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首页> 外文期刊>Clinical gastroenterology and hepatology: the official clinical practice journal of the American Gastroenterological Association >Diagnosis of celiac disease in adults based on serology test results, without small-bowel biopsy.
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Diagnosis of celiac disease in adults based on serology test results, without small-bowel biopsy.

机译:根据血清学检查结果诊断成人腹腔疾病,无需小肠活检。

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Celiac disease is underdiagnosed, with nonspecific symptoms and high morbidity. New diagnostic factors are needed. We aimed to estimate the frequency at which adult patients with positive results from serology tests are referred for small-bowel biopsies and to identify factors that improve the diagnosis of celiac disease.We performed a retrospective analysis of data from 2477 subjects who received serology tests for celiac disease between 2005 and 2007. We analyzed results for total levels of IgA, IgA against human tissue transglutaminase (hTTG), IgA and IgG against gliadin, as well as dilution titers of IgA against endomysial antibodies (EMA). Biopsy samples were analyzed by pathologists experienced in detecting mucosal changes associated with celiac disease and graded according to the Marsh system.Of the 2477 patients, 610 (25%) had abnormal results from serology tests, and 39% of these patients (240 of 610) underwent small-bowel biopsy analyses. Of these patients, 50 (21%) had biopsy findings consistent with celiac disease (Marsh 3 lesions) and were placed on gluten-free diets. Titers of IgA hTTG greater than 118 U identified patients with celiac disease with a 2% false-positive rate. Titers of 21 to 118 U, in combination with an EMA dilution titer of 1:160 or greater, had a positive predictive value of 83% for celiac disease. IgA hTTG levels less than 20 U, in combination with an EMA dilution titer less than 1:10, had a negative predictive value of 92% for celiac disease.Serum levels of IgA hTTG greater than 118 U, or 21 to 118 U in combination with an EMA dilution titer of 1:160 or greater, can be used to identify adult symptomatic patients with celiac disease, in the absence of a small-bowel biopsy.
机译:腹腔疾病诊断不足,具有非特异性症状和高发病率。需要新的诊断因素。我们的目的是估计接受血清学检查阳性结果的成年患者进行小肠活检的频率,并确定改善乳糜泻诊断的因素。我们对2477名接受血清学检查的受试者的数据进行了回顾性分析。 2005年至2007年之间的乳糜泻。我们分析了IgA,针对人体组织转谷氨酰胺酶(hTTG)的IgA,针对麦醇溶蛋白的IgA和IgG的总水平以及针对内膜肌抗体(EMA)的IgA稀释效价的结果。由经验丰富的病理学家分析活检样品,这些病理学家具有检测与乳糜泻相关的粘膜变化的经验,并根据Marsh系统进行分级。在2477例患者中,有610例(25%)血清学检查结果异常,其中39%(610例中的240例) )进行了小肠活检分析。在这些患者中,有50名(21%)的活检结果与乳糜泻(沼泽3病灶)一致,并接受无麸质饮食。大于118 U的IgA hTTG滴度可识别出患有腹腔疾病的患者,假阳性率为2%。滴度为21至118 U,再加上EMA稀释滴度为1:160或更高,则对乳糜泻的阳性预测值为83%。 IgA hTTG水平低于20 U且EMA稀释滴度低于1:10时,对乳糜泻的阴性预测值为92%.IgA hTTG血清水平高于118 U或21至118 U EMA稀释度为1:160或更高的,可用于在没有小肠活检的情况下鉴别出有症状的成人腹腔疾病患者。

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