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首页> 外文期刊>Pediatric diabetes. >Role of HLA‐DQ typing and anti‐tissue transglutaminase antibody titers in diagnosing celiac disease without duodenal biopsy in type 1 diabetes: A study of the population‐based pediatric type 1 diabetes cohort of Western Australia
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Role of HLA‐DQ typing and anti‐tissue transglutaminase antibody titers in diagnosing celiac disease without duodenal biopsy in type 1 diabetes: A study of the population‐based pediatric type 1 diabetes cohort of Western Australia

机译:HLA-DQ键入和抗组织转谷氨酰胺酶抗体滴度在1型糖尿病中没有十二指肠活检的诊断中的作用:对西澳大利亚群体的群体1型糖尿病队列的研究

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Abstract Aim The primary aim of the present study was to determine if it is cost effective to use human leukocyte antigen (HLA) typing as a first‐line screening test for celiac disease (CD) in children with type 1 diabetes (T1D), as recommended by the European Society of Paediatric Gastroenterology Hepatology and Nutrition (ESPGHAN). The second aim was to investigate whether anti‐tissue transglutaminase IgA (anti‐tTGA) antibodies can be used to diagnose CD without the need for a confirmatory duodenal biopsy in T1D. Methods Data for all T1D patients aged 18 years, who attended the diabetes clinics in Western Australia up to June 2017, were extracted from the Western Australian Children's Diabetes Database (WACDD) and analyzed for their demographic data and CD permissive HLA alleles (DQ2, DQ8, and DQ7). For T1D patients already diagnosed with CD, the mode of diagnosis of CD, anti‐tTGA titers, and CD permissive HLA alleles were analyzed. Results Of the 936 eligible T1D patients identified, HLA‐DQ typing was available for 551 (59%). Of these 551 patients, 504 (91.2%) were positive for celiac permissive HLA alleles. Eight percent (n?=?75) of the T1D patients had a co‐diagnosis of CD. High anti‐tTGA titers were observed in those who were diagnosed with a positive duodenal biopsy. Conclusion HLA‐DQ typing is not cost effective as a first‐line screening test for CD in T1D patients because of over‐representation of CD permissive HLA alleles in this group. Anti‐tTGA titers may be useful in diagnosing CD in T1D without duodenal biopsy, as high levels were found to be strongly predictive of CD.
机译:摘要目的本研究的主要目的是确定使用人白细胞抗原(HLA)作为患有1型糖尿病(T1D)的儿童腹腔疾病(CD)的一线筛查试验是否具有成本效益。欧洲儿科胃肠病学会肝脏和营养(Espghan)推荐。第二个目的是研究抗组织转谷氨酰胺酶IgA(抗TTGA)抗体是否可用于诊断CD,而无需在T1D中需要验证的十二指肠活检。方法对澳大利亚州西澳大利亚西部糖尿病诊所的所有T1D患者的数据从西澳大利亚儿童糖尿病数据库(WACDD)中提取,并分析了他们的人口统计数据和CD允许HLA等位基因(DQ2 ,dq8和dq7)。对于已经被诊断为CD的T1D患者,分析了CD,抗TTGA滴度和CD允许HLA等位基因的诊断方式。 936符合条件的T1D患者的结果,HLA-DQ打字可用于551(59%)。在这551名患者中,504例(91.2%)对于乳糜泻HLA等位基因是阳性的。 T1D患者的八分之八(N?=?75)对CD进行了共同诊断。在诊断患有正十二指肠活检的人中观察到高抗TTGA滴度。结论HLA-DQ打字在T1D患者中作为CD的一线筛选试验,由于该组的CD允许HLA等位基因的过度表示。抗TTGA滴度可用于在没有十二指肠活检的情况下在T1D中诊断CD,因为发现高水位是强烈预测CD的。

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