Celiac Disease

Celiac disease is an autoimmune condition where eating gluten damages the small intestine. It can cause stomach symptoms—or none at all—while silently leading to nutrient deficienciesanemiabone loss, and other issues. A proactive testing plan starts with the right blood tests while you are still eating gluten. The standard first step is tissue transglutaminase IgA (tTG-IgA) paired with total serum IgA to check for IgA deficiency. If IgA is low, tests that use IgG (such as tTG-IgG or deamidated gliadin peptide [DGP] IgG) are used instead. Highly specific endomysial antibody (EMA-IgA) can confirm positive results.

When bloodwork suggests celiac disease, your clinician may confirm with a small-bowel (duodenal) biopsy. Genetic testing for HLA-DQ2/DQ8 cannot diagnose celiac disease, but it can virtually rule it out if both are absent. After diagnosis—or if strongly suspected—baseline nutrient panels help find and monitor deficiencies. Lab results guide next steps but do not replace a clinician’s exam or gastroenterology care.

Signs, Symptoms & Related Situations

  • Digestive: bloating, abdominal pain, diarrhea, constipation, weight loss, foul-smelling or bulky stools

  • Nutritional: iron-deficiency anemia, low folate or B12, low vitamin D, unintentional weight loss

  • Bone & skin: bone pain, fractures, early osteoporosis/osteopenia; dermatitis herpetiformis (itchy, blistering rash)

  • General & neurologic: fatigue, headaches, brain fog, peripheral neuropathy

  • Reproductive: infertility, recurrent miscarriage, delayed growth or short stature in children

  • Associated autoimmune clues: type 1 diabetes, autoimmune thyroid disease

  • Urgent care: severe dehydration, black or bloody stools, fainting—seek immediate help
    All symptoms should be evaluated by a qualified clinician.

Why These Tests Matter

What testing can do

  • Screen and triage: identify antibody patterns consistent with celiac disease

  • Guide confirmation: help decide when endoscopy/biopsy is appropriate

  • Baseline and monitor: uncover nutrient deficits and track recovery after going gluten-free

What testing cannot do

  • Diagnose celiac disease after gluten has been removed from the diet (antibodies can normalize)

  • Replace endoscopic biopsy when confirmation is required

  • Detect non-celiac gluten sensitivity (these tests do not diagnose NCGS or wheat allergy)

What These Tests Measure (at a glance)

  • tTG-IgA (tissue transglutaminase IgA): first-line screen with high sensitivity/specificity if total IgA is normalCaveat: must be on a gluten-containing diet.

  • Total IgA: checks for IgA deficiency (more common in celiac). Caveat: if low, switch to IgG-based tests.

  • tTG-IgG / DGP-IgG (± DGP-IgA): useful when IgA deficient or in young children; DGP can add sensitivity in pediatrics. Caveat: interpret with clinical context.

  • EMA-IgA (endomysial antibody): very specific; often used to confirm positive tTG. Caveat: more expensive and operator-dependent.

  • HLA-DQ2/DQ8 genotyping: necessary but not sufficient for celiac; absence of both strongly argues againstdisease. Caveat: positive genotype is common in the general population.

  • Nutrient/impact profile: ferritin/ironfolatevitamin B1225-OH vitamin DzinccalciumalbuminCBCCMP, ± TSH/thyroid antibodies (autoimmune overlap). Caveat: abnormalities reflect malabsorption or co-conditions, not proof of celiac.

How the Testing Process Works

  1. Start on gluten: confirm you are eating gluten daily for several weeks before testing unless your clinician advises otherwise.

  2. Order initial screen: tTG-IgA + total IgA (reflex to tTG-IgG/DGP-IgG if IgA deficient). Consider EMA-IgA for confirmation.

  3. Add context labs: CBC, CMP, ferritin/iron, folate, B12, vitamin D, zinc; consider TSH/thyroid antibodies if indicated.

  4. Review & confirm: if serology suggests celiac, your clinician may arrange duodenal biopsy; consider HLA-DQ2/DQ8 when results are equivocal or if already gluten-free.

  5. Monitor recovery: after diagnosis and a gluten-free diet, repeat tTG-IgA (or DGP-IgG) and nutrient labs to track improvement.

Interpreting Results (General Guidance)

  • Positive tTG-IgA (normal total IgA) ± positive EMA-IgA strongly supports celiac disease; referral for biopsy is common.

  • Negative tTG-IgA with high suspicion: check total IgA; if low, use IgG-based DGP/tTG; consider HLA typingor biopsy per clinician.

  • Already gluten-free? Serology may be falsely negative; your clinician may discuss HLA testing or a supervised gluten challenge.

  • After diagnosis: antibody levels typically fall over months on a strict gluten-free diet; persistent elevation suggests ongoing gluten exposure or another issue.
    Always interpret results with a qualified healthcare professional.

