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Gluten-related disorders

February 16, 2024

This article is about disorders related to gluten, a natural ingredient in many cereals. It is not to be confused with sensitivities related to glutamate, a flavor-enhancing additive.

Gluten-related disorders is the term for the diseases triggered by gluten, including celiac disease (CD), non-celiac gluten sensitivity (NCGS), gluten ataxia, dermatitis herpetiformis (DH) and wheat allergy.[1][2] The umbrella category has also been referred to as gluten intolerance, though a multi-disciplinary physician-led study, based in part on the 2011 International Coeliac Disease Symposium, concluded that the use of this term should be avoided due to a lack of specificity.[1]

Gluten-related disorders

Gluten is a group of proteins, such as prolamins and glutelins,[3] stored with starch in the endosperm of various cereal (grass) grains.

As of 2017, gluten-related disorders were increasing in frequency in different geographic areas. The increase might be explained by the popularity of the Western diet, the expanded reach of the Mediterranean diet (which also includes grains with gluten), the growing replacement of rice by wheat in many countries,[4] the development in recent years of new types of wheat with a higher amount of cytotoxic gluten peptides,[5] and the higher content of gluten in bread and bakery products, due to the reduction of dough fermentation time.[5] However, a 2020 study by the Leibniz-Institute for Food Systems Biology casts doubt on the idea that modern wheat has higher gluten levels. From a seed bank, they grew and analyzed 60 wheat cultivars from between 1891 and 2010 and found no changes in albumin/globulin and gluten contents over time. "Overall, the harvest year had a more significant effect on protein composition than the cultivar. At the protein level, we found no evidence to support an increased immunostimulatory potential of modern winter wheat."[6]

Types edit

The following classification of gluten-related disorders was announced in 2011 by a panel of experts in London, and published in February 2012:[7][8]

Autoimmune disorders edit

Main articles: Celiac disease and Gluten-sensitive enteropathy-associated conditions

Autoimmune conditions related to gluten include celiac disease, dermatitis herpetiformis, and gluten ataxia. There is research showing that in people with gluten ataxia early diagnosis and treatment with a gluten-free diet can improve ataxia and prevent its progression.[9] The population of people with gluten ataxia and other neurological conditions appears to have a different HLA distribution, in particular more HLA-DQ1, compared to most persons with celiac disease, who have HLA-DQ2 and HLA-DQ8.[10]

Coeliac disease edit

Main article: Coeliac disease

Coeliac disease (American English: celiac) (CD) is one of the most common chronic, immune-mediated disorders, triggered by the eating of gluten, a mixture of proteins found in wheat, barley, rye, and derivatives.[11][12] Evidence has shown that this condition not only has an environmental component but a genetic one as well, due to strong associations of CD with the presence of HLA (Human leukocyte antigen) type II, specifically DQ2 and DQ8 alleles.[13] These alleles can stimulate a T cell, mediated immune response against tissue transglutaminase (TTG), an enzyme in the extracellular matrix, leading to inflammation of the intestinal mucosa and eventually villous atrophy of the small intestine.[14] This is where the innate and adaptive immune response systems collide.

 
Villous atrophy of the small intestine

CD is not only a gastrointestinal disease. It may involve several organs and cause an extensive variety of non-gastrointestinal symptoms. Most importantly, it may often be completely asymptomatic. Added difficulties for diagnosis are the fact that serological markers (anti-tissue transglutaminase [TG2]) are not always present[15] and many people may have minor mucosal lesions, without atrophy of the intestinal villi.[16] Diagnosis of CD should be based on a combination of person's familial history, genetics (i.e. presence of HLA DQ2/DQ8) serology and intestinal histology.[17]

CD affects approximately 1–2% of general population all over the world,[18] but most cases remain unrecognized, undiagnosed and untreated, and exposed to the risk of long-term complications.[17][19] People may experience severe disease symptoms and be subjected to extensive investigations for many years, before a proper diagnosis is achieved.[20] Untreated CD may result in the lack of absorption of nutrients, reduced quality of life, iron deficiency, osteoporosis, an increased risk of intestinal lymphomas and greater mortality.[12] CD is associated with some autoimmune diseases, such as diabetes mellitus type 1,[13] thyroiditis,[21] gluten ataxia, psoriasis, vitiligo, autoimmune hepatitis, dermatitis herpetiformis, primary sclerosing cholangitis, and more.[21]

CD with "classic symptoms", which include gastrointestinal manifestations such as chronic diarrhea and bloating, malabsorption of certain vitamins and minerals, loss of appetite, impaired growth and even bone pain, is currently the least common presentation form of the disease and affects predominantly to small children generally younger than two years of age.[14][19][20]

CD with "non-classic symptoms" is the most common clinical found type[20] and occurs in older children (over two years old),[20] adolescents and adults.[20] It is characterized by milder or even absent gastrointestinal symptoms and a wide spectrum of non-intestinal manifestations that can involve any organ of the body such as, cerebellar ataxia, hypertransaminasemia and peripheral neuropathy.[17] As previously mentioned, CD very frequently may be completely asymptomatic[19] both in children (at least in 43% of the cases[22]) and adults.[19]

To date, the only available medically accepted treatment for people with coeliac disease is to follow a lifelong gluten-free diet.[17][23][24]

With continuous mass genetic modification of grain crops, for instance for drought resistance and pest repellence, the occurrence of diagnosed CD had increased by 400% in the past 50 years alone.[19]

Dermatitis herpetiformis edit

Main article: Dermatitis herpetiformis

Dermatitis herpetiformis (DH), or Duhring-Brocq disease, is a chronic blistering skin autoimmune condition, characterized by the presence of skin lesions that have an extensive and symmetrical distribution, predominating in areas of greater friction, and affecting mainly both elbows, knees, buttocks, ankles, and may also affect the scalp and other parts of the body, and non-symmetrical occasionally. The lesions are vesicular-crusted and when flake off, they evolve to pigmented areas or achromic an intense burning, itchy and blistering rash.[25][26] Despite its name, DH is neither related to nor caused by herpes virus: the name means that it is a skin inflammation having an appearance similar to herpes.

The age of onset is variable starting in children and adolescence but can also affect individuals of both sexes indistinctly at any age of their lives.[26][27]

DH can relatively commonly present with atypical manifestations, which makes its diagnosis more difficult. Some people may show erythema or severe pruritus alone, wheals of chronic urticaria, purpuric lesions resembling petechiae on hands and feet, palmo-plantar keratosis, leukocytoclastic vasculitis-like appearance, and/or lesions mimicking prurigo pigmentosa. DH may be confused with many different cutaneous lesions, such as atopic dermatitis, eczema, urticaria, scabies, impetigo, polymorphic erythema and other autoimmune blistering diseases.[27]

DH is considered to be the "coeliac disease of the skin". For this reason, the new guidelines of the European Society for Pediatric Gastroenterology, Hepatology and Nutrition for the diagnosis of coeliac disease conclude that a proven diagnosis of DH, by itself, confirms the diagnosis of coeliac disease. Nevertheless, duodenal biopsy is recommended in doubtful cases, or if there are suspected gastrointestinal complications, including lymphoma.[27] People with DH have different degrees of intestinal involvement, ranging from milder mucosal lesions to the presence of villous atrophy.[25]

