| Title: | استخدام الأجسام المضادة الذاتية للأنسجة ناقلة الغلوتامين كتنبؤ بمرض الداء الزلاقي البطني(حساسية الأمعاء الدقيقة من الجلوتين) وعلاقتها بالتغيرات النسيجية المرضية من الخزعة المعوية.
TISSUE TRANSGLUTAMINASE AUTOANTIBODIES AS PREDICTORS OF CELIAC DISEASE AND ITS RELATIONSHIP TO HISTOPATHOLOGICAL FINDINGS OF INTESTINAL BIOPSY.
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| Authors: | أ.م.د. خالد عبد القوي إبراهيم1- د.احمد عبد الفتاح عزب1 - د. عبير مصطفي المحلاوي2 - د. عبد الرحمن الصاوي3 أقسام طب الأطفال1 والأنسجة وبيولوجيا الخلية2 , كلية طب بنها- جامعة بنها , قسم المكروبيولوجيا الطبية3 , كلية طب الأزهر, جامعة الأزهر. |
| Year: | 2008 |
| Keywords: | Not Available |
| Journal: | Not Available |
| Volume: | Not Available |
| Issue: | Not Available |
| Pages: | Not Available |
| Publisher: | Not Available |
| Local/International: | Local |
| Paper Link: | |
| Full paper | Not Available |
| Supplementary materials | Not Available |
| Abstract: |
Background: Celiac disease (CD) is a common autoimmune disorder, induced by the intake of gluten proteins present in wheat, barley and rye. Previously, it was considered to be a rare childhood disorder, but is actually considered a frequent condition, present at any age, which may have multiple complications. Active CD is characterized by intestinal and/or extra-intestinal symptoms, villous atrophy and crypt hyperplasia, and strongly positive IgA anti-endomysial antibody (EMA) and tissue transglutaminase (tTG) auto-antibodies. The duodenal biopsy is considered to be the “gold standard” for diagnosis. Objective(s): The use of screening tests for celiac disease has increased the number of patients referred for evaluation. We proposed that the subgroup of patients with very high tissue transglutaminase antibody (t-TGIgA) titers is positive for celiac disease and a small-bowel biopsy is not necessary to make the diagnosis. A gluten-free diet should be attempted and, if the patient’s symptoms do not improve, then a biopsy should be performed to confirm the diagnosis. Methods: It is a retrospective study, reviewed 51 patients who underwent both t-TGIgA testing and a small-bowel biopsy was performed. We examined the impact of using t-TGIgA values of >100 U and <20 U as cutoff values and suggested performing biopsies for patients with t-TGIgA values of 20 to 100 U, as is current practice. Results: Twenty-nine of 51 patients demonstrated positive biopsy results. Twenty-four of 51 patients had t-TGIgA levels of >100 U, with 23 of 24 exhibiting positive biopsy results. Only 3 of 8 patients with t-TGIgA values of 20 to 100 U exhibited positive biopsy results. Three patients with t-TGIgA levels of <20 U had positive biopsies; 2 were IgA negative and 1 had a duodenal ulcer. With the cutoff values of >100 U and <20 U with known IgA status, the sensitivity was 0.958 (23 of 24 cases) and the specificity was 0.941 (16 of 17 cases). Conclusions: When the cutoff values were changed to >100 and <20 U and IgA levels were verified, the sensitivity and specificity were very high. Patients with midrange t-TGIgA values (20–100 U) or values of <20 U with negative IgA status should continue to undergo biopsies for diagnosis of celiac disease |
