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  • Scott Adams
    Scott Adams

    Interpretation of Celiac Disease Blood Test Results

    Reviewed and edited by a celiac disease expert.
    Interpretation of Celiac Disease Blood Test Results - Images: CC--Scott Robinson
    Caption: Images: CC--Scott Robinson

    The following detailed explanation of serological tests for celiac disease was written by Tom Ryan, Technical Service Specialist, INOVA Diagnostics, Inc.

    There has been a lot of discussion about serological testing for celiac disease recently, specifically regarding tTG (tissue Transglutaminase) testing. I will try to answer some of the many questions that have appeared on this list about all of the tests. First, and this applies to any of the blood tests, you must currently be on a gluten containing diet for the tests to be accurate. Antibodies are produced by the immune system in response to substances that the body perceives as threatening. The immune response that your body produces is its response to being exposed to gluten in the diet and its subsequent effect on the intestinal mucosa. If there is no gluten in the diet, then there is no response that we can measure. A brief change in diet will not have a noticeable effect. If you have been gluten free for a week or so, it will not make any great difference. The response might be marginally less but the difference is insignificant because the body has not had time to respond to the change. Conversely, if you have been gluten free for a protracted period of time and decide to be tested, a brief challenge of a couple of weeks is not enough to elicit a response and get an accurate test.

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    There are several steps that take place to generate an immune response and it takes time both for the positive reaction when gluten is present and to clear the antibodies when gluten is eliminated. There has been a great deal of discussion about how much and how long a challenge should be and there is no consensus. Talk with your Doctor. My personal feeling is that the minimum is 2 slices of bread per day for 6 weeks to get an accurate test but I would not try to second-guess the Doctor. There are basically four tests that can be performed to aid in diagnosing celiac disease. Notice that I say they will aid in diagnosing celiac disease. Immunology is fairly accurate but it is far from being an exact science. All of the lab tests, regardless of the type or source, are presented as aids to diagnosis. They should not be used alone as a basis for diagnosis but rather are intended to be considered in conjunction with the physical examination of the patient as well as the reported symptoms, etc. by a trained physician. There has been a great deal of confusion about what the tests are and I hope to alleviate some of the misunderstandings. There are many terms that we hear. tTG, IgA, IgG, ELISA, etc. What are all of these? Some contributors to the list make reference to the IgA or IgG test or to the ELISA test. These labels are incomplete for our purposes and could be referring to any number of different tests.

    We all have, within our bodies, a family of closely related although not identical proteins which are capable of acting as antibodies. These are collectively referred to as immunoglobulins. Five major types of immunoglobulins are normally present in the human adult. They are IgG, IgA, IgM, IgE and IgD. Each of these is a shorthand way of writing immunoglobulin gamma G (or A or M, etc.) and they each perform a different function in our systems. IgG is the principal immunoglobulin in human serum. It is important in providing immunity in a developing fetus because it will pass across the placental barrier. IgA is the principal immunoglobulin in secretions from respiratory and intestinal mucosa. IgE is a gamma globulin produced by cells lining the intestinal and respiratory tracts. It produces the antibodies associated with most hypersensitivity (allergic) responses. It is associated with asthma, hay fever, etc. IgM is a globulin formed in almost every immune response in the early part of the reaction. IgD is a rare protein present in normal sera in a tiny amount. These designations refer to the type of protein that is carrying the antibody in question. Both IgG and IgA subtypes of anti-gliadin antibody are produced, hence we refer to them as IgG gliadin or IgA gliadin. Collectively they are anti-gliadin antibodies.

