Celiac Disease: The Past and The Present

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Celiac Disease: The Past and The Present The Center for Celiac Research and Mucosal Biology Research Center University of Maryland School of Medicine Baltimore, Maryland, U.S.A. 1

Celiac Disease Roadmap: Where we are coming from? Where are we going? Years 2.5 M The Human race appears on the face of hearth Diet Fruits, nuts, tubers Occasional meat 61 118 S. Gee 2,000 First description 10,000 of CD Change from nomadic to settled life style Gluten as cause of CD Gluten free products Advent of agriculture Development of gluten containing grains 2

Spreading of Agriculture and Celiac Disease 1 Cereals domestication started 10,000 years ago in the Fertile Crescent 2 Catalhuyuc, The first town in the world was built 9,000 y ago INVERSE RELATIONSHIP BETWEEN CD FREQUENCY AND LENGHT OF TIME SINCE THE INTRODUCTION OF AGRICOLTURE? 4 CD genes confer disadvantage in areas of high cereal consumption 3 Agricolture slowly spread with a East-West gradient (1 Km/y) 3

On the Coeliac Affection There is a kind of chronic indigestion which is met with in persons of all ages, yet is especially apt to affect children between one and five years old. Signs of the disease are yielded by the faeces; being loose, not formed, but not watery; more bulky than the food taken would seem to account for The causes of the disease are obscure. Children who suffer from it are not all weak in constitution. Errors in diet may perhaps be a cause, but what error? Why, out of a family of children all brought up in much the same way, should one alone suffer? To regulate the food is the main part of treatment. The allowance of farinaceous food must be small; highly starchy food, rice, sago, cornflour are unfit. Malted food is better, also rusks or bread cut thin and well toasted on both sides. Gee S. On the celiac affection. St Bart Hosp Rep 1890; 24: 17-20. 4

The Banana Babies WK Dicke, 1905-1962 1 st case of CD at UMB: 1938 5

Definition Celiac disease is an autoimmune condition Occurs in genetically susceptible individuals DQ2 and/or DQ8 positive HLA haplotype is necessary but not sufficient A unique autoimmune disorder because: both the environmental trigger (gluten) and the autoantigen (tissue Transglutaminase) are known elimination of the environmental trigger leads to a complete resolution of the disease 6

Normal small bowel Celiac disease Gluten Gluten-free diet 7

Pathogenesis + = 8

Genetics Several genes are involved The most consistent genetic component depends on the presence of HLA-DQ (DQ2 and / or DQ8) genes Other genes (not yet identified) account for 60 % of the inherited component of the disease HLA-DQ2 and / or DQ8 genes are necessary (No DQ2/8, no Celiac Disease!) but not sufficient for the development of the disease Genes???? + HLA Gluten Celiac Disease 9

Dietary Factors The Grass Family - (GRAMINEAE) Subfamily Festucoideae Tribe Zizaneae Oryzeae Hordeae Aveneae Festuceaea Chlorideae wild rice rice wheat oat finger millet teff rye (ragi) barley 10

The Celiac Iceberg Symptomatic Celiac Disease Manifest mucosal lesion Silent Celiac Disease Latent Celiac Disease Normal Mucosa Genetic susceptibility: - DQ2, DQ8 Positive serology 11

Gastrointestinal Manifestations Most common age of presentation: 6-24 months ( Classic ) Chronic or recurrent diarrhea Abdominal distension Anorexia Failure to thrive or weight loss Abdominal pain Vomiting Constipation Irritability Rarely: Celiac crisis 12

Non Gastrointestinal Manifestations Most common age of presentation: older child to adult Dermatitis Herpetiformis Dental enamel hypoplasia of permanent teeth Osteopenia/Osteoporosis Short Stature Delayed Puberty Iron-deficient anemia resistant to oral Fe Hepatitis Arthritis Epilepsy with occipital calcifications Listed in descending order of strength of evidence 13

The Clinical Manifestations of Celiac Disease are More Heterogeneous Than Previously Appreciated: The North American Paradox A. Fasano, N Engl J Med 2003;348:2568-70. 14