The main and more efficacious treatment for DH is following a lifelong gluten-free diet, which produces the improvement of skin and gut lesions. Nevertheless, the skin lesions may take several months or even years to disappear. To calm itching, dapsone is often recommended as a temporary treatment, during the time it takes for the diet to work, but it has no effect on the gastrointestinal changes and may have important side effects.[25][28]

Gluten ataxia edit

A male with gluten ataxia: previous situation and evolution after three months of gluten-free diet

Gluten ataxia is an autoimmune disease triggered by the ingestion of gluten.[2] With gluten ataxia, damage takes place in the cerebellum, the balance center of the brain that controls coordination and complex movements like walking, speaking and swallowing, with loss of Purkinje cells. People with gluten ataxia usually present gait abnormality or incoordination and tremor of the upper limbs. Gaze-evoked nystagmus and other ocular signs of cerebellar dysfunction are common. Myoclonus, palatal tremor, and opsoclonus-myoclonus may also appear.[29]

Early diagnosis and treatment with a gluten-free diet can improve ataxia and prevent its progression. The effectiveness of the treatment depends on the elapsed time from the onset of the ataxia until diagnosis, because the death of neurons in the cerebellum as a result of gluten exposure is irreversible.[29][30]

Gluten ataxia accounts for 40% of ataxias of unknown origin and 15% of all ataxias.[29][31] Less than 10% of people with gluten ataxia present any gastrointestinal symptom, yet about 40% have intestinal damage.[29]

Non-celiac gluten sensitivity (NCGS) edit

Main article: Non-celiac gluten sensitivity

Non-celiac gluten sensitivity (NCGS), or gluten intolerance,[1] is a syndrome in which people develop a variety of intestinal and/or extraintestinal symptoms that improve when gluten is removed from the diet,[32] after coeliac disease and wheat allergy are excluded.[33] NCGS, which is possibly immune-mediated, now appears to be more common than coeliac disease,[34] with a prevalence estimated to be 6–10 times higher.[35]

Gastrointestinal symptoms, which resemble those of irritable bowel syndrome (IBS),[32][36] may include any of the following: abdominal pain, bloating, bowel habit abnormalities (either diarrhea or constipation),[36][37] nausea, aerophagia, gastroesophageal reflux disease, and aphthous stomatitis.[33][36]

Extra-intestinal symptoms, which can be the only manifestation of NCGS even in absence of gastrointestinal symptoms, may be any of the following: headache or migraine, "foggy mind", fatigue,[33][36][37] fibromyalgia,[37][38][39] joint and muscle pain,[33][36][37] leg or arm numbness,[33][36][37] tingling of the extremities,[33][36] dermatitis (eczema or skin rash),[33][36] atopic disorders,[33] allergy to one or more inhalants, foods or metals[33][37] (such as mites, graminaceae, parietaria, cat or dog hair, shellfish, or nickel),[37] depression,[33][36][37] anxiety,[37] anemia,[33][36] iron-deficiency anemia, folate deficiency, asthma, rhinitis, eating disorders,[37] or autoimmune diseases.[33]

Among extra-intestinal manifestations, NCGS seems to be involved in some neuropsychiatric disorders,[40] principally schizophrenia,[12][36] autism[12][36][37] and peripheral neuropathy,[12][36] and also ataxia[12] and attention deficit hyperactivity disorder (ADHD).[33]

Gluten is likely responsible for the appearance of symptoms, but it has been suggested than in a subgroup of people with NCGS and symptoms like IBS, other components of wheat and related grains (oligosaccharides like fructans), or other plant proteins contained in gluten-containing cereals (agglutinins, lectins, and amylase trypsin inhibitors (ATIs)) may play a role in the development of gastrointestinal symptoms.[17] ATIs are about 2–4% of the total protein in modern wheat and 80–90% in gluten.[33] In a review of May 2015 published in Gastroenterology, Fasano et al. conclude that ATIs may be the inducers of innate immunity in people with coeliac disease or NCGS.[33] As of 2019, reviews conclude that although FODMAPs present in wheat and related grains may play a role in non-celiac gluten sensitivity, they only explain certain gastrointestinal symptoms, such as bloating, but not the extra-digestive symptoms that people with non-celiac gluten sensitivity may develop, such as neurological disorders, fibromyalgia, psychological disturbances, and dermatitis.[41][42][33] As occurs in people with coeliac disease, the treatment is a gluten-free diet (GFD) strict and maintained, without making any dietary transgression.[37] Whereas coeliac disease requires adherence to a strict lifelong gluten-free diet, it is not yet known whether NCGS is a permanent, or a transient condition.[22][37] The results of a 2017 study suggest that NCGS may be a chronic disorder, as is the case with celiac disease.[42] Theoretically, a trial of gluten reintroduction to observe reaction after 1–2 years of strict gluten-free diet might be advisable.[37]

Approximately one-third of persons with NCGS continue having symptoms despite gluten withdrawal. This may be due to diagnostic error, poor dietary compliance, or other reasons. Those with NCGS may be under the impression that they do not need to follow a strictly gluten free diet. However, the ingestion of even a small amount of gluten may cause more immediate symptoms in people with NCGS as compared with those with coeliac disease. People with NCGS should carefully read ingredient labels on food and be aware of potential cross contamination as a source of gluten in otherwise gluten-free foods. To find out if there are unintended ingestions of gluten, an exhaustive evaluation with the advice of a coeliac disease specialized dietitian could be necessary.[37]

In some cases, people can significantly improve with a low FODMAPs diet in addition to gluten withdrawal[5] and/or a GFD with a low content of preservatives and additives.[43] Furthermore, associated to gluten sensitivity, NCGS people may often present IgE-mediated allergies to one or more foods[37] and it is estimated that around 35% of people with some food intolerances, mainly lactose intolerance.[44]

Wheat allergy edit

Main article: Wheat allergy

People can also experience adverse effects of wheat as result of a wheat allergy.[17] Gastrointestinal symptoms of wheat allergy are similar to those of coeliac disease and non-celiac gluten sensitivity, but there is a different interval between exposure to wheat and onset of symptoms. Wheat allergy has a fast onset (from minutes to hours) after the consumption of food containing wheat and could be anaphylaxis.[15][45]

The treatment of wheat allergy consists of complete withdrawal of any food containing wheat and other gluten-containing cereals.[45][46] Nevertheless, some people can tolerate barley, rye or oats.[47]

Other conditions or risk factors edit

Antibodies to α-gliadin have been significantly increased in non-celiacs individuals with oral ulceration.[48] Anti-α-gliadin antibodies are frequently found in celiac disease (CD), to a lesser degree subclinical CD, but are also found in a subset who do not have the disease. Of people with pseudo-exfoliation syndrome, 25% showed increased levels of anti-gliadin IgA.[49] Other people that are also at risk are those taking gluten despite having the disorder, or whose family members have CD. In addition people with autoimmune conditions are also at risk for CD. It has just been found that there is a risk of death in CD. Therefore, gluten intake should be limited before or even after the diagnosis.[50] One-fourth of people with Sjögren's syndrome had responses to gluten; of five that had positive response to gluten, only one could be confirmed as CD and another was potentially GSE[clarification needed], the remaining three appeared to be gluten-sensitive. All were HLA-DQ2 and/or DQ8-positive.[51]