    Anti-Gliadin Antibodies:

    Both IgA and IgG anti-gliadin antibodies (AGA) are detected in sera of patients with gluten sensitive enteropathy (celiac disease). IgG anti-gliadin antibodies are more sensitive but are less specific markers for disease compared with IgA class antibodies. IgA anti-gliadin antibodies are less sensitive but are more specific. In clinical trials, the IgA antibodies have a specificity of 97% but the sensitivity is only 71%. That means that, if a patient is IgA positive, there is a 97% probability that they have celiac disease. Conversely, if the patient is IgA negative, there is only a 71% probability that the patient is truly negative for celiac disease. Therefore, a positive result is a strong indication that the patient has the disease but a negative result does not necessarily mean that they don not have it. False positive results are rather uncommon but false negative results can occur. On the other hand, the IgG anti-gliadin antibodies are 91% specific and have an 87% sensitivity. This means that they will show positive results more readily but there is not as strong a correlation with celiac disease. It is less specific. Patients with other conditions but not afflicted with celiac disease will occasionally show positive results. IgG anti-gliadin antibodies are detectable in approximately 21% of patients with other gastrointestinal disorders. This test might yield false positive results but is less likely to yield false negative results.

    A sensitive testing protocol includes testing for both IgA and IgG anti-gliadin antibodies since a significant portion of celiac patients (approx. 2-5%) are IgA deficient. This combined IgA and IgG anti-gliadin antibody assay has an overall sensitivity of 95% with a specificity of 90%. The type of test used to detect the anti-gliadin antibodies is called an ELISA. This is an acronym and it stands for Enzyme Linked Immuno-Sorbent Assay. ELISA is not a test in itself. It is a method of testing and it is a relatively simple test to perform. It involves putting a measured amount of diluted patient serum into the wells of a specially constructed and prepared plate and incubating it for a period of time with various chemicals. The end result is a color change, the intensity of which is dependent upon the concentration of anti-gliadin antibody (or other protein being measured) in the patient serum. The ability of this colored solution to absorb light at a particular wavelength can be measured on a laboratory instrument and mathematically compared with solutions that contain a known amount of anti-gliadin antibody to arrive at a number for the amount of antibody present. The sample can then be classified as negative, (0-20 units); weak positive, (21-30 units); or moderate to strong positive if greater than 30 units. The purpose of testing for anti-gliadin antibodies includes, in addition to diagnosis of gluten sensitive enteropathy, monitoring for compliance to a gluten free diet. IgA gliadin antibodies increase rapidly in response to gluten in the diet and decrease rapidly when gluten is absent from the diet. The IgA anti-gliadin antibodies can totally disappear in 2-6 months on a gluten free diet, so they are useful as a diet control. By contrast, IgG anti-gliadin antibodies need a long time, sometimes more than a year, to become negative. The reverse is also true. That is, a patient with celiac disease who has been on a gluten free diet and tests negative for IgA anti-gliadin antibodies, will show a rapid increase in antibody production when challenged by gluten in the diet. Approximately 90% of challenged patients will yield a positive IgA anti-gliadin result within 14-35 days after being challenged. The IgG antibodies are somewhat slower.

    Endomysial Antibodies:

    IgA class anti-endomysial antibodies (AEA) are very specific, occurring only in celiac disease and DH. These antibodies are found in approximately 80% of patients with DH and in essentially 100% of patients with active celiac disease. IgA endomysial antibodies are more sensitive and specific than gliadin antibodies for diagnosis of celiac disease. Antibody titers (dilutions) are found to parallel morphological changes in the jejunum and can also be used to reflect compliance with gluten-free diets. Titers decrease or become negative in patients on gluten free diets and reappear upon gluten challenge.

    The test for anti-endomysial antibodies is more subjective and more complicated for the lab to perform than the anti-gliadin assays. It involves serially diluting some of the patients serum, that is, diluting it by ½ then ¼, 1/8, 1/16, etc. and putting these dilutions on a glass slide that has some sort of tissue affixed to it. The slide is then processed with various solutions and examined under a fluorescent microscope to determine if any of that serum binds to any of the proteins in the tissue. If so, then that patient is confirmed as having antibodies to that particular protein. This method of testing is called an IFA or sometimes IIFA. It stands for Indirect Immuno-Fluorescent Assay. The selection of which tissue slide to use is determined by what specific protein, hence which antibody, you are specifically looking for. Endomysial antibodies react with the endomysium, which is a sheath of reticular fibrils that surround each muscle fiber. Therefore, to detect endomysial antibodies, you would want to use a tissue substrate that contains a lot of muscle tissue. The substrate used most often for this assay is distal sections of the esophagus. These are very thinly sliced and fixed to the slide. They contain muscle fibers and not much else so there is a lot of endomysium available to react with the anti-endomysial antibodies.