What Happened During the past 15 years? The Recent CD Past History Seen Through the Center For Celiac Research 1. Established in 1996 www.celiaccenter.org 2. Multidisciplinary operation 3. Engaged in both basic science and clinical/translational research 4. Unique point of referral for CD patients (both pediatrics and adults) in USA. 5. Paramount goal: To increase the quality of life of CD patients and their families 15

How to achieve the paramount mission of the CFCR? 1. Implement the diagnosis to minimize errors and discomfort 2. Establish the dimension of the problem in North America 3. Increase the awareness of the disease 4. Create a network to work together toward specific goals 5. Implement the food labeling policy 6. Research and development 16

The Evolution of CD Serological Tests The availability of sensitive serological markers made it possible to discover CD even when the clinical suspicion was low.. AGA EMA ttg 1980 199 0 200 0 CFCR HLA 200 3 17

Diagnosis Diagnostic principles Confirm diagnosis before treating Diagnosis of Celiac Disease mandates a strict gluten-free diet for life following the diet is not easy QOL implications Failure to treat has potential long term adverse health consequences increased morbidity and mortality 18

Serological Test Comparison Sensitivity % Specificity % AGA-IgG 69 85 73 90 AGA-IgA 75 90 82 95 EMA (IgA) 85 98 97 100 TTG (IgA) 90 98 94 97 Farrell RJ, and Kelly CP. Am J Gastroenterol 2001;96:3237-46. 19

HLA Tests HLA alleles associated with Celiac Disease DQ2 found in 95% of celiac patients DQ8 found in remaining patients DQ2 found in ~30% of general population Value of HLA testing High negative predictive value Negativity for DQ2/DQ8 excludes diagnosis of Celiac Disease with 99% confidence Schuppan. Gastroenterology 2000;119:234 Kaukinen. Am J Gastroenterol 2002;97:695 20

HLA Tests Potential role for DQ2/DQ8 asymptomatic relatives Down, Turner & Williams syndrome type 1 diabetes diagnostic dilemmas 21

Endoscopic Findings Conventional endoscopy Videocapsule Endoscopy 22

Histological Features Normal 0 Infiltrative 1 Hyperplastic 2 Partial atrophy 3a Subtotal atrophy 3b Total atrophy 3c Horvath K. Recent Advances in Pediatrics, 2002. 23

How to achieve the paramount mission of the CFCR? 1. Implement the diagnostic tools to minimize errors 2. Establish the dimension of the problem in North America 3. Increase the awareness of the disease 4. Create a network to achieve specific goals 5. Implement the food labeling policy 6. Research and development 24

Epidemiology The old Celiac Disease Epidemiology: A rare disorder typical of infancy Wide incidence fluctuates in space (1/400 Ireland to 1/10000 Denmark) and in time A disease of essentially European origin 25

Risk Factors The Grains The Genes 26

Celiac Disease Epidemiological Study in USA Population screened 13145 Healthy Individuals 4126 Risk Groups 9019 Symptomatic subjects 3236 1st degree relatives 4508 2nd degree relatives 1275 Positive 31 Negative 4095 Positive 81 Negative 3155 Positive 205 Negative 4303 Positive 33 Negative 1242 Prevalence 1:133 Prevalence 1:40 Prevalence 1:22 Prevalence 1:39 Projected number of celiacs in the U.S.A.: 2,115,954 Actual number of known celiacs in the U.S.A.: 40,000 For each known celiac there are 53 undiagnosed patients. A. Fasano et al., Arch Int Med 2003;163:286-292. 27

Where we go from here? Search for the other 2,091,212 CD Patients 28

What is the best Strategy to Look for CD Subjects? General Screening? Case Findings? 29

Case Finding Study Catassi et al Am J Gastroenterol 2007;102:1-7 30

Case Finding Study Prevalence of CD (and 95% CI) in selected at-risk subgroup of investigated patients. The dotted area is the prevalence of CD in the general U.S. population (2). Catassi et al Am J Gastroenterol 2007;102:1-31