Symptoms edit

More than 250 symptoms of gluten sensitivity have been reported, including bloating, abdominal discomfort or pain, constipation and diarrhea.[52] Sensitivity may also present with extraintestinal symptoms, including headache, "brain fog", tingling and/or numbness in hands and feet, fatigue, as well as muscular disturbances and bone or joint pain;[53][54][55] also neuropsychiatric manifestations ("gluten-sensitive idiopathic neuropathies") have been reported on.[56]

Complications edit

Studies using anti-gliadin antibodies (AGA) reveal that diagnosed or untreated[clarification needed] individuals with AGA have an increasing risk for lymphoid cancers and decreased risk for other conditions associated with affluence.[57]

Causes edit

When enteropathy develops in early childhood, symptomatic disease is more rapidly evident. A survey of geriatrics with celiac disease in Finland revealed that the incidence of disease was much higher than the general population.[58] Allergic disease may rise or fall with age; certain evidence points to the increased or daily use of non-steroidal anti-inflammatory factors (aspirin, ibuprofen) as an increased risk factor for urticaria or anaphylaxis, and the sensitizing dose may include low-dose aspirin therapy used in the treatment of heart disease. NCGS may be a late-onset condition: in a prospective study performed among adults of 18 to 80 years, the median age of disease onset was found to be 55 years, with a six times higher prevalence in females than in males.[5]

The pathogenesis of NCGS is not yet well understood. There is evidence that not only gliadin (the main cytotoxic antigen of gluten), but also other proteins named ATIs which are present in gluten-containing cereals (wheat, rye, barley, and their derivatives) may have a role in the development of symptoms. ATIs are potent activators of the innate immune system.[33][41] FODMAPs, especially fructans, are present in small amounts in gluten-containing grains and have been identified as a possible cause of some gastrointestinal symptoms in persons with NCGS.[33][5][41][59] As of 2019, reviews have concluded that although FODMAPs may play a role in NCGS, they only explain certain gastrointestinal symptoms, such as bloating, but not the extra-digestive symptoms that people with NCGS may develop, such as neurological disorders, fibromyalgia, psychological disturbances, and dermatitis.[41][42][33]

Immunochemistry of glutens edit

Main article: Gluten immunochemistry

Triticeae glutens are important factors in several inflammatory diseases. The immunochemistry can be subdivided into innate responses (direct stimulation of immune system), class II mediated presentation (HLA-DQ), class I mediated stimulation of killer cells, and antibody recognition. The responses to gluten proteins and polypeptide regions differs according to the type of gluten sensitivity. The response is also dependent on the genetic makeup of the human leukocyte antigen genes. In enteropathy, there are at least 3 types of recognition, innate immunity (a form of cellular immunity priming), HLA-DQ and antibody recognition of gliadin and transglutaminase.[60] In NCGS, there is high AGA IgG in more than half of the cases.[61] In wheat allergy, there appears to be an innate component and the response pathways are mediated through IgE against gliadin and other wheat proteins.[62][63][64]

Pathophysiology edit

Compared to the pathophysiology of celiac disease, the pathophysiology of NCGS is far less understood.

A literature review of 2014 found that people with NCGS "are a heterogeneous group, composed of several subgroups, each characterized by different pathogenesis and clinical history, and, probably, clinical course".[65]

Genetics edit

Celiac disease (CD) and NCGS are closely linked with human leukocyte antigen (HLA) class II genes, HLA-DQ2 and HLA-DQ8, located on chromosome 6p21.[2] Nearly all CD people are HLA-DQ2/HLA-DQ8 positive, with 95% HLA-DQ2 and the rest usually HLA-DQ8 (which is carried by 30% of Caucasians).[2] However, the specificity of HLA-DQ2 and/or HLA-DQ8 for CD is low, with estimates ranging from 36% to 53%. In persons with NCGS, the HLA-DQ2 and/or HLA-DQ8 alleles are present in only about 50%, which is still a greater proportion than in the general population.[2]

Diagnosis edit

A literature review of 2014 found that non-coeliac gluten sensitivity diagnosis can be reached only by excluding celiac disease (CD) and wheat allergy.[65]

Persons suspected of having celiac disease may undergo serological testing for IgA anti-tissue transglutaminase antibodies (abbreviated anti-tTG antibodies or anti-TG2 antibodies) and anti-endomysial antibodies (abbreviated EMA) provided the IgA-level is high, and if IgA is low, testing for certain IgG antibodies; in case of positive serological indication, a duodenal biopsy may confirm active celiac disease.[66]

Eliminating the possibility of CD can generally also be done by adding HLA-DQ typing. The absence of HLA-DQ2 and HLA-DQ8 has a very high negative predictive value for CD,[2][67] and the predictive value can be further enhanced by including HLA-DQ7.5 (HLA-DQ2 and HLA-DQ8 are found in coeliac disease 98% of the time in Caucasians, HLA-DQ7.5 present in the remaining 1.6% and only 0.4% of Caucasians are missed with the combination of these three).[citation needed] Without serological or HLA-DQ2/8 positivity, celiac disease is likely not present. HLA-DQ typing has a practical advantage in that it is the only diagnostic test that allows to exclude CD when a person is already on a gluten-free diet; however, as not only celiacs are HLA-DQ2/HLA-DQ8 positive, this method has a higher false positive rate than anti-TG2 and EMA antibody testing.

A four-of-five rule was proposed 2010 for confirming celiac disease, with the disease confirmed if at least four of the following five criteria are satisfied:[2][68]

  • typical symptoms of celiac disease;
  • positivity of serum celiac disease immunoglobulin, A class autoantibodies at high titer;
  • human leukocyte antigen (HLA)-DQ2 or DQ8 genotypes;
  • celiac enteropathy at the small bowel biopsy; and
  • response to the gluten-free diet.

For diagnosis of wheat allergy, allergy tests are available.

Treatment edit

Main article: Gluten-free diet

For people with celiac disease, a lifelong strict gluten-free diet is the only effective treatment to date;[23][69]

For people diagnosed with non-celiac gluten sensitivity, there are still open questions concerning for example the duration of such a diet. The results of a 2017 study suggest that non-celiac gluten sensitivity may be a chronic disorder, as is the case with celiac disease.[42]

For people with wheat allergy, the individual average is six years of gluten-free diet, excepting persons with anaphylaxis, for whom the diet is to be wheat-free for life.[69]

Preferably, newly diagnosed celiacs seek the help of a dietician to receive support for identifying hidden sources of gluten, planning balanced meals, reading labels, food shopping, dining out, and dining during travel.[70] Knowledge of hidden sources of gluten is important for people with celiac disease as they need to be very strict regarding eating only gluten-free food.[71] The degree of gluten cross contamination tolerated by people with non-celiac gluten sensitivity is not clear but there is some evidence that they can present with symptoms even after consumption of small amounts.[37] Sporadic accidental contaminations with gluten can reactivate movement disorders associated with non-celiac gluten sensitivity.[72] A part of people with gluten-related neuropathy or gluten ataxia appears not to be able to tolerate even the traces of gluten allowed in most foods labeled as "gluten-free".[73]

