Further studies of anti-endomysium and anti-gliadin antibodies in patients with suspected celiac disease

被引:17
作者
Del Rosario, MA [1 ]
Fitzgerald, JF [1 ]
Chong, SK [1 ]
Croffie, JM [1 ]
Gupta, SK [1 ]
机构
[1] Indiana Univ, Med Ctr, James Whitcomb Riley Hosp Children, Div Gastroenterol Hepatol Nutr, Indianapolis, IN 46202 USA
关键词
anti-endomysium antibody; anti-gliadin antibodies; biopsy; celiac disease; small intestine;
D O I
10.1097/00005176-199808000-00012
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background: The findin,o of characteristic small intestinal mucosal abnormalities on histologic examination of a biopsy specimen remains the first requirement for the diagnosis of celiac disease. A reliable and noninvasive test would be ideal for the patient's convenience and for reducing health-care costs, The sensitivity and specificity of anti-gliadin antibodies (AGA-immunoglobulin [Ig] G, AGA-IgA) have been variable; anti-endomysium IgA (EmA-IgA) is more helpful. In an earlier study conducted at the authors' institution, celiac disease was present in 19 patients examined from 1992 to 1995. Anti-endomysium titers were higher than normal in all 19 patients (100%). Total villous atrophy was seen in 14 of 17 biopsy specimens (82%) and subtotal atrophy in 3 (18%). The purpose of the current study was to evaluate further the accuracy of EmA-IgA in diagnosing celiac disease. Methods: One hundred seven patients were screened for celiac disease between March 1996 and July 1997. The level of EmA-IgA was measured in all patients, and AGA-IgG and AGA-IgA were measured in 104 patients. Forty-six patients underwent endoscopic biopsy of the small bowel, with measurement of disaccharidase enzymes in 45 patients. Results: Five of 46 patients had celiac disease (three boys and two girls; mean age: 5.3 years; 2-9.5 years); one also had cystic fibrosis and another had insulin-dependent diabetes mellitus. All five had marked to complete villous atrophy with crypt hyperplasia and increased serum EmA-IgA (100% sensitivity). None of the remaining patients had increased EmA-IgA (100% specificity). Serum levels of AGA-IgG and AGA-IgA were increased in all four celiac disease patients (100% sensitivity), but they were also high in patients without celiac disease (38% and 92% specificity, respectively), which compromises their diagnostic value. None of the patients confirmed to have celiac disease had IgA deficiency. Abnormal disaccharidase enzyme activities were documented in all five celiac disease patients: severe generalized deficiency (n = 2), moderately severe generalized deficiency tit = 2), and alactasia with moderate deficiency of the a-glucosidases (n = 1). Conclusions: This study confirmed the reliability and accuracy of EmA-IgA in the diagnosis of celiac disease. Small bowel biopsy may be unnecessary in EmA-positive patients in whom celiac disease is suspected.
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页码:191 / 195
页数:5
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