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在一项基于瑞典儿童总体人群的研究中,检测谷氨酸脱羧酶抗体、胰岛素抗体、胰岛细胞抗体及进行HLA分型以诊断糖尿病。

Glutamate decarboxylase-, insulin-, and islet cell-antibodies and HLA typing to detect diabetes in a general population-based study of Swedish children.

作者信息

Hagopian W A, Sanjeevi C B, Kockum I, Landin-Olsson M, Karlsen A E, Sundkvist G, Dahlquist G, Palmer J, Lernmark A

机构信息

Department of Medicine, University of Washington, Seattle 98195, USA.

出版信息

J Clin Invest. 1995 Apr;95(4):1505-11. doi: 10.1172/JCI117822.

Abstract

Most autoimmune diabetes occurs in those without a diabetic relative, but few cases are identifiable prospectively. To model general population prediction, 491 consecutive newly diabetic children from all of Sweden were tested for autoantibodies to glutamate decarboxylase (GAD65ab), insulin (IAA), and islet cells (ICA), and for HLA-DQ genotypes by PCR; 415 matched control children were tested in parallel. GAD65ab sensitivity/specificity was 70/96%, versus 84/96% for ICA, 56/97% for IAA, 93/93% (any positive), 39/99.7% (all positive), and 41/99.7% (GAD65ab plus IAA). The latter's 25% predictive value was not improved by requiring concomitant high-risk HLA genotypes. GAD65ab were associated with DQA10501/B10201 (DQ2; P = 0.007) but not DQA10301/B10302 (DQ8), and IAA with DQA10301/B10302 (DQ8; P = 0.03) but not DQA10501/B10201 (DQ2). GAD65ab were more prevalent in females than males (79 vs. 63%; P < 0.0001) but did not vary with onset age nor season. Combining the three antibody assays yielded sufficient sensitivity for screening. GADab were relatively sensitive/specific for diabetes, but even with HLA marker combinations yielded predictive values insufficient for early immunointervention in the low-prevalence general population.

摘要

大多数自身免疫性糖尿病发生在没有糖尿病亲属的人群中,但前瞻性可识别的病例很少。为了建立一般人群预测模型,对来自瑞典各地的491名连续新诊断的糖尿病儿童进行了谷氨酸脱羧酶自身抗体(GAD65ab)、胰岛素自身抗体(IAA)和胰岛细胞自身抗体(ICA)检测,并通过聚合酶链反应检测HLA - DQ基因型;同时对415名匹配的对照儿童进行了检测。GAD65ab的敏感性/特异性为70/96%,ICA为84/96%,IAA为56/97%,任何一项阳性为93/93%,三项均阳性为39/99.7%,GAD65ab加IAA为41/99.7%。即使要求同时存在高风险HLA基因型,后者25%的预测价值也没有提高。GAD65ab与DQA10501/B10201(DQ2;P = 0.007)相关,但与DQA10301/B10302(DQ8)无关,IAA与DQA10301/B10302(DQ8;P = 0.03)相关,但与DQA10501/B10201(DQ2)无关。GAD65ab在女性中比男性更普遍(79%对63%;P < 0.0001),但与发病年龄和季节无关。联合三项抗体检测对筛查具有足够的敏感性。GADab对糖尿病相对敏感/特异,但即使结合HLA标记组合,在低患病率的一般人群中预测价值仍不足以进行早期免疫干预。

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