Choosing Panels vs. Individual Tests

  • First-line screening (adults & most children): tTG-IgA + total IgA, with reflex to tTG-IgG/DGP-IgG if IgA deficient.

  • High-specificity confirmation: add EMA-IgA when tTG is positive or equivocal.

  • Equivocal/complex cases or already gluten-free: HLA-DQ2/DQ8 to help rule out disease; discuss biopsy or gluten challenge with your clinician.

  • Baseline/ongoing impact: CBC, ferritin/iron, folate, B12, vitamin D, zinc, CMP; repeat to document recovery.

  • Pediatrics: DGP (especially DGP-IgG) can improve sensitivity in children under 2; follow pediatric guidelines.

FAQs

Do I need to be eating gluten for these tests to work?
Yes. Most antibody tests require a gluten-containing diet for several weeks before testing.

Can a blood test diagnose celiac by itself?
Blood tests can be highly suggestive. Many patients still need endoscopic biopsy to confirm.

What if I’m IgA deficient?
Your clinician will use IgG-based tests such as tTG-IgG or DGP-IgG.

Does genetic (HLA) testing diagnose celiac disease?
No. DQ2/DQ8 positivity is common; absence of both makes celiac very unlikely.

How long until antibodies normalize after going gluten-free?
They usually fall over 6–12 months (sometimes longer). Your clinician sets the re-test schedule.

Is non-celiac gluten sensitivity detected by these tests?
No. These labs evaluate celiac disease, not NCGS or wheat allergy.

Internal Links & Cross-References

  • Digestive System Tests Hub

  • Irritable Bowel Evaluation

  •  Lactose Intolerance

  • H. pylori

  • Inflammatory Bowel Disease (IBD)

  • Nutrient Deficiency Panels

  • Key Lab Tests: tTG-IgA • Total IgA • EMA-IgA • DGP-IgA/IgG • tTG-IgG • HLA-DQ2/DQ8 • Ferritin/Iron • Folate • Vitamin B12 • Vitamin D • Zinc • CBC • CMP • TSH/Thyroid Antibodies

References

  1. American College of Gastroenterology. Clinical Guidelines for the Diagnosis and Management of Celiac Disease.

  2. American Gastroenterological Association. Technical Review and Clinical Practice Update on Celiac Disease.

  3. European Society for Paediatric Gastroenterology, Hepatology and Nutrition (ESPGHAN). Guidelines for Pediatric Celiac Disease.

  4. British Society of Gastroenterology. Celiac Disease Guidelines.

  5. National Institute of Diabetes and Digestive and Kidney Diseases. Celiac Disease—Overview and Testing.

  6. Celiac Disease Foundation. Physician Resources on Diagnosis and Management.

  7. National Institute for Health and Care Excellence (NICE). Coeliac Disease: Recognition, Assessment, and Management.

Available Tests & Panels

Your celiac disease test menu is pre-populated in the Ulta Lab Tests system. Start with tTG-IgA + total IgA (reflex to tTG-IgG/DGP-IgG if IgA deficient), add EMA-IgA for confirmation when needed, and use HLA-DQ2/DQ8 in equivocal or gluten-free cases. Include nutrient panels at baseline and for follow-up. Review all results with your clinician.

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The Milk Component Panel measures IgE antibodies to alpha-lactalbumin (F76), beta-lactoglobulin (F77), and casein (F78), the major milk proteins linked to allergic reactions. Elevated levels may confirm cow’s milk allergy, which can cause hives, digestive upset, or anaphylaxis. Doctors use this test to identify specific milk protein sensitivities, guide dietary restrictions, and support management of food allergies in children and adults.

Also Known As: Milk Allergy Panel, Milk Allergy Test

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Celiac disease is an autoimmune disorder that disrupts the body's ability to digest gluten. Gluten is a dietary protein in wheat products; the disease also affects some related proteins found in barley and rye. Celiac causes the small intestine to become inflamed when exposed to gluten; the inflammation can damage or destroy the intestine's lining.

The intestinal wall is studded with villi, projecting folds of tissue that increase the surface area available to absorb nutrients (including vitamins, fluids, minerals, and electrolytes) from food. When a person with celiac disease eats gluten, it triggers the body's immune system. Immune cells will attack the intestinal villi. This immune response usually, but not always, involves the production of auto-antibody proteins by the immune system.

The harmful immune response and autoantibody production will continue if the individual is exposed to gluten and the other relevant proteins. Over time, the immune system can do enough damage to the intestinal villi to reduce the body's ability to absorb nutrients. This results in the affected person developing symptoms associated with malnutrition.

Celiac disease occurs all over the world, with individuals of European descent being more likely to experience it. In the United States, celiac disorder occurs at a rate of one case in 100 to 150 individuals. Women are slightly more susceptible than men. While celiac can develop at any age, it is mostly seen in infants or people between 30 and 50 years of age.

