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Celiac disease

Changed by Amir Rezaee, 23 Sep 2015

Updates to Article Attributes

Body was changed:

Coeliac disease (also sometimes termedalso known asnon tropical sprue 6) is is a T cell mediated autoimmune chronic gluten intolerance condition characterised by loss of gastrointestinal villi in the proximal small bowel and gastrointestinal malabsorption (sprue) that results from the small intestine's response to dietary gluten.

It should always be be considered as thea possible underlying aetiology in cases of Iron deficiency anaemia of uncertain cause.

DemographicsEpidemiology

Coeliac disease is relatively common in Caucasians, 1 in 200, but it is extremely rare in asians or black people. There are two peaks of presentation, small number of patients present early in childhood and clinicalthe second more common group of patients presents at 3rd and 4th decade. 

Clinical presentation

Many patients have paucity of symptoms with no GI upset. However, abdominal pain is considered the most common symptoms. Other findings include:

  • iron deficiency anaemia and while the condition is relatively common (1 in 200 of the general population), the majority of patients will be adult when the diagnosis is made. There may a slight female predilection.guaiac-positive stools 
  • diarrhea
  • constipation
  • malabsorption including fat soluble vitamins
  • weight loss

Pathology

Coeliac disease is a chronic autoimmune disease induced in genetically susceptible individuals after ingestion of  glutengluten. Small bowel mucosa is primarily affected (submucosa, muscularis and serosa remain normal), resulting in progressive degrees of villous inflammation and destruction (which starts in duodenum and extends into ilium) with resulting of induction crypt hyperplasia. Loss of villi, which absorbs fluid, and hypertophy of crypts, which produce fluid , result in fluid excess in the small bowel lumen 8.  

The villous atrophy that occurs within the bowel also results in malabsorption of iron, folic acid, calcium and fat soluble vitamin resulting in a variety of signs, some of which may be non-specific.

The gold standard diagnostic test is a duodenal biopsy taken at UGIE.

Histological features include:

  • total villous loss (initially, initially blunting progressing to flattened mucosa).
  • hyperplasia of the crypts 
  • epithelial infiltration with T cell lymphocytes
    •

Additionally, serum endomysial antibodies antibodies may be raised:

  • anti-tissue transglutaminase antibody (anti-tTG), IgA
  • deamidated gliadin peptide (DGP) antibodies, IgA
  • anti-endomysial antibodies (EMA), IgA class
  • anti-reticulin antibodies (ARA), IgA class

Quantitative immunoglobulin A (IgA): measures the total level of IgA in the blood to determine if someone is deficient in the IgA class of antibodies. The IgG class of anti-tTG may be ordered for people who have a deficiency of IgA.

Associations

Radiographic features

Fluoroscopy (barium follow through)

Features of small bowel barium studies are not sensitive enough for confident diagnosis, but some changes may be seen:

CT enterocolysis

Features present on CT enterocolysis may include 3,6:

  • reversed jejunoileal fold pattern: thought to have the highest specificity is considered the most discriminating independent variable for the diagnosis of uncomplicated coeliac disease
  • ileal fold thickening
  • vascular engorgement
  • prominent mesenteric lymph nodes , may cavitate with fluid fat level
  • submucosal fat deposition in long standing cases
  • other adjunctive features

