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Antibodies to Deamidated Gliadin Peptide in Diagnosis of Celiac Disease in Children




TekijätLammi A, Arikoski P, Simell S, Kinnunen T, Simell V, Paavanen-Huhtala S, Hinkkanen A, Veijola R, Knip M, Toppari J, Vaarala O, Simell O, Ilonen J.

Julkaisuvuosi2015

JournalJournal of Pediatric Gastroenterology and Nutrition

Vuosikerta60

Numero5

Aloitussivu626

Lopetussivu631

Sivujen määrä6

ISSN0277-2116

eISSN1536-4801

DOIhttps://doi.org/10.1097/MPG.0000000000000666


Tiivistelmä

Objectives: Determinationof antibodies to synthetic deamidatedgliadin peptides (anti-DGP) may work as an alternative or complement the commonly used test for tissue transglutaminase antibodies (TGA) in the diagnosis of celiac disease (CD). We analyzed the performance of a time-resolved immunofluorometry (TR-IFMA) based anti-DGP assay in the diagnosis of CD in children and also retrospectively analyzed the appearance of anti-DGP antibodies before TGA seroconversion.

Methods: The study included 92 children with biopsy-confirmed CD. Serum samples were taken at the time or just before the clinical diagnosis. The control group comprised of 82 TGA-negative children who were positive for HLA-DQ2 or -DQ8.

Results: Based on receiver operating characteristics (ROC) curves, the optimal cut-off value for IgA anti-DGP positivity was 153 arbitrary units (AU) with a sensitivity of 92.4% and specificity of 97.6% and that for IgG anti-DGP 119 AU, with a sensitivity of 97.8% and specificity of 97.6%. All of the 92 children with CD were either IgA or IgG anti-DGP positive at the time of diagnosis. Sera from 48 children with CD were also analyzed retrospectively before the diagnosis. Anti-DGP antibodies preceded TGA positivity in 35 of 48 CD children and appeared a median of one year earlier.

Conclusions: The TR-IFMA assay for detecting anti-DGP antibodies shows high sensitivity and specificity for the diagnosis of CD in children. In a majority of our study population anti-DGP seropositivity preceded TGA positivity, indicating that earlier detection of CD may be possible by monitoring anti-DGP antibodies frequently in genetically susceptible children.




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