Adult celiac disease was much less common at one time, and infant celiac disease was much more serious. The disease's demographics have changed, with the frequency of adult cases growing more abundant in recent years.

The celiac disorder is an inherited condition, but it appears that some event — physical, environmental, or psychological — is required to trigger the disease. The mechanism that causes celiac to manifest is not yet fully understood by doctors.

Data from the National Digestive Diseases Information Clearinghouse points out the genetic component of celiac disease. The celiac disorder is more common among the first-degree relatives (parents, children, and siblings) of individuals who already have it. The celiac disorder occurs in approximately 4 to 12 percent of first-degree relatives of those who already have it.

Celiac Disease Symptoms

Researchers estimate that there may be as many as 20 million people with celiac worldwide, with two to three million of them in the United States. Exact figures are difficult to come by as 90 percent of people with celiac disorder in the US go undiagnosed. One fact that makes the disease hard to pin down is that individual sufferers' symptoms vary widely.

How celiac disorder manifests tends to vary based on age and physical development. Digestive symptoms are more common in infants and children. At the same time, adult sufferers tend to experience symptoms affecting other parts of the body. The symptoms of celiac disease can also be caused by many other medical conditions, such as a food allergy. This leads to many cases going undiagnosed for years.

These are all common symptoms of celiac disease:

  • Abdominal bloating and pain
  • Chronic constipation or diarrhea
  • Vomiting
  • Greasy, foul-smelling stool
  • Susceptibility to bruising and bleeding
  • Pain in bones and joints
  • Fatigue
  • Mental focus problems
  • Oral ulcers
  • Dental enamel defects
  • Osteoporosis
  • Weight Loss
  • Anemia/iron deficiency that cannot be corrected via supplements

Celiac disorder can retard growth and development, delay puberty, and cause short stature in children. Adults with celiac disease may suffer from reproductive issues, including infertility.

People living with Celiac disease also often develop dermatitis herpetiformis, a skin condition that raises itchy blisters.

Celiac disorder is associated with an increased risk of developing intestinal lymphoma (cancer).

Testing For Celiac Disease

The first step in making a celiac disease diagnosis is to test for the presence of specific autoantibodies associated with the condition. A biopsy is performed to confirm the diagnosis if auto-antibody tests suggest celiac disease's presence. Further auto-antibody testing can be used to monitor the progression of celiac disease and its treatment, which is often done for symptomatic patients. Auto-antibody testing can also be used to screen relatives after one family member has been diagnosed.

There are two classes of intestinal autoantibodies that can be detected, IgA and IgG. IgA tests are more specific, leading to them being heavily preferred in diagnosing celiac disease. IgA is the most common antibody found in gastrointestinal secretions. IgG tests are still useful because a small fraction of celiac disease patients (two to three percent) also have an IgA deficiency.

Common IgA tests for celiac disease include the following:

Testing for anti-tTG antibodies in the blood is the most sensitive and specific way to detect celiac disease, so this is usually the first test performed. There is a less-sensitive test for anti-tTG in the IgG class; this usually is only used if the individual is IgA-deficient.

This test is often included in the celiac testing process because it will detect the presence of an IgA deficiency.

People with celiac disease who test negative for anti-tTG may test positive for DGP. This test is especially effective at diagnosing celiac disease in young children.

The American College of Gastroenterology recommends performing both DGP IgGtesting and anti-tTG IgG testing for any patients with low IgA levels.

There are additional auto-antibody tests that are less commonly used to diagnose the celiac disorder. These include:

  • Anti-Endomysial Antibodies (EMA)

This test can provide clarification if initial test results are inconclusive. EMA tests are difficult to perform when compared with anti-tTG tests.

  • Anti-Reticulin Antibodies (ARA)

ARA testing is surpassed by all the above tests for specificity and sensitivity. Thus, it is rarely ordered today.

As noted above, a celiac disorder diagnosis is generally confirmed by performing a biopsy on the small intestine. This can directly detect any damage to the intestinal villi. See the article on Histopathology for more information on biopsies.

There are genetic tests that can detect markers associated with celiac disease, but these are not used routinely. The key markers for celiac disease are the Human Leukocyte Antigen (HLA) markers DQ2 and DQ8. Genetic testing may be ordered for patients whose other test results are inconclusive and for screening family members in high-risk categories.

Genetic tests cannot make a conclusive diagnosis of celiac disease. The markers mentioned above are carried by roughly 30 percent of the general population, most of whom do not have the condition. Negative genetic results are useful, though, because they can rule out celiac disorder for individuals with inconclusive results on other tests (including biopsies).

Additional tests may be used to evaluate the extent of the disease and patients' symptoms. Examples include:

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