Your search keyword '"S. Percopo"' showing total 45 results

1. Concordance, disease progression, and heritability of coeliac disease in Italian twins

Author

M.G. Limongelli, Luigi Greco, Mara Giordano, Giuseppe Magazzù, Corrado Fagnani, Lorenza Nisticò, Iolanda Coto, Patricia Momigliano-Richiardi, Sandra D'Alfonso, Concettina Sferlazzas, Franco Paparo, Maria Antonietta Stazi, Rodolfo Cotichini, S. Percopo, Nistico, L, Fagnani, C, Coto, I, Percopo, S, Cotichini, R, Limongelli, Mg, Paparo, F, D'Alfonso, S, Giordano, M, Sferlazzas, C, Magazzu, G, MOMIGLIANO RICHIARDI, P, Greco, Luigi, and Stazi, Ma

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Concordance, Population, Coeliac Disease, Environment, Biology, FAMILIES, HLA-DQ Antigens, Internal medicine, Genotype, Diseases in Twins, Twins, Dizygotic, medicine, Humans, Genetic Predisposition to Disease, ASSAY, Registries, EUROPEAN POPULATIONS, PREVALENCE, TISSUE, PSORIASIS, ANTIBODY, ONSET, PAIRS, RISK, education, Survival analysis, education.field_of_study, Histocompatibility Testing, Hazard ratio, Gastroenterology, HLA-DR Antigens, Twins, Monozygotic, Heritability, DNA Fingerprinting, Survival Analysis, Zygosity, Confidence interval, Celiac Disease, Italy, Immunology, Disease Progression, Female

Abstract

Background and aims: We adopted the twin method to disentangle the genetic and environmental components of susceptibility to coeliac disease (CD). We estimated disease concordance rate by zygosity and HLA genotypes, discordance times, progression rates to disease, and heritability. Methods: We crosslinked the Italian Twin Registry with the membership lists of the Italian Coeliac Disease Association and recruited 23 monozygotic (MZ) and 50 dizygotic (DZ) twin pairs with at least one affected member. Zygosity was assigned by DNA fingerprinting, and HLA-DQ and DR alleles were genotyped. Disease status was ascertained by antiendomysial, anti-human tissue transglutaminase antibodies, and bowel biopsy. Results: Concordance was significantly higher in MZ (83.3% probandwise, 71.4% pairwise) than in DZ (16.7% probandwise, 9.1% pairwise) pairs. Concordance was not affected by sex or HLA genotype of the co-twin and being MZ was significantly associated with the occurrence of CD (Cox adjusted hazard ratio 14.3 (95% confidence interval 4.0–50.3)). In 90% of concordant pairs the discordance time was ⩽2 years. MZ and DZ co-twins had 70% and 9% cumulative probability of having symptomatic or silent forms of CD, respectively, within five years. Under ACE (additive genetic, common, and unshared environmental factors) models, with CD population prevalences of 1/91 and 1/1000, heritability estimates were 87% and 57%, respectively. Conclusion: MZ pairs have a high probability of being concordant, regardless of sex or HLA genotype. Most of the affected co-twins receive a diagnosis within two years. A remarkable proportion of phenotypic variance is due to genetic factors.

Published

2006

2. Additional factor in some HLA DR3/DQ2 haplotypes confers a fourfold increased genetic risk of celiac disease

Author

Patricia Momigliano-Richiardi, Kati Karell, V. Mantovani, Iolanda Coto, E. Suoraniemi, S. Percopo, Elisabetta Bolognesi, K. Mustalahti, Luigi Greco, Jukka Partanen, and Markku Mäki

Subjects

Genetics, Immunology, Haplotype, HLA-DR3, General Medicine, Human leukocyte antigen, Disease, Biology, Biochemistry, Immunology and Allergy, Risk factor, Genetic risk, Allele, Gene

Abstract

Although HLA-DQ genes are the major celiac disease (CD) susceptibility genes, results from Finnish families suggest that not all DQ2-encoding haplotypes confer equal susceptibility to CD, implying the effect of other gene(s) in the HLA region. The aim of the present work was to extend and confirm the aforementioned results in a southern European population ( Italian) and to better localize the additional risk factor/s. The association of nine loci spanning the HLA region from DR to HFE, 4.5-Mb telomeric of HLA-A, was tested. The analysis was performed by comparing marker frequencies in DR3-DQ2 haplotypes transmitted and non-transmitted to the affected offspring in 156 Italian CD families selected for having at least one DR3-positive parent. The same analysis was performed independently in 101 Finnish CD families selected with the same criteria. Three alleles, MICA-A5.1, MICB-CA24 and MIB-350, all characteristic of the B8-DR3 extended haplotype, showed a significantly increased frequency in DR3 transmitted haplotypes in the Italian families. DR3 haplotypes carrying the combination of these alleles conferred an approximate fourfold increased CD risk. B8-DR3 transmitted haplotypes were significantly more conserved telomerically down to the MIC-Class I region. Similar results were seen in the Finnish families. The major conclusion that holds true in both populations is that, while DQ2 is an absolute requirement for the development of CD, the presence of an additional genetic factor within the MIC-Class I region confers an approximate 4-fold increased risk of the disease.