    Reading this test involves viewing the reacted slides with a fluorescent microscope to make the determination. This requires a highly skilled and trained eye and, of necessity, is somewhat subjective. You are looking for a green fluorescence in the endomysium covering the muscle fibers. The test is reported as the titer or final dilution in which the fluorescence can still clearly be seen. As you can imagine, this is very subjective. There are no standardized values and it is up to the judgment of the particular technician what the endpoint titer is. Recently, (1998) the endomysial antigen targeted by the anti-endomysial antibodies was identified as the protein cross-linking enzyme known as tissue transglutaminase (tTG). This has enabled the production of an antigen specific ELISA assay incorporating tTG as a reliable and objective alternative to the traditional and subjective Immunofluorescence based assays. In clinical trials, the correlation with the endomysial IFA assay has been shown to be close to 100%. This is a test that has been very well received in the professional community. It is an ELISA, like the anti-gliadin antibody test and, as such, is not subject to interpretation like the IFA. That is the greatest advantage to this new test! With this or any ELISA, the response is measured on an instrument that calculates the amount of light of a particular wavelength that is absorbed by the solution and prints out a numerical result. There is no chance of human error skewing the results because there is no judgment call involved. The ELISA plate, regardless of what you are testing for, is processed with at least three control sera (sometimes as many as eight) in addition to the unknown sample being tested. There is a negative serum and at least two positive sera containing different levels of the antibody being tested. There are specific requirements for the absorption levels of these three controls. That is, each of them has a minimum or maximum (or both) number that must be seen by the instrument in order for it to be a valid test. If there is any variance from these expected numbers, it is an indication that something went wrong and the test results are discarded and the test repeated. There is therefore no way the technician could report inaccurate results, (assuming they diluted the sample correctly). Either the test was valid, and you can rely upon the accuracy of the result, or the test is invalid, and the entire result discarded. If any error was made during the processing of the ELISA plate, it would result in the control sera numbers being out of range and the entire test result would be thrown out.

    In summary, the tTG ELISA is measuring the same thing that the endomysial IFA is measuring but with a method that is more sensitive and specific and not subject to interpretation. IgA class Reticulin antibodies are found only in Celiac disease and dermatitis herpetiformis. These antibodies are found in approximately 60% of celiac disease patients and 25% of DH patients. This test is falling into disuse because of the limited utility and the availability of better tests. It is an IFA performed on a tissue substrate with all the attendant problems that go along with it. The development of all of these serum assays has tremendously simplified the diagnosis of celiac disease and improved the accuracy as well. The original criteria for diagnosis according to the European Society for Pediatric Gastroenterology and Nutrition, (ESPGAN), involved a year of arduous studies with:

    • An initial positive gut biopsy;
    • 6 months on a gluten free diet;
    • A second, negative gut biopsy;
    • A gluten challenge for 6 months and;
    • A third, positive gut biopsy. The revised ESPGAN criteria call for positive results in two of the serological tests confirmed by a single positive biopsy. In practice, many gastroenterologists are utilizing the serologies in conjunction with a controlled diet and the clinical presentation to form a basis for diagnosis without the need for the invasive procedure.

    Through the auspices of the Celiac Disease Foundation and others, a professional symposium and workshop was organized earlier this year in Marina Del Rey, California with participants from Europe as well as the U.S. to establish standards for reporting test results. This should improve testing and diagnosis even more. At the conclusion of this conference a Celiac Disease Standardization Committee was formed to investigate and make recommendations on a standardized method of reporting results.



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    Guest Audrey
    Very good article for us laymen. I am having the testing done in 2 days. I wasn't told whether or not to fast for the test.

    My doctor said doing it right means fasting.

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    Guest Lynn

    I am awaiting results from my test. Also having colonoscopy done. I have had awful allergies/asthma all my life. This last 3 weeks I've had horrific diarrhea. I have had spells of that but normally only 1-2 days. Afraid to travel because no control. Started not eating gluten today. And yes it happened to me on a second date in the car. I'm hoping this will clear it up!!!!

