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首页> 外文期刊>Diabetes care >Successful prospective prediction of type 1 diabetes in schoolchildren through multiple defined autoantibodies: an 8-year follow-up of the Washington State Diabetes Prediction Study.
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Successful prospective prediction of type 1 diabetes in schoolchildren through multiple defined autoantibodies: an 8-year follow-up of the Washington State Diabetes Prediction Study.

机译:通过多种定义的自身抗体成功地对小学生中的1型糖尿病进行前瞻性预测:华盛顿州糖尿病预测研究的8年随访。

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OBJECTIVE: Almost 90% of type 1 diabetes appears in individuals without a close family history. We sought to evaluate the best current predictive strategy, multiple defined autoantibodies, in a long-term prospective study in the general population. RESEARCH DESIGN AND METHODS: Autoantibodies to pancreatic islets (islet cell antibodies [ICAs]) and defined autoantibodies (d-aab) to human GAD, IA2/ICA512, and insulin were tested in 4,505 Washington schoolchildren. Eight years later, 3,000 (67%) subjects were recontacted, including 97% of subjects with any test >99th percentile. RESULTS: Six subjects developed diabetes (median interval 2.8 years), all from among the 12 individuals with multiple d-aab, representing 50% positive predictive value (95% CI 25-75%) and 100% sensitivity (58-100%). Among the others, diabetes occurred in 0 of 6 with one d-aab plus ICA, 0 of 26 with ICA only, 0 of 7 with one d-aab equaling the 99th percentile and another d-aab equaling the 97.5th percentile, 0 of 86 with one d-aab, and 0 of 2,863 with no d-aab or ICA. Adjusted for verification bias, multiple d-aab were 99.9% specific (99.86-99.93%). At this age, new d-aab seldom appeared. Once present, d-aab usually persisted regardless of disease progression, although less so for insulin autoantibodies. Insulin secretion by sequential glucose tolerance testing remained normal in four multiple d-aab subjects not developing diabetes. Of children developing diabetes, five of six (83%) would be included if HLA-DQ genotyping preceded antibody testing, but HLA-DQ did not explain outcomes among high-risk subjects, even when considered along with other genetic markers. CONCLUSIONS: Multiple d-aab were established by age 14 years and prospectively identified all schoolchildren who developed type 1 diabetes within 8 years.
机译:目的:几乎90%的1型糖尿病患者均无家族史。我们力求在一项针对一般人群的长期前瞻性研究中,评估当前最佳的预测策略,多种定义的自身抗体。研究设计和方法:在4,505名华盛顿学童中测试了针对胰岛的自身抗体(胰岛细胞抗体[ICAs])和针对人GAD,IA2 / ICA512和胰岛素的明确自身抗体(d-aab)。八年后,重新联系了3,000(67%)位受试者,其中97%的受试者的测试结果> 99%。结果:6名受试者患了糖尿病(中位间隔2.8年),全部来自12名多发d-aab个体,分别代表50%的阳性预测值(95%CI 25-75%)和100%的敏感性(58-100%) 。其中,糖尿病发生率为6的0,其中1 d-aab加ICA,26的0为仅ICA,7的0为1 d-aab等于99%,另一d-aab的97.5百分点,0为0 86个,其中一个为d-aab,2,863中的0个为无d-aab或ICA。调整验证偏倚后,多个d-aab的特异性为99.9%(99.86-99.93%)。在这个年龄,很少出现新的d-aab。一旦存在,无论疾病进展如何,d-aab通常都会持续存在,尽管对于胰岛素自身抗体而言则较少。通过连续的葡萄糖耐量测试,胰岛素分泌在四个未患糖尿病的多发性d-aab受试者中保持正常。在HLA-DQ基因分型之前先进行抗体测试的儿童中,将有6个患糖尿病的儿童中有5个(83%)被包括在内,但是HLA-DQ不能解释高风险受试者的预后,即使与其他遗传标记一起考虑时也是如此。结论:在14岁时建立了多个d-aab,并前瞻性鉴定了所有在8年内患上1型糖尿病的学童。

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