Complications

  • -<p><strong>Coeliac disease</strong> (also sometimes termed as <strong>non tropical sprue </strong><sup>6</sup>) is a condition of gastrointestinal malabsorption (<a href="/articles/sprue">sprue</a>) that results from the small intestine's response to dietary gluten.</p><p>It should always be considered as the possible underlying aetiology in cases of <a href="/articles/iron-deficiency-anaemia">Iron deficiency anaemia</a> of uncertain cause.</p><h4>Demographics and clinical presentation</h4><p>Many patients have paucity of symptoms with no GI upset and while the condition is relatively common (1 in 200 of the general population), the majority of patients will be adult when the diagnosis is made. There may a slight female predilection.</p><h4>Pathology</h4><p>Coeliac disease is a chronic autoimmune disease induced in genetically susceptible individuals after ingestion of  gluten. Small bowel mucosa is primarily affected (submucosa, muscularis and serosa remain normal), resulting in progressive degrees of villous inflammation and destruction (which starts in duodenum and extends into ilium) with resulting of induction crypt hyperplasia. Loss of villi, which absorbs fluid, and hypertophy of crypts, which produce fluid , result in fluid excess in the small bowel lumen <sup>8</sup>.  </p><p>The villous atrophy that occurs within the bowel also results in <a href="/articles/malabsorption">malabsorption</a> of iron, folic acid, calcium and fat soluble vitamin resulting in a variety of signs, some of which may be non-specific.</p><p>The gold standard diagnostic test is a duodenal biopsy taken at UGIE. Histological features include total villous loss (initially blunting progressing to flattened mucosa). Additionally, serum endomysial antibodies may be raised.</p><h5>Associations</h5><ul><li>
  • +<p><strong>Coeliac disease</strong> also known as <strong>non tropical sprue </strong><sup>6</sup> is a T cell mediated autoimmune chronic gluten intolerance condition characterised by loss of villi in the proximal small bowel and gastrointestinal malabsorption (<a href="/articles/sprue">sprue</a>).</p><p>It should always be considered as a possible underlying aetiology in cases of <a href="/articles/iron-deficiency-anaemia">Iron deficiency anaemia</a> of uncertain cause.</p><h4>Epidemiology</h4><p>Coeliac disease is relatively common in Caucasians, 1 in 200, but it is extremely rare in asians or black people. There are two peaks of presentation, small number of patients present early in childhood and the second more common group of patients presents at 3rd and 4th decade. </p><h4>Clinical presentation</h4><p>Many patients have paucity of symptoms with no GI upset. However, abdominal pain is considered the most common symptoms. Other findings include:</p><ul>
  • +<li>iron deficiency anaemia and guaiac-positive stools </li>
  • +<li>diarrhea</li>
  • +<li>constipation</li>
  • +<li>malabsorption including fat soluble vitamins</li>
  • +<li>weight loss</li>
  • +</ul><h4>Pathology</h4><p>Coeliac disease is a chronic autoimmune disease induced in genetically susceptible individuals after ingestion of gluten. Small bowel mucosa is primarily affected (submucosa, muscularis and serosa remain normal), resulting in progressive degrees of villous inflammation and destruction (which starts in duodenum and extends into ilium) with resulting of induction crypt hyperplasia. Loss of villi, which absorbs fluid, and hypertophy of crypts, which produce fluid , result in fluid excess in the small bowel lumen <sup>8</sup>.  </p><p>The villous atrophy that occurs within the bowel also results in <a href="/articles/malabsorption">malabsorption</a> of iron, folic acid, calcium and fat soluble vitamin resulting in a variety of signs, some of which may be non-specific.</p><p>The gold standard diagnostic test is a duodenal biopsy taken at UGIE.</p><p>Histological features include:</p><ul>
  • +<li>total villous loss, initially blunting progressing to flattened mucosa</li>
  • +<li>hyperplasia of the crypts </li>
  • +<li>epithelial infiltration with T cell lymphocytes</li>
  • +</ul><p>Additionally, serum antibodies may be raised:</p><ul>
  • +<li>anti-tissue transglutaminase antibody (anti-tTG), IgA</li>
  • +<li>deamidated gliadin peptide (DGP) antibodies, IgA</li>
  • +<li>anti-endomysial antibodies (EMA), IgA class</li>
  • +<li>anti-reticulin antibodies (ARA), IgA class</li>
  • +</ul><p>Quantitative immunoglobulin A (IgA): measures the total level of IgA in the blood to determine if someone is deficient in the IgA class of antibodies. The IgG class of anti-tTG may be ordered for people who have a deficiency of IgA.</p><h5>Associations</h5><ul>
  • +<li>
  • -</li></ul><h4>Radiographic features</h4><h5>Fluoroscopy (barium follow through)</h5><p>Features of small bowel barium studies are not sensitive enough for confident diagnosis, but some changes may be seen:</p><ul>
  • +</li>
  • +<li>dermatitis herpetiformis</li>
  • +<li>IgA deficiency</li>
  • +<li><a href="/articles/cavitatory-mesenteric-lymph-node-syndrome">cavitatory lymph node syndrome</a></li>
  • +</ul><h4>Radiographic features</h4><h5>Fluoroscopy (barium follow through)</h5><p>Features of small bowel barium studies are not sensitive enough for confident diagnosis, but some changes may be seen:</p><ul>
  • -<li>non-obstructing <a href="/articles/intussusception">intussusception</a>
  • +<li>multiple non-obstructing <a href="/articles/intussusception">intussusception</a>
  • +<li>prominent mesenteric lymph nodes , may cavitate with fluid fat level</li>
  • +<li>submucosal fat deposition in long standing cases</li>
  • -<li>increased risk of malignant conditions such as <a href="/articles/small-bowel-lymphoma-1">small bowel lymphoma</a><a href="/articles/small-bowel-lymphoma-"> </a>(mainly T cell type) and <a href="/articles/small-bowel-adenocarcinoma">small bowel adenocarcinoma</a>.</li>
  • -<li>
  • -<a href="/articles/hyposplenism">hyposplenism</a> <sup>1</sup>
  • +<li>increased risk of malignant conditions such as <a href="/articles/small-bowel-lymphoma-1">small bowel lymphoma</a><a href="/articles/small-bowel-lymphoma-"> </a>(mainly T cell type) and <a href="/articles/small-bowel-adenocarcinoma">small bowel adenocarcinoma</a>
  • -<li>increase risk of development of <a href="/articles/carcinoma-of-the-oesophagus-1">carcinoma of oesophagus</a>
  • +<li>increase risk of development of <a href="/articles/oesophageal-carcinoma-1">carcinoma of oesophagus</a>
  • -<a href="/articles/cavitatory-mesenteric-lymph-node-syndrome">cavitatory lymph node syndrome</a><a href="/articles/cavitating-mesenteric-lymphadenopathy-syndrome"> </a><sup>1-2</sup>
  • +<a href="/articles/cavitatory-mesenteric-lymph-node-syndrome">cavitatory lymph node syndrome</a><a href="/articles/cavitating-mesenteric-lymphadenopathy-syndrome"> </a><sup>1-2</sup><ul><li>
  • +<a href="/articles/hyposplenism">hyposplenism</a> <sup>1</sup>
  • +</li></ul>

References changed:

  • 9. Bürgin-Wolff A, Gaze H, Hadziselimovic F et al. Antigliadin and Antiendomysium Antibody Determination for Coeliac Disease. Arch Dis Child. 1991;66(8):941-7. <a href="https://doi.org/10.1136/adc.66.8.941">doi:10.1136/adc.66.8.941</a> - <a href="https://www.ncbi.nlm.nih.gov/pubmed/1819255">Pubmed</a>
  • 10. Vinay Kumar, Abul K. Abbas, Jon C. Aster. Robbins and Cotran Pathologic Basis of Disease. (2014) ISBN: 9781455726134 - <a href="http://books.google.com/books?vid=ISBN9781455726134">Google Books</a>

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