The inclusion of oats in gluten-free diets remains controversial. Avenin present in oats may also be toxic for individuals with celiacs.[74] Its toxicity depends on the cultivar consumed.[75] Furthermore, oats are frequently cross-contaminated with gluten-containing cereals.[74]

Risks of non-medical and self-diagnosed adoption of a gluten-free diet edit

Withdrawing gluten from the diet without previously carrying out a complete medical examination can hamper the diagnosis of celiac disease. Diagnostic tests (antibodies and duodenum biopsies) lose their usefulness if the person is already eating a gluten-free diet.[76]

Potential nutritional deficiencies edit

Gluten proteins have low nutritional value and replacing grains that contain gluten is easy from the nutritional point of view.[23] However, an unbalanced selection of food and an incorrect choice of gluten-free replacement products may lead to nutritional deficiencies. Replacing flour from wheat or other gluten-containing cereals with gluten-free flours in commercial products may lead to a lower intake of important nutrients, such as iron and B vitamins. Some gluten-free commercial replacement products are not enriched or fortified as their gluten-containing counterparts, and often have greater lipid/carbohydrate content. Children especially often over-consume these products, such as snacks and biscuits.[74]

Pseudocereals (quinoa, amaranth, and buckwheat) and some minor cereals are healthier alternatives to these prepared products and have higher nutritional value.[74][23] Furthermore, they contain protein of higher nutritional quality than those of wheat, and in greater quantities.[74]

Nutritional complications can be prevented by a correct dietary education.[74]

Epidemiology edit

In the United States, fewer cases of CD have been found compared to other countries.[77] The incidence of celiac disease and of wheat allergy is estimated each to lie at around 1% of the population. There has been a 6.4 increase in the case reports of celiac disease between 1990 and 2009.[50] The incidence of NCGS is unknown; some estimates range from 0.6% to 6%,[69] and a systematic review of 2015 reported on studies with NCGS prevalence rates between 0.5% and 13%.[78]

In Europe, the average consumption of gluten is 10g to 20g per day, with parts of the population reaching 50g or more per day.[2]

Histology edit

Changes in inflammatory cells affect the body, which reduces the intake of "nutrients, fat-soluble vitamins and minerals" in the body.[50]

Regulations edit

 
Crossed-grain symbol, similar to that of the Association Of European Coeliac Societies (AOECS)

In various countries, regulations and labelling requirements for gluten-free food products have been implemented.

For Europe, the Commission Regulation (EC) No. 41/2009 of 20 January 2009 concerning the composition and labelling of foodstuffs suitable for people intolerant to gluten has laid down harmonised rules on the content and labelling of these foodstuffs, setting out the conditions under which foods may be labelled as "gluten-free" or "very low gluten".[79] Having entered into force on 10 February 2009 and taken effect on 1 January 2012, these rules have been repealed with effect as of 20 July 2016. The background is that, in line with the Regulation (EU) No 609/2013 on food for specific groups, gluten-free foods shall, in future, be legislated for under the EU Food Information for Consumers Regulation (Regulation (EU) No. 1169/2011). Furthermore, the Commission Implementing Regulation (EU) No 828/2014 of 30 July 2014 on the requirements for the provision of information to consumers on the absence or reduced presence of gluten in food extends the rules of Regulation (EC) 41/2009 on "gluten-free" and "very low gluten" statements also to non pre-packed foods such as those served in restaurants. The implementing regulation also clarifies how consumers are to be informed of the difference between foods that are naturally free of gluten and products that are specially formulated for gluten-intolerant persons.[80]

Recognition of gluten-free packaged foods is facilitated by the crossed-grain symbol, representing a crossed ear of wheat. The symbol is used as a logo that facilitates food shopping for people with CD and other gluten-related disorders. The symbol, which is protected as a trademark in Europe and the United States and is covered by worldwide copyright, can be represented in any colour.[81][82]

Research edit

Research has attempted to discern, by double-blind placebo-controlled trials, between a "fad component" to the recent popularity of the gluten-free diet and an actual sensitivity to gluten or other components of wheat.[33][36][83]

In a 2013 double-blind, placebo-controlled challenge (DBPC) by Biesiekierski et al. in a few people with irritable bowel syndrome, the authors found no difference between gluten or placebo groups and the concept of NCGS as a syndrome was questioned. Nevertheless, this study had design errors and an incorrect selection of participants, and probably the reintroduction of both gluten and whey protein had a nocebo effect similar in all people, and this could have masked the true effect of gluten/wheat reintroduction.[17][44]

In a 2015 double-blind placebo cross-over trial, small amounts of purified wheat gluten triggered gastrointestinal symptoms (such as abdominal bloating and pain) and extra-intestinal manifestations (such as foggy mind, depression and aphthous stomatitis) in self-reported NCGS. Nevertheless, it remains elusive whether these findings specifically implicate gluten or proteins present in gluten-containing cereals.[44]

A 2016 review of the recent research advancements in understanding diet's role in attenuating IBS patient's symptoms concluded that gluten was a common trigger. However, because on the different compounds responsible for symptoms, many patients that could be inaccurately labelled non-coeliac gluten sensitive; and it may be more appropriate to use nomenclature such as "non-coeliac wheat sensitive" (NCWS), "non-coeliac wheat protein sensitive" (NCWPS), or even FODMAP sensitive when referring to these patients.[84]

In a 2018 double-blind, crossover research study on 59 persons on a gluten-free diet with challenges of gluten, fructans or placebo, intestinal symptoms (specifically bloating) were borderline significantly higher after challenge with fructans, in comparison with gluten proteins (P=0.049).[41][42] Although the differences between the three interventions was very small, the authors concluded that fructans (the specific type of FODMAP found in wheat) are more likely to be the cause of NCGS gastrointestinal symptoms, rather than gluten.[41] In addition, fructans used in the study were extracted from chicory root, so it remains to be seen whether the wheat fructans produce the same effect.[42]

