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首页> 外文期刊>Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology >Antibodies against neo‐epitope of microbial and human transglutaminase complexes as biomarkers of childhood celiac disease
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Antibodies against neo‐epitope of microbial and human transglutaminase complexes as biomarkers of childhood celiac disease

机译:针对微生物和人转谷氨酰胺酶复合物的新表位的抗体作为儿童腹腔疾病的生物标志物

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摘要

Summary Tissue transglutaminase (tTG) and microbial transglutaminase (mTG) cross‐link gliadins to form complexes that expose immunogenic neo‐epitopes to produce tTG and mTG‐neo‐epitope antibodies. The aim of this study was to test the diagnostic performance of antibodies against non‐complexed and complexed forms of transglutaminases, to correlate their activities to the intestinal damage and to explore age group dependency in celiac disease (CD). A total of 296 children with untreated CD and 215 non‐celiac disease controls were checked by in‐house enzyme‐linked immunosorbent assays detecting immunoglobulin (Ig)A, IgG or combined detection of IgA and IgG (check) against tTG, AESKULISA ? tTG New Generation (tTG‐neo) and mTG‐neo (RUO), IgA and IgG antibodies against deamidated gliadin peptide (DGP) and human IgA anti‐endomysium antibodies (EMA) using AESKUSLIDES ? EMA. Intestinal pathology was graded according the revised Marsh criteria, and age dependencies of the antibody activities were analysed. Using cut‐offs estimated from receiver operating characteristic (ROC) curves, the highest area under curve (AUC) of the TG assays was 0·963 for tTG‐neo check, followed by tTG check (0·962) when the diagnosis was based on enteric mucosal histology. tTG‐neo check was the most effective to reflect the intestinal abnormalities in CD ( r ?=?0·795, P ??0·0001). High levels of anti‐mTG‐neo IgG and anti‐tTG‐neo IgG appeared in the earlier age groups, as compared to anti‐tTG IgG ( P ??0·001). Considering antibody diagnostic performance based on AUC, enteric damage reflection and predictability at an early age, the anti‐neo tTG check was the most effective diagnostic biomarker for pediatric CD. The mTG neo check might represent a new marker for CD screening, diagnosis and predictability.
机译:发明内容组织转谷氨酰胺酶(TTG)和微生物转谷氨酰胺酶(MTG)交联胶质蛋白,形成露出免疫原性新表位的复合物以产生TTG和MTG-Neo-Epitope抗体。本研究的目的是测试抗体对非络合和络合形式的转谷氨酰胺酶的诊断性能,以将它们的活性与肠道损伤相关,并探讨腹腔疾病(CD)的年龄组依赖性。通过内部酶联免疫吸附测定检测免疫球蛋白(Ig)A,IgG或Chinod检测IgA和IgG(Check)对抗TTG,Aeskulisa的IgA和IgG(Check)组合的296名具有未处理的CD和215个非乳糜泻对照的儿童。使用Aeskuslides,TTG新一代(TTG-NEO)和MTG-NEO(RUO),IgA和IgG抗体和人IGA抗末端抗体(EMA)的人IGA抗末端抗体(EMA)? Ema。根据经修订的沼泽标准评分肠道病理学,分析了抗体活性的年龄依赖性。使用从接收器操作特征(ROC)曲线估计的截止,TG测定的曲线(AUC)下的最高面积为0·963,对于TTG-NEO检查,其次是TTG检查(0·962)当诊断基础时在肠溶粘膜组织学上。 TTG-Neo检查是最有效的,最有效地反映CD中的肠道异常(R?= 0·795,p≤≤0·0001)。与抗TTG IgG相比,在较早的年龄组中出现高水平的抗MTG-NeO IgG和抗TTG-Neo IgG(P 1 0·001)。考虑到基于AUC,肠溶损伤反射和预测性的抗体诊断性能在休眠期,抗NEO TTG检查是儿科CD最有效的诊断生物标志物。 MTG Neo Check可能代表CD筛选,诊断和可预测性的新标记。

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