB1等位基因并不能保护最初未患病的学龄儿童的β细胞功能受损或预防进展为显性疾病。

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