Published

2003

3. The first large population based twin study of coeliac disease

Author

C. D'Agate, Roberto Tosi, Iolanda Coto, Rodolfo Cotichini, Maria Antonietta Stazi, M.G. Limongelli, S. Percopo, Valeria Gasperi, Lucia Sacchetti, Maria Maglio, Nadia Tinto, Luigi Greco, F. Paparo, N Di Cosmo, and R Romino

Subjects

Adult, Male, medicine.medical_specialty, Adolescent, Concordance, Biology, HLA-DQ alpha-Chains, Genetic determinism, Coeliac disease, HLA-DQ Antigens, Internal medicine, Genotype, Diseases in Twins, Odds Ratio, medicine, HLA-DQ beta-Chains, Humans, Genetic Predisposition to Disease, Genetics, Histocompatibility Testing, Gastroenterology, nutritional and metabolic diseases, HLA-DR Antigens, Odds ratio, medicine.disease, DNA Fingerprinting, Twin study, digestive system diseases, Zygosity, Genetic load, Celiac Disease, Logistic Models, Small Intestine, Female, HLA-DRB1 Chains

Abstract

Background and aims: The genetic load in coeliac disease has hitherto been inferred from case series or anecdotally referred twin pairs. We have evaluated the genetic component in coeliac disease by estimating the concordance rate for the disease among twin pairs in a large population based study. Methods: The Italian Twin Registry was matched with the membership lists of a patient support group. Forty seven twin pairs were recruited and screened for antiendomysial (EMA) and antihuman-tissue transglutaminase (anti-tTG) antibodies; zygosity was verified by DNA fingerprinting and twins were typed for HLA class II DRB1 and DQB1 molecules. Results: Concordance rates for coeliac disease differ significantly between monozygotic (MZ) (0.86 probandwise and 0.75 pairwise) and dizygotic (DZ) (0.20 probandwise and 0.11 pairwise) twins. This is the highest concordance so far reported for a multifactorial disease. A logistic regression model, adjusted for age, sex, number of shared HLA haplotypes, and zygosity, showed that genotypes DQA1*0501/DQB1*0201 and DQA1*0301/DQB1*0302 (encoding for heterodimers DQ2 and DQ8, respectively) conferred to the non-index twin a risk of contracting the disease of 3.3 and 1.4, respectively. The risk of being concordant for coeliac disease estimated for the non-index twin of MZ pairs was 17 (95% confidence interval 2.1–134), independent of the DQ at risk genotype. Conclusion: This study provides substantial evidence for a very strong genetic component in coeliac disease, which is only partially due to the HLA region.

Published

2002

4. Linkage and association study of the CTLA-4 region in coeliac disease for Italian and Tunisian populations

Author

Idriss Djilali-Saiah, Françoise Clerget-Darpoux, Sophie Caillat-Zucman, S. Percopo, M. C. Fulchignoni-Lataud, F. Clot, F. Bouguerra, J.L. Serre, C. Renoux, Luigi Greco, and Marie-Claude Babron

Subjects

Genetics, Linkage disequilibrium, education.field_of_study, Immunology, Population, chemical and pharmacologic phenomena, General Medicine, Transmission disequilibrium test, Biology, medicine.disease, Biochemistry, Coeliac disease, Exon, Genetic marker, Genetic linkage, CTLA-4, medicine, Immunology and Allergy, education

Abstract

Coeliac disease (CD) is a multifactorial disease for which there is an intensive search for genetic risk factors. Some authors found an association between the CTLA-4 region and CD. In the present work, we investigate the possible implication of the CTLA-4 region as a genetic risk factor for CD, through two statistical approaches: the maximum likelihood score (MLS) test in a large Italian sample of affected sib-pairs using polymorphic genetic markers on chromosome 2, and the transmission disequilibrium test (TDT) in continental Italian and Tunisian families using the CTLA-4 exon 1 49 A/G polymorphism. None of these approaches provides evidence for linkage or association between the CTLA-4 region and CD. This might result from a difference in the CTLA-4 region from population to population, either in its involvement as a risk factor or in the strength of linkage disequilibrium.

