Celiac disease (CD) is a permanent intolerance to gluten that results in damage to the mucosa of the small intestine. The prevalence of CD in developing countries may be undervalued due to different factors, but lack of awareness and low suspicion of the disease could be the main factors. The aim of the present work was to estimate the occurrence of CD among children suffering from chronic diarrhea in Gaza Strip and to adopt dependable non -invasive immunological techniques for diagnosis of CD in the laboratories of the Ministry of Health. This study was conducted on children (6-96 months) suffering from frequent (>3times/day) chronic diarrhea that not caused by infection. The study population comprised 123 symptomatic Palestinian children. Five ml peripheral blood were collected, sera were separated and stored at -70 ⁰C until performing the following assays: IgA Anti-endomysial antibodies(EMAs) using indirect immunofluorescence technique (IF), anti- tissue transglutaminase enzyme antibodies (tTG, IgG, IgA) and (tTG, IgA) using ELISA technique, anti smooth muscle antibodies (ASMA) using indirect immunofluorescence and total IgA using radial immunodiffusion (RID). The prevalence of CD using EMAs test was 3.25% but 12.2% when (tTG IgG, IgA) assay was applied. However, the prevalence of ASMA was 28.5% which may mask the EMAs antibodies and hence giving false negative results of EMAs. Our results showed comparable sensitivity of both (tTG IgG, IgA) and EMAs. Deficient or low IgA represented 33.3% of all (tTG IgG, IgA) positive samples. It was concluded that EMAs and (tTG IgG, IgA) tests could be used as noninvasive techniques on children suffering from CD. However for those having low or IgA deficiency, the class IgG of EMAs and tTG should be performed.
| Published in | American Journal of BioScience (Volume 2, Issue 6) |
| DOI | 10.11648/j.ajbio.20140206.11 |
| Page(s) | 192-195 |
| Creative Commons |
This is an Open Access article, distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution and reproduction in any medium or format, provided the original work is properly cited. |
| Copyright |
Copyright © The Author(s), 2014. Published by Science Publishing Group |
Celiac Disease, Tissue Transglutaminase Antibodies, Anti-Endomysial Antibodies, Antismooth Muscle Antibodies,Gaza Strip.
| [1] | Bardella MT, Minoli G, Radaelli F, Quatrini M, Bianchi PA, Conte D. (2000). Reevaluation of duodenal endoscopic markers in the diagnosis of celiac disease. Gastrointestinal endoscopy 51(6):714-716. |
| [2] | Ferguson A. (1997). Celiac disease, an eminently treatable condition, may be underdiagnosed in the United States. The American journal of gastroenterology 92(8):1252-1254. |
| [3] | Antonioli DA. (2003). Celiac disease: a progress report. Modern Pathology 16(4):342-346. |
| [4] | Mazzarella G, Maglio M, Paparo F, Nardone G, Stefanile R, Greco L, van de Wal Y, Kooy Y, Koning F, Auricchio S, Troncone R.. (2003). An immunodominant DQ8 restricted gliadin peptide activates small intestinal immune response in in vitro cultured mucosa from HLA-DQ8 positive but not HLA-DQ8 negative coeliac patients. Gut 52(1):57-62. |
| [5] | Fasano A, Berti I, Gerarduzzi T, Not T, Colletti RB, Drago S, Elitsur Y, Green PH, Guandalini S, Hill ID, Pietzak M, Ventura A, Thorpe M, Kryszak D, Fornaroli F, Wasserman SS, Murray JA, Horvath K. (2003). Prevalence of celiac disease in at-risk and not-at-risk groups in the United States: a large multicenter study. Archives of internal medicine 163(3):286-292. |
| [6] | Barada K, Bitar A, Mokadem MA, Hashash JG, Green P. (2010). Celiac disease in Middle Eastern and North African countries: a new burden?. World Journal Gastroenterology 16(12):1449-57. |
| [7] | Barada K, Abu Daya H, Rostami K, Catassi C. (2012). Celiac disease in the developing world. Gastrointest Endosc Clin N Am 22(4):773-96. |