    This article was wonderful because now I know what the test means. Thanks.

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    Guest Mike
    Megan -- I am just now reading your post. Just because a person has an M.D. after his or her name does not indicate at which level he or she was graduated from Medical School. You know 1/2 of the class graduated under the 50% mark. I also have several university degrees -- however, none of them in medicine, but I was educated in how to think. On top of that I am a human being with an innate desire to be well, and happy and have a good life. Of course, that part of my being was never utilized, because in our culture, I was just like everyone else, I believed doctors are here to tell us how to do that, and we are supposed to do what they say, no matter how inane it may appear to be. Therefore, I had to come to the belief that I could listen to myself and my body. I -- as none of us -- don't need to have fancy medical terms told to me; to make me know how I feel. And no matter what the current medical name is for a disease, it is the same thing systemically whether it is called "ague" (old timey name for flu), "flu," "bad cough," etc., etc.

     

    I put myself on a gluten-free diet (following my own independent study) and following the recommendation from my doctors -- supposed to be the best -- that I have a $10,000 colon surgery. It has always been my reasoning that if a person is not feeling good at all, that putting them through surgery is not a good way to make them feel better. I also feel this way about medications. There is no doctor -- or huge scientist in Big Pharma -- who knows how a certain synthesized drug is going to react with my (or your) DNA. Also, any drug can be checked out in the medical dictionaries MDs use, to see its toxicity. The word "toxic" is a better sounding word than "poison." Well I hated to shatter my M.D.'s hopes for the profit on that $10,000 colon operation, but I told him and the other doctor with him that I was going to try a gluten-free diet. Both of them looked at each other like "What in the heck is she talking about?" But I made them feel better, I told them I would be back if my gluten-free test did not work out.

     

    What was my test? I had heard that Narcotics Anonymous -- I hope I have this right, because narcotics were not one of my problems -- tells its new people who want to get off drugs that it will take 3-months to feel better. So, I figured that was a good sane way for me to go about my gluten-free experiment. The upshot is that my recovery was remarkable -- because, like you, my main problem was always wondering if I was going to get to the nearest toilet in time. That is a terrible thing to have happen to a person when they are in their car with tapestry seats, in huge traffic on the freeway, miles from home. [And for those persons who have never been in this position, it is not a matter of pulling off the freeway at the next offramp; the damage has already been done. No self-respecting person would get out of their car and to into a filing station to ask for a key to the Lady's Room.] Non-celiac persons have no concept of these kinds of things -- and, worse, like at a formal ball -- or an important reception. They just do not know how a Celiac-person's all-around life is affected.

     

    Also, at the end, I had much wooziness and muddled thinking, and sometimes my speech would blur, like I was a daytime drinker. Thank God, I did not go to Alzheimer's doctors -- but what if I was very old and weak looking, what would the prognosis have been? (Just a thought!)

     

    So, because of my gluten-free trial, the need to know where every toilet in my town is, and the wooziness and slurred speech went away first. But, at first I hated to "always have to" eat plain meat and steamed veggies. (Sad, wasn't it? Some people don't even have food!) Now, I have been eating gluten-free for seven years -- and I have learned how to cook gourmet gluten-free that is so good I don't want to take any chances in going to the fanciest up-scale restaurants in the world.

     

    You may wonder if I ever went off the diet. You bet I did! After being gluten-free-pure for about seven months I said "THIS A CROCK." I mostly bemoaned my fate during that time and hadn't learned how to cook Gluten-free gourmet. I now believe I was bored with my good fortune of feeling good all of the time. Now, I can look back to my childhood (when my parents gave me lovely BD parties and I threw up!!!! -- they called it the excitement of so many kids; if I were a kid today, I would be taking doctor-ordered Ritalin for ADD, or whatever it is called). So I got used to the dramas of illness; that was "normal" for me. You know, like being sent home from school -- when I was away at school -- because I was so sick and no one knew what to do with me. Also, Celiac people have the societal disadvantage of never looking sick even when they are dying! So what do schools think? Well, they think: "This kid is putting us on -- because my big flair-ups were always around exam time!!"