See also edit

References edit

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  7. ^ Sapone, Anna; et al. (7 February 2012). "Spectrum of gluten-relate disorders: consensus on new nomenclature and classification". BMC Medicine. 2012 (10:13): 13. doi:10.1186/1741-7015-10-13. PMC 3292448. PMID 22313950.
  8. ^ Czaja-Bulsa G (August 2014). "Non coeliac gluten sensitivity - A new disease with gluten intolerance". Clinical Nutrition (Edinburgh, Scotland) (Review). 34 (2): 189–194. doi:10.1016/j.clnu.2014.08.012. PMID 25245857. See section 9 and Figure 2: Classification of gluten-dependent disorders.
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February 16, 2024
gluten, related, disorders, this, article, about, disorders, related, gluten, natural, ingredient, many, cereals, confused, with, sensitivities, related, glutamate, flavor, enhancing, additive, term, diseases, triggered, gluten, including, celiac, disease, cel. This article is about disorders related to gluten a natural ingredient in many cereals It is not to be confused with sensitivities related to glutamate a flavor enhancing additive Gluten related disorders is the term for the diseases triggered by gluten including celiac disease CD non celiac gluten sensitivity NCGS gluten ataxia dermatitis herpetiformis DH and wheat allergy 1 2 The umbrella category has also been referred to as gluten intolerance though a multi disciplinary physician led study based in part on the 2011 International Coeliac Disease Symposium concluded that the use of this term should be avoided due to a lack of specificity 1 Gluten related disordersGluten is a group of proteins such as prolamins and glutelins 3 stored with starch in the endosperm of various cereal grass grains As of 2017 update gluten related disorders were increasing in frequency in different geographic areas The increase might be explained by the popularity of the Western diet the expanded reach of the Mediterranean diet which also includes grains with gluten the growing replacement of rice by wheat in many countries 4 the development in recent years of new types of wheat with a higher amount of cytotoxic gluten peptides 5 and the higher content of gluten in bread and bakery products due to the reduction of dough fermentation time 5 However a 2020 study by the Leibniz Institute for Food Systems Biology casts doubt on the idea that modern wheat has higher gluten levels From a seed bank they grew and analyzed 60 wheat cultivars from between 1891 and 2010 and found no changes in albumin globulin and gluten contents over time Overall the harvest year had a more significant effect on protein composition than the cultivar At the protein level we found no evidence to support an increased immunostimulatory potential of modern winter wheat 6 Contents 1 Types 1 1 Autoimmune disorders 1 1 1 Coeliac disease 1 1 2 Dermatitis herpetiformis 1 1 3 Gluten ataxia 1 2 Non celiac gluten sensitivity NCGS 1 3 Wheat allergy 1 4 Other conditions or risk factors 2 Symptoms 2 1 Complications 3 Causes 3 1 Immunochemistry of glutens 4 Pathophysiology 4 1 Genetics 5 Diagnosis 6 Treatment 6 1 Risks of non medical and self diagnosed adoption of a gluten free diet 6 2 Potential nutritional deficiencies 7 Epidemiology 8 Histology 9 Regulations 10 Research 11 See also 12 ReferencesTypes editThe following classification of gluten related disorders was announced in 2011 by a panel of experts in London and published in February 2012 7 8 Autoimmune disorders celiac disease dermatitis herpetiformis gluten ataxia Non autoimmune non allergic disorder with unknown cause likely immune modulated non celiac gluten sensitivity NCGS Allergic food allergy IgE mediated and non IgE mediated wheat dependent exercise induced anaphylaxis WDEIA baker s asthma contact dermatitis Autoimmune disorders edit Main articles Celiac disease and Gluten sensitive enteropathy associated conditions Autoimmune conditions related to gluten include celiac disease dermatitis herpetiformis and gluten ataxia There is research showing that in people with gluten ataxia early diagnosis and treatment with a gluten free diet can improve ataxia and prevent its progression 9 The population of people with gluten ataxia and other neurological conditions appears to have a different HLA distribution in particular more HLA DQ1 compared to most persons with celiac disease who have HLA DQ2 and HLA DQ8 10 Coeliac disease edit Main article Coeliac disease Coeliac disease American English celiac CD is one of the most common chronic immune mediated disorders triggered by the eating of gluten a mixture of proteins found in wheat barley rye and derivatives 11 12 Evidence has shown that this condition not only has an environmental component but a genetic one as well due to strong associations of CD with the presence of HLA Human leukocyte antigen type II specifically DQ2 and DQ8 alleles 13 These alleles can stimulate a T cell mediated immune response against tissue transglutaminase TTG an enzyme in the extracellular matrix leading to inflammation of the intestinal mucosa and eventually villous atrophy of the small intestine 14 This is where the innate and adaptive immune response systems collide nbsp Villous atrophy of the small intestineCD is not only a gastrointestinal disease It may involve several organs and cause an extensive variety of non gastrointestinal symptoms Most importantly it may often be completely asymptomatic Added difficulties for diagnosis are the fact that serological markers anti tissue transglutaminase TG2 are not always present 15 and many people may have minor mucosal lesions without atrophy of the intestinal villi 16 Diagnosis of CD should be based on a combination of person s familial history genetics i e presence of HLA DQ2 DQ8 serology and intestinal histology 17 CD affects approximately 1 2 of general population all over the world 18 but most cases remain unrecognized undiagnosed and untreated and exposed to the risk of long term complications 17 19 People may experience severe disease symptoms and be subjected to extensive investigations for many years before a proper diagnosis is achieved 20 Untreated CD may result in the lack of absorption of nutrients reduced quality of life iron deficiency osteoporosis an increased risk of intestinal lymphomas and greater mortality 12 CD is associated with some autoimmune diseases such as diabetes mellitus type 1 13 thyroiditis 21 gluten ataxia psoriasis vitiligo autoimmune hepatitis dermatitis herpetiformis primary sclerosing cholangitis and more 21 CD with classic symptoms which include gastrointestinal manifestations such as chronic diarrhea and bloating malabsorption of certain vitamins and minerals loss of appetite impaired growth and even bone pain is currently the least common presentation form of the disease and affects predominantly to small children generally younger than two years of age 14 19 20 CD with non classic symptoms is the most common clinical found type 20 and occurs in older children over two years old 20 adolescents and adults 20 It is characterized by milder or even absent gastrointestinal symptoms and a wide spectrum of non intestinal manifestations that can involve any organ of the body such as cerebellar ataxia hypertransaminasemia and peripheral neuropathy 17 As previously mentioned CD very frequently may be completely asymptomatic 19 both in children at least in 43 of the cases 22 and adults 19 To date the only available medically accepted treatment for people with coeliac disease is to follow a lifelong gluten free diet 17 23 24 With continuous mass genetic modification of grain crops for instance for drought resistance and pest repellence the occurrence of diagnosed CD had increased by 400 in the past 50 years alone 19 Dermatitis herpetiformis edit Main article Dermatitis herpetiformis Dermatitis herpetiformis DH or Duhring Brocq disease is a chronic blistering skin autoimmune condition characterized by the presence of skin lesions that have an extensive and symmetrical distribution predominating in areas of greater friction and affecting mainly both elbows knees buttocks ankles and may also affect the scalp and other parts of the body and non symmetrical occasionally The lesions are vesicular crusted and when flake off they evolve to pigmented areas or achromic an intense burning itchy and blistering rash 25 26 Despite its name DH is neither related to nor caused by herpes virus the name means that it is a skin inflammation having an appearance similar to herpes The age of onset is variable starting in children and adolescence but can also affect individuals of both sexes indistinctly at any age of their lives 26 27 DH can relatively commonly present with