| [8] | The American Celiac disease alliance http://americanceliac.org/celiac-disease/diagnosis/. |
| [9] | National Institutes of Health Consensus Development Conference on Celiac Disease: final statement. June 28–30, 2004. Available at (http://consensus.nih.gov/2004/2004CeliacDisease118html.htm) |
| [10] | Aetna. Clinical Policy Bulletin: Celiac Disease Laboratory Testing. Number: 0561 http://www.aetna.com/cpb/medical/data/500_599/0561.html |
| [11] | Tesija Kuna A. (2009). Laboratory diagnosis of autoimmune disease. Biochemia Medica 19 (suppl 1): S21-S22. |
| [12] | Chirdo FG, Rumbo M, Carabajal P, Castagnino N, Mavromatopulos E, Cirincione V, Anon MC, Fossati CA (1999). Analysis of anti-gliadin antibodies by immunoblot analysis and enzyme-linked immunosorbent assay using gliadin fractions as antigens. Journal of Pediatric Gastroenterology and Nutrition 29(2):171-177. |
| [13] | Not T, Horvath K, Hill ID, Partanen J, Hammed A, Magazzu G, Fasano A. (1998). Celiac disease risk in the USA: high prevalence of antiendomysium antibodies in healthy blood donors. Scandinavian Journal of gastroenterology 33(5):494-498. |
| [14] | Llorente MJ, Sebastian M, Fernandez-Acenero MJ, Serrano G, Villanueva S. (2004). IgA antibodies against tissue transglutaminase in the diagnosis of celiac disease: concordance with intestinal biopsy in children and adults. Clinical Chemistry 50(2):451-453. |
| [15] | Lasagni D, Ferrari R, Lapini M. (1999). Unmasking anti-endomysial antibodies in coeliac subjects positive for anti-smooth muscle antibodies. Acta Paediatrica 88(4):462-464. |
| [16] | Kumar V, Jarzabek-Chorzelska M, Sulej J, Karnewska K, Farrell T, Jablonska S. (2002). Celiac disease and immunoglobulin a deficiency: how effective are the serological methods of diagnosis? Clinical and Diagnostic Laboratory Immunology 9(6):1295-1300. |
| [17] | Korponay-Szabo IR, Dahlbom I, Laurila K, Koskinen S, Woolley N, Partanen J, Kovacs JB, Maki M, Hansson T. (2003). Elevation of IgG antibodies against tissue transglutaminase as a diagnostic tool for coeliac disease in selective IgA deficiency. Gut 52(11):1567-1571. |
| [18] | Vitoria JC, Arrieta A, Arranz C, Ayesta A, Sojo A, Maruri N, Garcia-Masdevall MD. (1999). Antibodies to gliadin, endomysium, and tissue transglutaminase for the diagnosis of celiac disease. Journal of Pediatric Gastroenterology and Nutrition 29(5):571-574. |
APA Style
Ahmed Mahmood Ruby, Randa Al-Khodary, Mohammad Shubair, Mahmoud Sirdah. (2014). Immunodiagnosis of Celiac Disease among Children with Chronic Diarrhea in Gaza Strip, Palestine. American Journal of BioScience, 2(6), 192-195. https://doi.org/10.11648/j.ajbio.20140206.11
ACS Style
Ahmed Mahmood Ruby; Randa Al-Khodary; Mohammad Shubair; Mahmoud Sirdah. Immunodiagnosis of Celiac Disease among Children with Chronic Diarrhea in Gaza Strip, Palestine. Am. J. BioScience 2014, 2(6), 192-195. doi: 10.11648/j.ajbio.20140206.11
AMA Style
Ahmed Mahmood Ruby, Randa Al-Khodary, Mohammad Shubair, Mahmoud Sirdah. Immunodiagnosis of Celiac Disease among Children with Chronic Diarrhea in Gaza Strip, Palestine. Am J BioScience. 2014;2(6):192-195. doi: 10.11648/j.ajbio.20140206.11
Share This Article
Twitter
Linked In
Facebook
Copy
Download@article{10.11648/j.ajbio.20140206.11,
author = {Ahmed Mahmood Ruby and Randa Al-Khodary and Mohammad Shubair and Mahmoud Sirdah},
title = {Immunodiagnosis of Celiac Disease among Children with Chronic Diarrhea in Gaza Strip, Palestine},
journal = {American Journal of BioScience},
volume = {2},
number = {6},
pages = {192-195},
doi = {10.11648/j.ajbio.20140206.11},
url = {https://doi.org/10.11648/j.ajbio.20140206.11},
eprint = {https://article.sciencepublishinggroup.com/pdf/10.11648.j.ajbio.20140206.11},
