双时相胰岛自身抗体筛查用于儿童 1 型糖尿病:一项前瞻性队列研究。
Two-age islet-autoantibody screening for childhood type 1 diabetes: a prospective cohort study.
机构信息
Center for Computational Health, IBM Research, Yorktown Heights, NY, USA; Faculty of Science, Ain Shams University, Cairo, Egypt.
Juvenile Diabetes Research Foundation, New York, NY, USA.
出版信息
Lancet Diabetes Endocrinol. 2022 Aug;10(8):589-596. doi: 10.1016/S2213-8587(22)00141-3. Epub 2022 Jul 5.
BACKGROUND
Early prediction of childhood type 1 diabetes reduces ketoacidosis at diagnosis and provides opportunities for disease prevention. However, only highly efficient approaches are likely to succeed in public health settings. We sought to identify efficient strategies for initial islet autoantibody screening in children younger than 15 years.
METHODS
We harmonised data from five prospective cohorts from Finland (DIPP), Germany (BABYDIAB), Sweden (DiPiS), and the USA (DAISY and DEW-IT) into the Type 1 Diabetes Intelligence (T1DI) cohort. 24 662 children at high risk of diabetes enrolled before age 2 years were included and followed up for islet autoantibodies and diabetes until age 15 years, or type 1 diabetes onset, whichever occurred first. Islet autoantibodies measured included those against glutamic acid decarboxylase, insulinoma antigen 2, and insulin. Main outcomes were sensitivity and positive predictive value (PPV) of detected islet autoantibodies, tested at one or two fixed ages, for diagnosis of clinical type 1 diabetes.
FINDINGS
Of the 24 662 participants enrolled in the Type 1 Diabetes Intelligence cohort, 6722 total were followed up to age 15 years or until onset of type 1 diabetes. Type 1 diabetes developed by age 15 years in 672 children, but did not develop in 6050 children. Optimal screening ages for two measurements were 2 years and 6 years, yielding sensitivity of 82% (95% CI 79-86) and PPV of 79% (95% CI 75-80) for diabetes by age 15 years. Autoantibody positivity at the beginning of each test age was highly predictive of diagnosis in the subsequent 2-5·99 year or 6-15-year age intervals. Autoantibodies usually appeared before age 6 years even in children diagnosed with diabetes much later in childhood.
INTERPRETATION
Our results show that initial screening for islet autoantibodies at two ages (2 years and 6 years) is sensitive and efficient for public health translation but might require adjustment by country on the basis of population-specific disease characteristics.
FUNDING
Juvenile Diabetes Research Foundation.
背景
早期预测儿童 1 型糖尿病可减少诊断时的酸中毒,并为疾病预防提供机会。然而,只有高效的方法才有可能在公共卫生环境中取得成功。我们旨在确定在 15 岁以下儿童中进行初始胰岛自身抗体筛查的有效策略。
方法
我们将来自芬兰(DIPP)、德国(BABYDIAB)、瑞典(DiPiS)和美国(DAISY 和 DEW-IT)的五个前瞻性队列的数据纳入到 1 型糖尿病智能(T1DI)队列中进行了协调。纳入了 2 岁前有糖尿病高风险的 24662 名儿童,并对胰岛自身抗体和糖尿病进行随访,直至 15 岁或 1 型糖尿病发病,以先发生者为准。测量的胰岛自身抗体包括谷氨酸脱羧酶、胰岛素瘤抗原 2 和胰岛素自身抗体。主要结局是在一个或两个固定年龄进行检测时,胰岛自身抗体检测对临床 1 型糖尿病诊断的敏感性和阳性预测值(PPV)。
结果
在 1 型糖尿病智能队列中,共纳入了 24662 名参与者,其中 6722 名参与者随访至 15 岁或 1 型糖尿病发病。672 名儿童在 15 岁前发展为 1 型糖尿病,但 6050 名儿童未发展为 1 型糖尿病。两次检测的最佳筛查年龄为 2 岁和 6 岁,在 15 岁时,对糖尿病的敏感性为 82%(95%CI 79-86),PPV 为 79%(95%CI 75-80)。每次检测起始时的自身抗体阳性高度提示在随后的 2-5.99 年或 6-15 年的年龄间隔内进行诊断。即使在儿童被诊断为较晚发病的糖尿病,自身抗体通常也会在 6 岁之前出现。
解释
我们的研究结果表明,在两个年龄段(2 岁和 6 岁)进行初始胰岛自身抗体筛查既敏感又高效,适用于公共卫生转化,但可能需要根据各国的具体疾病特征进行调整。
资助
青少年糖尿病研究基金会。
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