     

    I hope this helps you; I want you to have a happy first-time mom life with your child. And watch that child closely, which I am sure you are.

    This really touched me. The disadvantage of not looking sick, because I have been telling my family I'm sick for 26 years and they think I'm crazy, as I don't look sick but I'm really dying.

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    Guest cmw

    An excellent read. I was able to learn a lot about testing and the results.

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    Guest Louise

    Posted

    It seems cruel and unnecessary to put someone back on a diet containing gluten after 6 months of being gluten free. I quit eating gluten after my mother and sister were diagnosed with celiac . I feel so much better that I don't need a 'confirmation ' by a doctor or invasive procedure.

    I too self-diagnosed as I logged symptoms and reactions, searched reliable internet sites. I kept putting off the blood tests and biopsy until my intolerance went from just bread causing the reaction to everything containing wheat/gluten (even porridge oats) to the stage I was very limited in foods. Gluten-free diet is very expensive and in the UK a confirmed diagnosis of celiac disease allows you a limited amount of gluten-free food on prescription. I also have stronger anti-histamines from my GP for any reactions.

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    Guest Jennifer

    Posted

    Thank you. I am still trying to understand it all and this helps. I have tested negative for the biopsy and blood tests but been eating gluten-free for three months and the pain is getting much better. I just can't get swelling in upper abdomen to stop. I swell each time I eat whether it's gluten-free or not.

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    Guest Trisha

    Posted

    I just had a positive small intestinal biopsy 7/2012 and am now having labs done. I had TTG IgA done and it was >3 and negative Endomyisal Ab in 2010. Do you think I just wasn't fully reacting to gluten? Has anyone else had similar issues? I'm Fibromyagia, Chronic Iron Deficiency Anemia, irritable bowel syndrome, migraines, sleep problems, depression, anxiety, hair loss, burning/sore tongue, & vision problems.

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    Guest Audy

    What other stomach symptoms could be associated with blood results typical of celiac disease?

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    Guest Gillian Jones

    Posted

    I'm with you Matt! I mean is medicine about the patient or the disease - I would feel terrible all the time for 6 months back on gluten and can't see what difference it would make to my care - you can still have regular endoscopies, I would imagine on request?

    I've been treated for coeliac disease and it's very useful to read the excellent article before my results - thank you!

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    Guest The5trahans

    Posted

    Can anyone tell me what an IgA of 44 means when the test range states 81-463?

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    Guest VCH

    So... IgA of 219 means I have celiac disease?

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    Guest jodieB

    Posted

    In the hopes this will help someone, I'm posting my before and after Celiac panel test results.

     

    On 4/10/09 (diagnosed)

    Deamidated Gliad IgAH 127

    Deaminated Gliad IgGH 104

    Tranglut IgA 43

     

    On 6/12/09 (gluten free diet)

    127 -> 58 (goal under 10)

    104-> 48 (goal under 10)

    43 -> 10 (goal under 3)

     

    So after being on gluten free diet from 4/10/09-6/12/09, 8 weeks, already seeing dramatic reductions in antibody levels. Not done yet, but are headed in the right direction. I didn't see this kind of information posted anywhere, so hoping this information is helpful.

    Wow everyone else has much lower IgA Counts than me. Mine at diagnosis was 474 and after 3 weeks of gluten-free diet now is 519 !!

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  • About Me

    Scott Adams

    Scott Adams was diagnosed with celiac disease in 1994, and, due to the nearly total lack of information available at that time, was forced to become an expert on the disease in order to recover. In 1995 he launched the site that later became Celiac.com to help as many people as possible with celiac disease get diagnosed so they can begin to live happy, healthy gluten-free lives.  He is co-author of the book Cereal Killers, and founder and publisher of the (formerly paper) newsletter Journal of Gluten Sensitivity. In 1998 he founded The Gluten-Free Mall which he sold in 2014. Celiac.com does not sell any products, and is 100% advertiser supported.


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