atypical manifestations which makes its diagnosis more difficult Some people may show erythema or severe pruritus alone wheals of chronic urticaria purpuric lesions resembling petechiae on hands and feet palmo plantar keratosis leukocytoclastic vasculitis like appearance and or lesions mimicking prurigo pigmentosa DH may be confused with many different cutaneous lesions such as atopic dermatitis eczema urticaria scabies impetigo polymorphic erythema and other autoimmune blistering diseases 27 DH is considered to be the coeliac disease of the skin For this reason the new guidelines of the European Society for Pediatric Gastroenterology Hepatology and Nutrition for the diagnosis of coeliac disease conclude that a proven diagnosis of DH by itself confirms the diagnosis of coeliac disease Nevertheless duodenal biopsy is recommended in doubtful cases or if there are suspected gastrointestinal complications including lymphoma 27 People with DH have different degrees of intestinal involvement ranging from milder mucosal lesions to the presence of villous atrophy 25 The main and more efficacious treatment for DH is following a lifelong gluten free diet which produces the improvement of skin and gut lesions Nevertheless the skin lesions may take several months or even years to disappear To calm itching dapsone is often recommended as a temporary treatment during the time it takes for the diet to work but it has no effect on the gastrointestinal changes and may have important side effects 25 28 Gluten ataxia edit source source source source A male with gluten ataxia previous situation and evolution after three months of gluten free dietGluten ataxia is an autoimmune disease triggered by the ingestion of gluten 2 With gluten ataxia damage takes place in the cerebellum the balance center of the brain that controls coordination and complex movements like walking speaking and swallowing with loss of Purkinje cells People with gluten ataxia usually present gait abnormality or incoordination and tremor of the upper limbs Gaze evoked nystagmus and other ocular signs of cerebellar dysfunction are common Myoclonus palatal tremor and opsoclonus myoclonus may also appear 29 Early diagnosis and treatment with a gluten free diet can improve ataxia and prevent its progression The effectiveness of the treatment depends on the elapsed time from the onset of the ataxia until diagnosis because the death of neurons in the cerebellum as a result of gluten exposure is irreversible 29 30 Gluten ataxia accounts for 40 of ataxias of unknown origin and 15 of all ataxias 29 31 Less than 10 of people with gluten ataxia present any gastrointestinal symptom yet about 40 have intestinal damage 29 Non celiac gluten sensitivity NCGS edit Main article Non celiac gluten sensitivity Non celiac gluten sensitivity NCGS or gluten intolerance 1 is a syndrome in which people develop a variety of intestinal and or extraintestinal symptoms that improve when gluten is removed from the diet 32 after coeliac disease and wheat allergy are excluded 33 NCGS which is possibly immune mediated now appears to be more common than coeliac disease 34 with a prevalence estimated to be 6 10 times higher 35 Gastrointestinal symptoms which resemble those of irritable bowel syndrome IBS 32 36 may include any of the following abdominal pain bloating bowel habit abnormalities either diarrhea or constipation 36 37 nausea aerophagia gastroesophageal reflux disease and aphthous stomatitis 33 36 Extra intestinal symptoms which can be the only manifestation of NCGS even in absence of gastrointestinal symptoms may be any of the following headache or migraine foggy mind fatigue 33 36 37 fibromyalgia 37 38 39 joint and muscle pain 33 36 37 leg or arm numbness 33 36 37 tingling of the extremities 33 36 dermatitis eczema or skin rash 33 36 atopic disorders 33 allergy to one or more inhalants foods or metals 33 37 such as mites graminaceae parietaria cat or dog hair shellfish or nickel 37 depression 33 36 37 anxiety 37 anemia 33 36 iron deficiency anemia folate deficiency asthma rhinitis eating disorders 37 or autoimmune diseases 33 Among extra intestinal manifestations NCGS seems to be involved in some neuropsychiatric disorders 40 principally schizophrenia 12 36 autism 12 36 37 and peripheral neuropathy 12 36 and also ataxia 12 and attention deficit hyperactivity disorder ADHD 33 Gluten is likely responsible for the appearance of symptoms but it has been suggested than in a subgroup of people with NCGS and symptoms like IBS other components of wheat and related grains oligosaccharides like fructans or other plant proteins contained in gluten containing cereals agglutinins lectins and amylase trypsin inhibitors ATIs may play a role in the development of gastrointestinal symptoms 17 ATIs are about 2 4 of the total protein in modern wheat and 80 90 in gluten 33 In a review of May 2015 published in Gastroenterology Fasano et al conclude that ATIs may be the inducers of innate immunity in people with coeliac disease or NCGS 33 As of 2019 reviews conclude that although FODMAPs present in wheat and related grains may play a role in non celiac gluten sensitivity they only explain certain gastrointestinal symptoms such as bloating but not the extra digestive symptoms that people with non celiac gluten sensitivity may develop such as neurological disorders fibromyalgia psychological disturbances and dermatitis 41 42 33 As occurs in people with coeliac disease the treatment is a gluten free diet GFD strict and maintained without making any dietary transgression 37 Whereas coeliac disease requires adherence to a strict lifelong gluten free diet it is not yet known whether NCGS is a permanent or a transient condition 22 37 The results of a 2017 study suggest that NCGS may be a chronic disorder as is the case with celiac disease 42 Theoretically a trial of gluten reintroduction to observe reaction after 1 2 years of strict gluten free diet might be advisable 37 Approximately one third of persons with NCGS continue having symptoms despite gluten withdrawal This may be due to diagnostic error poor dietary compliance or other reasons Those with NCGS may be under the impression that they do not need to follow a strictly gluten free diet However the ingestion of even a small amount of gluten may cause more immediate symptoms in people with NCGS as compared with those with coeliac disease People with NCGS should carefully read ingredient labels on food and be aware of potential cross contamination as a source of gluten in otherwise gluten free foods To find out if there are unintended ingestions of gluten an exhaustive evaluation with the advice of a coeliac disease specialized dietitian could be necessary 37 In some cases people can significantly improve with a low FODMAPs diet in addition to gluten withdrawal 5 and or a GFD with a low content of preservatives and additives 43 Furthermore associated to gluten sensitivity NCGS people may often present IgE mediated allergies to one or more foods 37 and it is estimated that around 35 of people with some food intolerances mainly lactose intolerance 44 Wheat allergy edit Main article Wheat allergy People can also experience adverse effects of wheat as result of a wheat allergy 17 Gastrointestinal symptoms of wheat allergy are similar to those of coeliac disease and non celiac gluten sensitivity but there is a different interval between exposure to wheat and onset of symptoms Wheat allergy has a fast onset from minutes to hours after the consumption of food containing wheat and could be anaphylaxis 15 45 The treatment of wheat allergy consists of complete withdrawal of any food containing wheat and other gluten containing cereals 45 46 Nevertheless some people can tolerate barley rye or oats 47 Other conditions or risk factors edit This section relies excessively on references to primary sources Please improve this section by adding secondary or tertiary sources Find sources Gluten related disorders news newspapers books scholar JSTOR January 2015 Learn how and when to remove this template message Antibodies to a gliadin have been significantly increased in non celiacs individuals with oral ulceration 48 Anti a gliadin antibodies are frequently found in celiac disease CD to a lesser degree subclinical CD but are also found in a subset who do not have the disease Of people with pseudo exfoliation syndrome 25 showed increased levels of anti gliadin IgA 49 Other people that are also at risk are those taking gluten despite having the disorder or whose family members have CD In addition people with autoimmune conditions are also at risk for CD It has just been found that there is a risk of death in CD Therefore gluten intake should be