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Publication Date:
26 09 2011
ISSN:
1437-4331
DOI:
10.1515/cclm.2011.714

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Clinical Chemistry and Laboratory Medicine (CCLM)

Published in Association with the International Federation of Clinical Chemistry and Laboratory Medicine and the European Federation of Clinical Chemistry and Laboratory Medicine

Editor-in-Chief: Plebani, Mario

null Lippi, Giuseppe / Gillery, Philippe / Kazmierczak, Steven / Lackner, Karl J. / Melichar, Bohuslav / Siest, Gérard / Whitfield, John B. / Abi Fadel, Marianne / Alvarez Menendez, Francisco V. / Azzazy, Hassan M.E. / Diamandis, Eleftherios P. / Eckardstein, Arnold / Favaloro, Emmanuel J. / Griesmacher, Andrea / Herrmann, Wolfgang / Hoffmann, Johannes J.M.L. / Hooijkaas, Herbert / Ichihara, Kiyoshi / Kaabachi, Naziha / Kim, Jeong-Ho / Korte, Wolfgang / Kroupis, Christos / Lai, Leslie Charles / Lam, Wai Kei Christopher / Marc, Janja / Miyoshi, Eiji / Özben, Tomris / Palicka, Vladimir / Panteghini, Mauro / Queralto, Jose M. / Scartezini, Marileia / Simundic, Ana-Maria / Tsongalis, Gregory J. / Wallemacq, Pierre E. / Yan, Shengkai / Young, Ian S. / Chiu, Rossa Wai Kwun / Ghosh, Debabrata / Kappelmayer, Janos / Lehmann, Sylvain / Sypniewska, Grazyna

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Increased IMPACT FACTOR 2010: 2.069
Rank 9 out of 30 in category Medical Laboratory Technology in the 2010 Thomson Reuters Journal Citation Report/Science Edition

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The old and new tests for celiac disease: which is the best test combination to diagnose celiac disease in pediatric patients?

1 / Carroccio, Antonio 2 / Tonutti, Elio 3 / Villalta, Danilo 4 / Tozzoli, Renato 5 / Barrale, Maria 1 / Sarullo, Filippo M. 1 / Mansueto, Pasquale 6 / Chiusa, Stella Maria La 1 / Iacono, Giuseppe 7 / Bizzaro, Nicola 8

1Department of Clinical Pathology “Buccheri La Ferla” Hospital, Palermo, Italy

2Internal Medicine, Ospedali Civili Riuniti, Sciacca, Italy

3Immunopatologia e Allergologia, Azienda Ospedaliero-Universitaria S. Maria della Misericordia, Udine, Italy

4Allergologia e Immunologia Clinica, DML, AO Maria degli Angeli, Pordenone, Italy

5Laboratory of Clinical Pathology, AO Maria degli Angeli, Pordenone, Italy

6Internal Medicine, Department of Clinical Medicine and Emerging Diseases, University of Palermo, Italy

7Pediatric Gastroenterology, “Di Cristina” Hospital, Palermo, Italy

8Laboratory of Clinical Pathology, Ospedale S. Antonio, Tolmezzo, Italy

Corresponding author: Dr. Ignazio Brusca, “Buccheri La Ferla” Hospital, via Messina Marine 197, 90100 Palermo, Italy Phone: +39 091479271, Fax: +39 091479268

Citation Information: Clinical Chemistry and Laboratory Medicine. Volume 50, Issue 1, Pages 111–117, ISSN (Online) 1437-4331, ISSN (Print) 1434-6621, DOI: 10.1515/cclm.2011.714, September 2011

Publication History:

Received: 04/04/2011;
Accepted: 28/08/2011;
Published Online: 22/03/2012

Abstract

Background: In the diagnosis of celiac disease (CD), serum assays for anti-endomysium (EMA) and anti-transglutaminase (anti-tTG) antibodies have excellent diagnostic accuracy. However, these assays are less sensitive in young pediatric patients. Recently, a new ELISA test using deamidated gliadin peptides (DGP) as antigen has proved to be very sensitive and specific even in pediatric patients. In addition, anti-actin IgA antibodies (AAA) is another test that can be used in CD patients because antibody concentrations correlate with the degree of villous atrophy. This study evaluated the clinical accuracy of anti-tTG, EMA, AGA, anti-DGP and AAA and the effectiveness of these in different combinations for diagnosing CD in a large cohort of pediatric patients.

Methods: Sera of 150 children under 6 years of age were tested: 95 patients had a diagnosis of CD, while 55 patients who did not suffer from CD were used as controls. Anti-DGP IgA/IgG and AAA were assayed with ELISA kits, while anti-tTG IgA/IgG and AGA IgG/IgA were assayed using a quantitative fluoroimmunoassay. The EMA test was conducted by indirect immunofluorescence.

Results: Seventy-six of 95 (80%) CD patients were positive for DGP IgA and/or tTG IgA. Eighty of 95 (84.2%) patients were positive for DGP IgG and/or tTG IgA. None of the controls were positive for these antibodies. Eighty-four of 95 (88.4%) patients and 8/55 (14.5%) controls were positive for AAA and/or anti-tTG IgA.

Conclusions: In very young children, association of anti-tTG IgA with anti-DGP IgG is the best test combination for diagnosing CD, yielding a cumulative sensitivity of 84.2% and a specificity of 100%.

Keywords: actin; celiac disease; children; diagnostic accuracy; endomysium; gliadin; transglutaminase

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