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β细胞自身免疫的逆转改变1型糖尿病风险:TEDDY研究

Reversion of β-Cell Autoimmunity Changes Risk of Type 1 Diabetes: TEDDY Study.

作者信息

Vehik Kendra, Lynch Kristian F, Schatz Desmond A, Akolkar Beena, Hagopian William, Rewers Marian, She Jin-Xiong, Simell Olli, Toppari Jorma, Ziegler Anette-G, Lernmark Åke, Bonifacio Ezio, Krischer Jeffrey P

机构信息

Health Informatics Institute, Department of Pediatrics, Morsani College of Medicine, University of South Florida, Tampa, FL

Health Informatics Institute, Department of Pediatrics, Morsani College of Medicine, University of South Florida, Tampa, FL.

出版信息

Diabetes Care. 2016 Sep;39(9):1535-42. doi: 10.2337/dc16-0181. Epub 2016 Jun 16.

Abstract

OBJECTIVE

β-Cell autoantibodies are a feature of the preclinical phase of type 1 diabetes. Here, we asked how frequently they revert in a cohort of children at risk for type 1 diabetes and whether reversion has any effect on type 1 diabetes risk.

RESEARCH DESIGN AND METHODS

Children were up to 10 years of age and screened more than once for insulin autoantibody, GAD antibody, and insulinoma antigen-2 antibodies. Persistent autoantibody was defined as an autoantibody present on two or more consecutive visits and confirmed in two reference laboratories. Reversion was defined as two or more consecutive negative visits after persistence. Time-dependent Cox regression was used to examine how reversion modified the risk of development of multiple autoantibodies and type 1 diabetes.

RESULTS

Reversion was relatively frequent for autoantibodies to GAD65 (19%) and insulin (29%), but was largely restricted to children who had single autoantibodies (24%) and rare in children who had developed multiple autoantibodies (<1%). Most (85%) reversion of single autoantibodies occurred within 2 years of seroconversion. Reversion was associated with HLA genotype, age, and decreasing titer. Children who reverted from single autoantibodies to autoantibody negative had, from birth, a risk for type 1 diabetes of 0.14 per 100 person-years; children who never developed autoantibodies, 0.06 per 100 person-years; and, children who remained single-autoantibody positive, 1.8 per 100 person-years.

CONCLUSIONS

Type 1 diabetes risk remained high in children who had developed multiple β-cell autoantibodies even when individual autoantibodies reverted. We suggest that monitoring children with single autoantibodies for at least 1 year after seroconversion is beneficial for stratification of type 1 diabetes risk.

摘要

目的

β细胞自身抗体是1型糖尿病临床前期的一个特征。在此,我们探讨了它们在1型糖尿病高危儿童队列中逆转的频率,以及逆转是否对1型糖尿病风险有任何影响。

研究设计与方法

研究对象为10岁及以下儿童,多次进行胰岛素自身抗体、谷氨酸脱羧酶(GAD)抗体和胰岛瘤相关抗原2抗体的筛查。持续性自身抗体定义为在两次或更多次连续就诊时出现且在两个参考实验室得到确认的自身抗体。逆转定义为在持续性自身抗体出现后连续两次或更多次就诊呈阴性。采用时间依赖性Cox回归分析来研究逆转如何改变多种自身抗体和1型糖尿病发生的风险。

结果

GAD65自身抗体(19%)和胰岛素自身抗体(29%)的逆转相对常见,但主要局限于仅有单一自身抗体的儿童(24%),而在已出现多种自身抗体的儿童中很少见(<1%)。大多数(85%)单一自身抗体的逆转发生在血清转换后的2年内。逆转与HLA基因型、年龄和滴度降低有关。从单一自身抗体转为自身抗体阴性的儿童,自出生起1型糖尿病发病风险为每100人年0.14例;从未出现自身抗体的儿童,每100人年0.06例;而持续单一自身抗体阳性的儿童,每100人年1.8例。

结论

即使个别自身抗体逆转,已出现多种β细胞自身抗体的儿童1型糖尿病风险仍然很高。我们建议,对单一自身抗体阳性儿童在血清转换后至少监测1年,这有助于对1型糖尿病风险进行分层。

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