limited before or even after the diagnosis 50 One fourth of people with Sjogren s syndrome had responses to gluten of five that had positive response to gluten only one could be confirmed as CD and another was potentially GSE clarification needed the remaining three appeared to be gluten sensitive All were HLA DQ2 and or DQ8 positive 51 Symptoms editMore than 250 symptoms of gluten sensitivity have been reported including bloating abdominal discomfort or pain constipation and diarrhea 52 Sensitivity may also present with extraintestinal symptoms including headache brain fog tingling and or numbness in hands and feet fatigue as well as muscular disturbances and bone or joint pain 53 54 55 also neuropsychiatric manifestations gluten sensitive idiopathic neuropathies have been reported on 56 Complications edit This section relies excessively on references to primary sources Please improve this section by adding secondary or tertiary sources Find sources Gluten related disorders news newspapers books scholar JSTOR December 2014 Learn how and when to remove this template message Studies using anti gliadin antibodies AGA reveal that diagnosed or untreated clarification needed individuals with AGA have an increasing risk for lymphoid cancers and decreased risk for other conditions associated with affluence 57 Causes editWhen enteropathy develops in early childhood symptomatic disease is more rapidly evident A survey of geriatrics with celiac disease in Finland revealed that the incidence of disease was much higher than the general population 58 Allergic disease may rise or fall with age certain evidence points to the increased or daily use of non steroidal anti inflammatory factors aspirin ibuprofen as an increased risk factor for urticaria or anaphylaxis and the sensitizing dose may include low dose aspirin therapy used in the treatment of heart disease NCGS may be a late onset condition in a prospective study performed among adults of 18 to 80 years the median age of disease onset was found to be 55 years with a six times higher prevalence in females than in males 5 The pathogenesis of NCGS is not yet well understood There is evidence that not only gliadin the main cytotoxic antigen of gluten but also other proteins named ATIs which are present in gluten containing cereals wheat rye barley and their derivatives may have a role in the development of symptoms ATIs are potent activators of the innate immune system 33 41 FODMAPs especially fructans are present in small amounts in gluten containing grains and have been identified as a possible cause of some gastrointestinal symptoms in persons with NCGS 33 5 41 59 As of 2019 reviews have concluded that although FODMAPs may play a role in NCGS they only explain certain gastrointestinal symptoms such as bloating but not the extra digestive symptoms that people with NCGS may develop such as neurological disorders fibromyalgia psychological disturbances and dermatitis 41 42 33 Immunochemistry of glutens edit Main article Gluten immunochemistry Triticeae glutens are important factors in several inflammatory diseases The immunochemistry can be subdivided into innate responses direct stimulation of immune system class II mediated presentation HLA DQ class I mediated stimulation of killer cells and antibody recognition The responses to gluten proteins and polypeptide regions differs according to the type of gluten sensitivity The response is also dependent on the genetic makeup of the human leukocyte antigen genes In enteropathy there are at least 3 types of recognition innate immunity a form of cellular immunity priming HLA DQ and antibody recognition of gliadin and transglutaminase 60 In NCGS there is high AGA IgG in more than half of the cases 61 In wheat allergy there appears to be an innate component and the response pathways are mediated through IgE against gliadin and other wheat proteins 62 63 64 Pathophysiology editCompared to the pathophysiology of celiac disease the pathophysiology of NCGS is far less understood A literature review of 2014 found that people with NCGS are a heterogeneous group composed of several subgroups each characterized by different pathogenesis and clinical history and probably clinical course 65 Genetics edit Celiac disease CD and NCGS are closely linked with human leukocyte antigen HLA class II genes HLA DQ2 and HLA DQ8 located on chromosome 6p21 2 Nearly all CD people are HLA DQ2 HLA DQ8 positive with 95 HLA DQ2 and the rest usually HLA DQ8 which is carried by 30 of Caucasians 2 However the specificity of HLA DQ2 and or HLA DQ8 for CD is low with estimates ranging from 36 to 53 In persons with NCGS the HLA DQ2 and or HLA DQ8 alleles are present in only about 50 which is still a greater proportion than in the general population 2 Diagnosis editA literature review of 2014 found that non coeliac gluten sensitivity diagnosis can be reached only by excluding celiac disease CD and wheat allergy 65 Persons suspected of having celiac disease may undergo serological testing for IgA anti tissue transglutaminase antibodies abbreviated anti tTG antibodies or anti TG2 antibodies and anti endomysial antibodies abbreviated EMA provided the IgA level is high and if IgA is low testing for certain IgG antibodies in case of positive serological indication a duodenal biopsy may confirm active celiac disease 66 Eliminating the possibility of CD can generally also be done by adding HLA DQ typing The absence of HLA DQ2 and HLA DQ8 has a very high negative predictive value for CD 2 67 and the predictive value can be further enhanced by including HLA DQ7 5 HLA DQ2 and HLA DQ8 are found in coeliac disease 98 of the time in Caucasians HLA DQ7 5 present in the remaining 1 6 and only 0 4 of Caucasians are missed with the combination of these three citation needed Without serological or HLA DQ2 8 positivity celiac disease is likely not present HLA DQ typing has a practical advantage in that it is the only diagnostic test that allows to exclude CD when a person is already on a gluten free diet however as not only celiacs are HLA DQ2 HLA DQ8 positive this method has a higher false positive rate than anti TG2 and EMA antibody testing A four of five rule was proposed 2010 for confirming celiac disease with the disease confirmed if at least four of the following five criteria are satisfied 2 68 typical symptoms of celiac disease positivity of serum celiac disease immunoglobulin A class autoantibodies at high titer human leukocyte antigen HLA DQ2 or DQ8 genotypes celiac enteropathy at the small bowel biopsy and response to the gluten free diet For diagnosis of wheat allergy allergy tests are available Treatment editMain article Gluten free diet For people with celiac disease a lifelong strict gluten free diet is the only effective treatment to date 23 69 For people diagnosed with non celiac gluten sensitivity there are still open questions concerning for example the duration of such a diet The results of a 2017 study suggest that non celiac gluten sensitivity may be a chronic disorder as is the case with celiac disease 42 For people with wheat allergy the individual average is six years of gluten free diet excepting persons with anaphylaxis for whom the diet is to be wheat free for life 69 Preferably newly diagnosed celiacs seek the help of a dietician to receive support for identifying hidden sources of gluten planning balanced meals reading labels food shopping dining out and dining during travel 70 Knowledge of hidden sources of gluten is important for people with celiac disease as they need to be very strict regarding eating only gluten free food 71 The degree of gluten cross contamination tolerated by people with non celiac gluten sensitivity is not clear but there is some evidence that they can present with symptoms even after consumption of small amounts 37 Sporadic accidental contaminations with gluten can reactivate movement disorders associated with non celiac gluten sensitivity 72 A part of people with gluten related neuropathy or gluten ataxia appears not to be able to tolerate even the traces of gluten allowed in most foods labeled as gluten free 73 The inclusion of oats in gluten free diets remains controversial Avenin present in oats may also be toxic for individuals with celiacs 74 Its toxicity depends on the cultivar consumed 75 Furthermore oats are frequently cross contaminated with gluten containing cereals 74 Risks of non medical and self diagnosed adoption of a gluten free diet edit Withdrawing gluten from the diet without previously carrying out a complete medical examination can hamper the diagnosis of celiac disease Diagnostic tests antibodies and duodenum biopsies lose their usefulness if the person is already eating a gluten free diet 76 Potential nutritional deficiencies edit Gluten proteins have low nutritional value and replacing grains that contain gluten is easy from the nutritional point of view 23 However an unbalanced selection of food and an incorrect choice of gluten free replacement products may lead to nutritional deficiencies Replacing flour from wheat or other gluten containing cereals with gluten free flours in commercial products may lead to a lower intake of important nutrients such as iron and B vitamins Some gluten free commercial replacement products are not enriched or fortified as their gluten containing counterparts and often have greater lipid carbohydrate content Children especially often over consume these products such as snacks and biscuits 74 Pseudocereals quinoa amaranth and buckwheat and some minor cereals are healthier alternatives to these prepared products and have higher nutritional value 74 23 Furthermore they contain protein of higher nutritional quality than those of wheat and in greater quantities 74 Nutritional complications can be prevented by a correct dietary education 74 Epidemiology editIn the United States fewer cases of CD have been found compared to other countries 77 The incidence of celiac disease and of wheat allergy is estimated each to lie at around 1 of the population There has been a 6 4 increase in the case reports of celiac disease between 1990 and 2009 50 The incidence of NCGS is unknown some estimates range from 0 6 to 6 69 and a systematic review of 2015 reported on studies with NCGS prevalence rates between 0 5 and 13 78 In Europe the average consumption of gluten is 10g to 20g per day with parts of the population reaching 50g or more per day 2 Histology editChanges in inflammatory cells affect the body which reduces the intake of nutrients fat soluble vitamins and minerals in the body 50 Regulations edit nbsp Crossed grain symbol similar to that of the Association Of European Coeliac Societies AOECS In various countries regulations and labelling requirements for gluten free food products have been implemented For Europe the Commission Regulation EC No 41 2009 of 20 January 2009 concerning the composition and labelling of foodstuffs suitable for people intolerant to gluten has laid down harmonised rules on the content and labelling of these foodstuffs setting out the conditions under which foods may be labelled as gluten free or very low gluten 79 Having entered into force on 10 February 2009 and taken effect on 1 January 2012 these rules have been repealed with effect as of 20 July 2016 The background is that in line with the Regulation EU No 609 2013 on food for specific groups gluten free foods shall in future be legislated for under the EU Food Information for Consumers Regulation Regulation EU No 1169 2011 Furthermore the Commission Implementing Regulation EU No 828 2014 of 30 July 2014 on the requirements for the provision of information to consumers on the absence or reduced presence of gluten in food extends the rules of Regulation EC 41 2009 on gluten free and very low gluten statements also to non pre packed foods such as those served in restaurants The implementing regulation also clarifies how consumers are to be informed of the difference between foods that are naturally free of gluten and products that are specially formulated for gluten intolerant persons 80 Recognition of gluten free packaged foods is facilitated by the crossed grain symbol representing a crossed ear of wheat The symbol is used as a logo that facilitates food shopping for people with CD and other gluten related disorders The symbol which is protected as a trademark in Europe and the United States and is covered by worldwide copyright can be represented in any colour 81 82 Research editResearch has attempted to discern by double blind placebo controlled trials between a fad component to the recent popularity of the gluten free diet and an actual sensitivity to gluten or other components of wheat 33 36 83 In a 2013 double blind placebo controlled challenge DBPC by Biesiekierski et al in a few people with irritable bowel syndrome the authors found no difference between gluten or placebo groups and the concept of NCGS as a syndrome was questioned Nevertheless this study had design errors and an incorrect selection of participants and probably the reintroduction of both gluten and whey protein had a nocebo effect similar in all people and this could have masked the true effect of gluten wheat reintroduction 17 44 In a 2015 double blind placebo cross over trial small amounts of purified wheat gluten triggered gastrointestinal symptoms such as abdominal bloating and pain and extra intestinal manifestations such as foggy mind depression and aphthous stomatitis in self reported NCGS Nevertheless it remains elusive whether these findings specifically implicate gluten or proteins present in gluten containing cereals 44 A 2016 review of the recent research advancements in understanding diet s role in attenuating IBS patient s symptoms concluded that gluten was a common trigger However because on the different compounds responsible for symptoms many patients that could be inaccurately labelled non coeliac gluten sensitive and it may be more appropriate to use nomenclature such as non coeliac wheat sensitive NCWS non coeliac wheat protein sensitive NCWPS or even FODMAP sensitive when referring to these patients 84 In a 2018 double blind crossover research study on 59 persons on a gluten free diet with challenges of gluten fructans or placebo intestinal symptoms specifically bloating were borderline significantly higher after challenge with fructans in comparison with gluten proteins P 0 049 41 42 Although the differences between the three interventions was very small the authors concluded that fructans the specific type of FODMAP found in wheat are more likely to be the cause of NCGS gastrointestinal symptoms rather than gluten 41 In addition fructans used in the study were extracted from chicory root so it remains to be seen whether the wheat fructans produce the same effect 42 See also editList of allergies Vomitoxin a mycotoxin which can give rise to somewhat comparable symptoms References edit a b c Ludvigsson JF Leffler DA Bai JC Biagi F Fasano A Green PH Hadjivassiliou M Kaukinen K Kelly CP Leonard JN Lundin KE Murray JA Sanders DS Walker MM Zingone F Ciacci C January 2013 The Oslo definitions for coeliac disease and related terms Gut 62 1 43 52 doi 10 1136 gutjnl 2011 301346 PMC 3440559 PMID 22345659 a b c d e f g h Sapone A Bai JC Ciacci C Dolinsek J Green PH Hadjivassiliou M Kaukinen K Rostami K Sanders DS Schumann M Ullrich R Villalta D Volta U Catassi C Fasano A 2012 Spectrum of gluten related disorders consensus on new nomenclature and classification BMC Medicine Review 10 13 doi 10 1186 1741 7015 10 13 PMC 3292448 PMID 22313950 Food and Drug Administration January 2007 Food Labeling Gluten Free Labeling of Foods PDF Food and Drug Administration Archived from the original PDF on 2007 01 26 Tovoli F Masi C Guidetti E Negrini G Paterini P Bolondi L March 16 2015 Clinical and diagnostic aspects of gluten related disorders World J Clin Cases 3 3 275 84 doi 10 12998 wjcc v3 i3 275 PMC 4360499 PMID 25789300 a b c d e Volta U Caio G Tovoli F De Giorgio R September 2013 Non celiac gluten sensitivity questions still to be answered despite increasing awareness Cellular amp Molecular Immunology Review 10 5 383 92 doi 10 1038 cmi 2013 28 PMC 4003198 PMID 23934026 Pronin Darina Borner Andreas Weber Hans Scherf Ann 10 July 2020 Wheat Triticum aestivum L Breeding from 1891 to 2010 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and Other Edible Agents of Mental Disease Frontiers in Human Neuroscience 10 130 doi 10 5281 zenodo 1004705 PMC 4809873 PMID 27065833 a b c d e f Verbeke K February 2018 Nonceliac Gluten Sensitivity What Is the Culprit Gastroenterology 154 3 471 473 doi 10 1053 j gastro 2018 01 013 PMID 29337156 Although intolerance to fructans and other FODMAPs may contribute to NCGS they may only explain gastrointestinal symptoms and not the extraintestinal symptoms observed in NCGS patients such as neurologic dysfunction psychological disturbances fibromyalgia and skin rash 15 Therefore it is unlikely that they are the sole cause of NCGS a b c d e f Volta U De Giorgio R Caio G Uhde M Manfredini R Alaedini A March 2019 Nonceliac Wheat Sensitivity An Immune Mediated Condition with Systemic Manifestations Gastroenterol Clin North Am Review 48 1 165 182 doi 10 1016 j gtc 2018 09 012 PMC 6364564 PMID 30711208 Furthermore a role for the FODMAP eg fructans component of wheat as the sole trigger for 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