Consequences of testing for celiac disease

Cranney, Ann; Rostom, Alaa; Sy, Richmond; Dubé, Catherine; Saloogee, Navaz; Garritty, Chantal; Moher, David; Sampson, Margaret; Zhang, Li; Yazdi, Fatemeh; Mamaladze, Vasil; Pan, Irene; MacNeil, Joanne

doi:10.1053/j.gastro.2005.02.019

« Previous Next »Gastroenterology
Volume 128, Issue 4, Supplement 1 , Pages S109-S120, April 2005

Consequences of testing for celiac disease

Ann Cranney
- Ottawa Health Research Institute, Ottawa, Canada
- Address requests for reprints to: Ann Cranney, MD, FRCPC, C402, Clinical Epidemiology Program, Ottawa Hospital Civic Campus, 1053 Carling Ave, Ottawa, Ontario, K1Y 4E9. fax: (613) 761-5492
Alaa Rostom
- Gastrointestinal Clinical Research Unit, Ottawa Hospital, Ottawa, Canada
Richmond Sy
- Gastrointestinal Clinical Research Unit, Ottawa Hospital, Ottawa, Canada
Catherine Dubé
- Gastrointestinal Clinical Research Unit, Ottawa Hospital, Ottawa, Canada
Navaz Saloogee
- Gastrointestinal Clinical Research Unit, Ottawa Hospital, Ottawa, Canada
Chantal Garritty
- Children’s Hospital of Eastern Ontario Research Institute, Ottawa, Canada
David Moher
- Children’s Hospital of Eastern Ontario Research Institute, Ottawa, Canada
- University of Ottawa, Ottawa, Ontario, Canada
Margaret Sampson
- Children’s Hospital of Eastern Ontario Research Institute, Ottawa, Canada
Li Zhang
- University of Saskatchewan, Saskatoon, Saskatchewan, Canada
Fatemeh Yazdi
- Children’s Hospital of Eastern Ontario Research Institute, Ottawa, Canada
Vasil Mamaladze
- Children’s Hospital of Eastern Ontario Research Institute, Ottawa, Canada
Irene Pan
- University of Ottawa, Ottawa, Ontario, Canada
Joanne MacNeil
- Gastrointestinal Clinical Research Unit, Ottawa Hospital, Ottawa, Canada

Population screening studies have identified that up to two thirds of celiac disease (CD) cases are asymptomatic. The aim of this study was to conduct a systematic review of the expected consequences of testing for CD in the following populations: (1) patients with symptoms suggestive of CD, (2) asymptomatic at-risk populations, and (3) general population. Standard systematic review methodology was used. A comprehensive literature search was conducted in MEDLINE (1996–2003), EMBASE (1974–2003), CAB (1972 forward), PsychINFO (1840–2003), AGRICOLA (1970–2003), and Sociological Abstracts (1963 forward); searches were conducted in December 2003. Pooled summary estimates were not calculated. The majority of the included studies were before-after studies, case control, or retrospective cohorts. The quality of evidence for the before-after studies is weaker. The overall strength of the evidence for this issue was fair to good. This area of research is relatively new, and further high-quality studies are required. The consequences of testing for celiac disease in symptomatic individuals appears to have a positive impact on patient-relevant outcomes. The data are less clear for those with silent CD or those with lower grade histologic lesions in small bowel biopsy. The literature suggests that compliance is less than ideal in these individuals, especially if diagnosed when adults. Long-term outcomes have not been extensively studied in those with silent CD.

Abbreviations used in this paper: AGA, antigliadin , AMA, arm muscle area , BMC, bone mineral content , BMD, bone mineral density , BMI, body mass index , CD, celiac disease , EMA, antiendomysial IgA antibody , FAI, fat area index , FN, femoral neck , GFD, gluten-free diet , HbA1c, hemoglobin A1c , IRR, incidence rate ratio , IUGR, intrauterine growth retardation , LS, lumbar spine , OR, odds ratio , PY, person years , SDS, standard deviation score , SMR, standardized mortality ratio , SSSF, suprascapular skin fold area , TSF, triceps skin fold , tTG, tissue transglutaminase IgA antibody , WHI, weight for height index