abstract = {Celiac disease (CD) is a permanent intolerance to gluten that results in damage to the mucosa of the small intestine. The prevalence of CD in developing countries may be undervalued due to different factors, but lack of awareness and low suspicion of the disease could be the main factors. The aim of the present work was to estimate the occurrence of CD among children suffering from chronic diarrhea in Gaza Strip and to adopt dependable non -invasive immunological techniques for diagnosis of CD in the laboratories of the Ministry of Health. This study was conducted on children (6-96 months) suffering from frequent (>3times/day) chronic diarrhea that not caused by infection. The study population comprised 123 symptomatic Palestinian children. Five ml peripheral blood were collected, sera were separated and stored at -70 ⁰C until performing the following assays: IgA Anti-endomysial antibodies(EMAs) using indirect immunofluorescence technique (IF), anti- tissue transglutaminase enzyme antibodies (tTG, IgG, IgA) and (tTG, IgA) using ELISA technique, anti smooth muscle antibodies (ASMA) using indirect immunofluorescence and total IgA using radial immunodiffusion (RID). The prevalence of CD using EMAs test was 3.25% but 12.2% when (tTG IgG, IgA) assay was applied. However, the prevalence of ASMA was 28.5% which may mask the EMAs antibodies and hence giving false negative results of EMAs. Our results showed comparable sensitivity of both (tTG IgG, IgA) and EMAs. Deficient or low IgA represented 33.3% of all (tTG IgG, IgA) positive samples. It was concluded that EMAs and (tTG IgG, IgA) tests could be used as noninvasive techniques on children suffering from CD. However for those having low or IgA deficiency, the class IgG of EMAs and tTG should be performed.},
year = {2014}
}
TY - JOUR T1 - Immunodiagnosis of Celiac Disease among Children with Chronic Diarrhea in Gaza Strip, Palestine AU - Ahmed Mahmood Ruby AU - Randa Al-Khodary AU - Mohammad Shubair AU - Mahmoud Sirdah Y1 - 2014/10/30 PY - 2014 N1 - https://doi.org/10.11648/j.ajbio.20140206.11 DO - 10.11648/j.ajbio.20140206.11 T2 - American Journal of BioScience JF - American Journal of BioScience JO - American Journal of BioScience SP - 192 EP - 195 PB - Science Publishing Group SN - 2330-0167 UR - https://doi.org/10.11648/j.ajbio.20140206.11 AB - Celiac disease (CD) is a permanent intolerance to gluten that results in damage to the mucosa of the small intestine. The prevalence of CD in developing countries may be undervalued due to different factors, but lack of awareness and low suspicion of the disease could be the main factors. The aim of the present work was to estimate the occurrence of CD among children suffering from chronic diarrhea in Gaza Strip and to adopt dependable non -invasive immunological techniques for diagnosis of CD in the laboratories of the Ministry of Health. This study was conducted on children (6-96 months) suffering from frequent (>3times/day) chronic diarrhea that not caused by infection. The study population comprised 123 symptomatic Palestinian children. Five ml peripheral blood were collected, sera were separated and stored at -70 ⁰C until performing the following assays: IgA Anti-endomysial antibodies(EMAs) using indirect immunofluorescence technique (IF), anti- tissue transglutaminase enzyme antibodies (tTG, IgG, IgA) and (tTG, IgA) using ELISA technique, anti smooth muscle antibodies (ASMA) using indirect immunofluorescence and total IgA using radial immunodiffusion (RID). The prevalence of CD using EMAs test was 3.25% but 12.2% when (tTG IgG, IgA) assay was applied. However, the prevalence of ASMA was 28.5% which may mask the EMAs antibodies and hence giving false negative results of EMAs. Our results showed comparable sensitivity of both (tTG IgG, IgA) and EMAs. Deficient or low IgA represented 33.3% of all (tTG IgG, IgA) positive samples. It was concluded that EMAs and (tTG IgG, IgA) tests could be used as noninvasive techniques on children suffering from CD. However for those having low or IgA deficiency, the class IgG of EMAs and tTG should be performed. VL - 2 IS - 6 ER -
Email: