The prevalence of Coeliac disease is approximately one in a hundred individuals. The prevalence has been increasing over the past few decades. Individuals with other autoimmune disorders or first-degree relatives with Coeliac disease are more likely to be affected.

Coeliac disease is caused by a combination of genetic, dietary, and environmental factors. The genes most associated with Coeliac disease are Human Leukocyte Antigen (HLA) DQ2 and HLA-DQ8. These are both involved in proteins involved in the recognition of foreign particles by the immune system. All individuals affected by coeliac disease have a mutation in one of these genes. Genetic predisposition is necessary for the development of Coeliac disease but it is not sufficient. 

Another important factor in developing Coeliac disease is exposure to gluten. A molecule derived from gluten, gliadin, can damage the surface of the small intestine and make it more permeable. As a result, gliadin can the surface barrier on small intestine which exposes them to immune cells. In genetically predisposed individuals, the immune system will react to gliadin, leading to inflammation and further immune attack. These immune processes damage microscopic structures on the surface of the small intestine called villi. Villi are finger-like projections that increase the surface area of the small intestine and are responsible for the absorption of nutrients. Damage to these villi will reduce absorption and lead to symptoms associated with Coeliac disease.  Milk-feeding patterns and duration also seem to be involved in triggering Coeliac disease. Consumption of gluten-containing foods before three months of age increases the likelihood of developing Coeliac disease. Finally, certain bacterial infections have also been noted as a triggering factor.

Some individuals are affected by silent or asymptomatic Coeliac disease. These individuals have damaged intestinal villi but do not present any symptoms. The individuals affected by classical types exhibit digestive symptoms such as diarrhea, nausea, vomiting, bloating, abdominal pain, and constipation. Digestive symptoms are more common in children than in adults. In children, failure to thrive or slow physical growth is also common. In adults, sudden and unexplained weight loss is observed.  

Many adults are affected by the atypical type and experience symptoms unrelated to the gastrointestinal system. These include anemia due to iron deficiency, loss of bone density or osteoporosis, mouth ulcers, chronic headaches, delayed menarche, and dental enamel problems. Coeliac disease can also occur with dermatitis herpetiformis. This is a blistering skin disease that occurs on the elbows, knees, torso, scalp, and buttocks. 

In addition, malabsorption in children may also result in delayed puberty, irritability, and neurological symptoms such as attention-deficit and hyperactivity disorder (ADHD).

The first step in the diagnosis of Coeliac disease is blood tests. Antibodies are proteins released by the immune system in response to specific molecules that are identified as foreign. In Coeliac disease, certain antibodies are elevated in the blood. If these blood antibodies appear to be elevated, the next step and the most certain diagnostic test for Coeliac disease is biopsy. Genetic testing can also be performed in uncertain cases to confirm the diagnosis. The presence of HLA-DC2 or HLA-DQ8 can strengthen the diagnosis. 

Blood testing is the first step in the diagnosis of Coeliac disease. In this test, a blood sample is drawn and tested for the presence of specific antibodies using techniques that identify specific proteins. It is important to do this test prior to committing to a gluten-free diet because such a diet can lead to a reduction in antibody levels. 

The diagnostic standard for Coeliac disease is a biopsy. A biopsy is a procedure in which a sample of the affected tissue is removed and examined microscopically. In Coeliac disease, endoscopy is used to obtain a small sample from the small intestine. Endoscopy is a test in which a long tube with a small camera at the tip is inserted into the mouth and passed through the throat. The removed sample can be examined for the presence of villi damage and other characteristics of Coeliac disease.

If dermatitis herpetiformis is suspected, then a skin sample will be obtained and examined.

Currently, the only treatment that exists for Coeliac disease is a lifelong, gluten-free diet. Affected individuals must strictly avoid all dietary sources of gluten such as wheat, rye, and barley. This treatment is however not effective in individuals with refractory Coeliac disease. In such cases, immunosuppressive medications such as corticosteroids may be required to reduce the activity of the immune system and inflammation.  

If left untreated, Coeliac disease can lead to the development of many other conditions such as intestinal cancer and other autoimmune disorders such as type I diabetes. Compliance with a gluten-free diet is typically effective in symptom reduction and leads to the recovery of damaged intestinal surface within a few years. Prognosis also depends on the type of Coeliac disease. The refractory type is more difficult to manage is it does not respond to a gluten-free diet. 

Complying to a gluten-free diet can be challenging and a dietitian can help affected individuals plan a gluten-free diet that is healthy and satisfies their nutritional needs. Additionally, gluten contamination can occur in food sources that do not typically contain gluten. Therefore, being mindful about this contamination can be helpful. 

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