Case Finding Study The level of awareness of the disease among health-care professional is still low. Therefore, the disease remains highly under-diagnosed in North America. Our studies showed that our active case-finding strategy increased the rate of diagnosis by primary care physicians by 32- to 43-fold. Patients experiencing both intestinal symptoms (diarrhea, irritable bowel syndrome, constipation, and bloating) and extraintestinal symptoms (thyroid diseases, iron deficient anemia, osteoporosis) are at higher risk for CD compared with the general population. Our results have implications that may resolve in better patient care a more cost-effective approach to the diagnosis of CD, and a greater awareness among health-care professionals. Catassi et al Am J Gastroenterol 2007;102:1-32

How to achieve the paramount mission of the CFCR? 1. Implement the diagnostic tools to minimize errors 2. Establish the dimension of the problem in North America 3. Increase the awareness of the disease 4. Create a network to achieve specific goals 5. Implement the food labeling policy 6. Research and development 33

CFCR initiatives to increase the awareness of celiac disease in the North America 1. International Walk for Celiac Disease; 2. Capitalization on the epidemiology study for PR coverage 3. Aggressive educational campaign for HCP; 4. High profile speak person (Rich Gannon) 5. Local and national coverage on newspapers (Wall Street Journal, Washington Post) and TV networks (Today Show). 34

CFCR initiatives to increase the awareness of celiac disease in the North America: The educational initiatives 1. 9 th International Symposium on Celiac Disease (2000); 2. NIH Consensus Conference (June 2004); 3. CDHNF initiative for CD national campaign (2004); 4. NASPGHAN CD Guidelines (2005); 5. State of the Art Lecture at the World Congress of Gastroenterology, Montreal Sept 11-14, 2005; 6. State of the Art Lecture at the NASPGHAN Annual Meeting (Oct 2005) where CD has been named the Disease of the Year ; 7. State of the Art Lecture at the American Academy of Pediatrics, October 2005. 35

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How to achieve the paramount mission of the CFCR? 1. Implement the diagnostic tools to minimize errors 2. Establish the dimension of the problem in the U.S.A. 3. Increase the awareness of the disease 4. Create a network to achieve specific goals (ACDA) 5. Implement the food labeling policy 6. Research and development Catassi et al Am J Clin Nutr. 2007;85:160-6 39

n e t u l g 20000 15000 10000 5000 1000 The dose-effect response (typical CD cases) y l i a d 500 50 0 1 2 3 4 small intestinal mucosa damage 40

Gluten Treshold in GF food IT TAKES TWO TO TANGO! The daily gluten intake is the product of gluten ppm in food and daily intake of wheat substitutes Then the decision on the gluten threshold in GF food must take into account the variable intake of wheat substitutes 41

Intake of gluten-free products in Europe Gibert A et al, EJGH 2006 42

Tolerable daily intake of gluten and ppm of gluten in food for celiacs 50 g 100 g 200 g 300 g 200 ppm 100 ppm 50 ppm 10 mg 5 mg 2.5 mg 20 mg 10 mg 5 mg 40 mg 20 mg 10 mg 60 mg 30 mg 15 mg 20 ppm 1 mg 2 mg 4 mg 6 mg Catassi et al Am J Clin Nutr. 2007;85:160-43

Toward a safe gluten p p ( n e t u l g 180 160 140 120 100 80 60 40 20 0 threshold WHERE DO WE STAND NOW 200 risk area 0 100 200 300 400 500 wheat substitutes (g x day) 44

Toward a safe gluten p p ( n e t u l g 200 180 160 140 120 100 80 60 40 20 0 safe area threshold A PRUDENT VIEW grey area risk area 0 100 200 300 400 500 wheat substitutes (g x day) 45

Key Questions About the Double Threshold Proposed by Codex Is there an advantage in terms of availability of products? Is there an advantage in terms of palatability? Is there an advantage in terms of economics? f the answer is no to any of these questions, why risking? 46

Catassi et al Am J Clin Nutr. 2007;85:160-6 47

How to achieve the paramount mission of the CFCR? 1. Implement the diagnostic tools to minimize errors 2. Establish the dimension of the problem in the U.S.A. 3. Increase the awareness of the disease 4. Create a network to achieve specific goals 5. Implement the food labeling policy 6. Research and development 48

Celiac Disease: The Future To Be Continued. 49