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Immunological response in coeliac disease is age related

Published online by Cambridge University Press:  12 May 2008

M. Calzado
Affiliation:
Pediatric Gastroenterology and Hepatology Section, La Fe Hospital, Valencia, Spain
E. Donat
Affiliation:
Pediatric Gastroenterology and Hepatology Section, La Fe Hospital, Valencia, Spain
B. Polo
Affiliation:
Pediatric Gastroenterology and Hepatology Section, La Fe Hospital, Valencia, Spain
B. Baena
Affiliation:
Pediatric Gastroenterology and Hepatology Section, La Fe Hospital, Valencia, Spain
C. Ribes
Affiliation:
Pediatric Gastroenterology and Hepatology Section, La Fe Hospital, Valencia, Spain
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Abstract

Type
1st International Immunonutrition Workshop, Valencia, 3–5 October 2007, Valencia, Spain
Copyright
Copyright © The Authors 2008

Anti-tissue transglutaminase antibodies (t-TG), mostly IgA class, is considered to be the most specific serological immune response in coeliac disease, and is associated with enteropathy, specific Ig A class antibody against t-TG being found at the intestinal level(Reference Salmi, Collin and Jarvinen1, Reference Salmi, Collin and Korponay-Szabó2).

The objective was to evaluate the serological immune response in coeliac disease according to age by measuring antibodies against the autoantigen, i.e. t-TG and if t-TG can be used as a screening method. A retrospective study was done reviewing the files of all patients who had undergone a small intestinal biopsy in the previous 3 years for diagnostic purposes. IgA t-TG (Varelisa™, Phadia, cut off 6 IU/ml) and IgA anti-gliadin antibodies (AGA; home method, cut off 0.3 arbitrary units) were determined when the biopsy was performed. In patients with negative IgA t-TG, IgG t-TG (Varelisa™; Phadia, Freiburg, Germany; cut off 10 IU/ml) was determined. A total of 280 patients were included, 160 of them showed Marsh 3 lesions and one of them showed Marsh 2 lesions. All of them were consuming gluten at the time the biopsy was performed. Diagnosis of coeliac disease was established in all of them. No patient had IgA deficiency. All children with t-TG>100 (upper detection limit) were classified as Marsh 3. Specificity for AGA was lower than that for t-TG. Eighty-eight patients (55%) were <3 years of age and sixty-one were <2 years of age. Ten of the eighty-eight patients (11.4%) were IgA t-TG negative, only one being >2 years of age. All ten subjects had elevated IgA AGA and no Ig G class antibodies against t-TG were detected. Clinical symptoms in patients who were t-TG positive and t-TG negative were the same.

The results show negative IgA class t-TG is expected in about 10% of patients with coeliac disease who are <2 years of age. Furthermore, no Ig G response is to be expected in those patients. It can be speculated that the immature development of the immune system slowly responding to gluten exposure delays the appearance of autoimmunity. This notion would be in keeping with reports of no IgA t-TG antibodies deposited at the intestinal level in younger patients(Reference Stene, Honeyman and Hoffenberg3Reference Tosco, Maglio, Paparo, Colicchio, Sannino, Granata, Rapacciulo and Troncone5). Moreover, the data confirm the response against gliadin is the immunological trigger in coeliac disease.

References

1. Salmi, TT, Collin, P, Jarvinen, O et al. (2006) Aliment Pharmacol Ther 24, 541552.Google Scholar
2. Salmi, TT, Collin, P, Korponay-Szabó, IR et al. (2006) Gut 55, 17461753.CrossRefGoogle Scholar
3. Stene, LC, Honeyman, MC, Hoffenberg, EJ et al. (2006) Am J Gastroenterol 101, 23332340.Google Scholar
4. Norris, JM, Barriga, K, Hoffenberg, EJ et al. (2005) JAMA 293, 23432351.Google Scholar
5. Tosco, A, Maglio, M, Paparo, F, Colicchio, B, Sannino, A, Granata, V, Rapacciulo, L & Troncone, R (2007) Proceedings of the 40th Meeting of the European Society of Paediatric Gastroenterology, Hepatology and Nutrition, Barcelona 2007, Abstr (In the Press).Google Scholar