Published

1999

5. The coeliac disease task force 'Free from Gluten' 'Improved knowledge to cure coeliac disease'

Author

L Greco and S Percopo

Subjects

Adult, Pediatrics, medicine.medical_specialty, Glutens, Population Dynamics, Fund Raising, Patient Advocacy, digestive system, Coeliac disease, Cost of Illness, Basic research, Cohort Effect, Prevalence, medicine, Humans, Mass Screening, Selection, Genetic, Child, chemistry.chemical_classification, Organizations, Task force, business.industry, Incidence, nutritional and metabolic diseases, Gluten intolerance, General Medicine, European population, medicine.disease, Gluten, digestive system diseases, Biotechnology, Celiac Disease, Italy, chemistry, Pediatrics, Perinatology and Child Health, Cost analysis, Disease Susceptibility, Population screening, business, Food Hypersensitivity

Abstract

Gluten has recently been introduced into the diet of the Mediterranean and European population, but a considerable proportion has not adapted to this change and has developed intolerance to gluten. At least one million EEC citizens are gluten intolerant. In Italy each year 12 million ECU is spent in the diagnosis of uncomplicated gluten intolerance, 10 million ECU for complex diagnosis and 32 million ECU for long-term complications and malignancies. The total financial load of gluten intolerance, in its present state, is about 150 million ECU/year in Italy. Four million ECU is actually needed to develop a genetic probe, which may make the population screening feasible. A National Task Force "Free from Gluten" has been set up by the Italian Coeliac Society to stimulate fund-raising activities supporting genetic and basic research on gluten intolerance.

Published

1996

6. The first large population-based twin study of Coeliac Disease

Author

GRECO, LUIGI, MAGLIO, MARIANTONIA, R. ROMINO, I. COTO, N. DI COSMO, S. PERCOPO, F. PAPARO, V. GASPERI, MG LIMONGELLI, R. COTICHINI, C. D\'AGATE, Greco, Luigi, R., Romino, I., Coto, N., DI COSMO, S., Percopo, Maglio, Mariantonia, F., Paparo, V., Gasperi, Mg, Limongelli, R., Cotichini, and C., D\'Agate

Published

2002

7. TheIL12Bgene does not confer susceptibility to coeliac disease

Author

Lena Samuelsson, Patricia Momigliano-Richiardi, A.S. Louka, Ludvig M. Sollid, J. Ek, S. Percopo, A. H. Gudjonsdottir, Iolanda Coto, Jan Wahlström, Henry Ascher, Sandra D'Alfonso, Marta Mellai, Luigi Greco, Å. Torinsson Naluai, and Mara Giordano

Subjects

chemistry.chemical_classification, Immunology, nutritional and metabolic diseases, Single-nucleotide polymorphism, General Medicine, Human leukocyte antigen, Disease, Biology, medicine.disease, Biochemistry, Gluten, Coeliac disease, chemistry, Genetics, medicine, Interleukin 12, Immunology and Allergy, Allele, Gene

Abstract

Coeliac disease (CD) is a chronic inflammatory disorder where dietary gluten is not tolerated. In the lesion there are gluten reactive T cells predominantly secreting gamma-interferon. Both HLA and non-HLA genes contribute to CD susceptibility. Interleukin-12 (IL-12) regulates gamma-interferon production. The IL12B gene is located in a region (5q31.1-33.1) where there is evidence for linkage with CD. Allele 1 of an IL12B 3'UTR single-nucleotide polymorphism leads to increased expression of IL-12, and was recently implicated in susceptibility for type 1 diabetes (T1D). We found no evidence for association of allele 1 to CD by the transmission/disequilibrium test or case-control approach. No increased frequency was observed in patients belonging to families where the disease was linked to markers on chromosome 5q. Unlike T1D, allele 1 does not appear to confer susceptibility to CD.

Published

2002

8. Variable phenotype associated with SP-C gene mutations: fatal case with the I73T mutation

Author

Francesca Santamaria, Silvia Montella, H.S. Cameron, G. Pettinato, S. Percopo, L.M. Nogee, S., Percopo, H. S., Cameron, L. M., Nogee, Pettinato, Guido, S., Montella, and Santamaria, Francesca

Subjects

Pulmonary and Respiratory Medicine, Pregnancy, Mutation, business.industry, Interstitial lung disease, respiratory system, Gene mutation, medicine.disease, medicine.disease_cause, Phenotype, respiratory tract diseases, Immunology, Missense mutation, Medicine, business, Pulmonary alveolar proteinosis, Gene

Abstract

To the Editors: We read with great interest the report by Brasch et al . 1 on a case of interstitial lung disease (ILD) due to a de novo heterozygous missense mutation in the surfactant protein-C gene (SFTPC), which resulted in the substitution of threonine for isoleucine in codon 73 of the propeptide of the surfactant protein (SP)-C proprotein (I73T). Histological findings were consistent with nonspecific interstitial pneumonia (NSIP) and pulmonary alveolar proteinosis (PAP) features. Therapy included whole-lung lavages and anti-inflammatory drugs, and the child is still alive. The natural history of lung disease associated with SP-C mutations is poorly characterised, with unpredictable short- and long-term outcomes. In order to emphasise the phenotypic variability of SFTPC mutations, we now report a child with fatal lung disease due to the SP-C I73T mutation. The child was a full-term male, born to unrelated parents from an uneventful twin dizygotic pregnancy. At 3 months, he developed episodes of asthmatic bronchitis. At 9 months, he was admitted to the …

Published

2004

9. Evidence of a correlation between mannose binding lectin and celiac disease: a model for other autoimmune diseases

Author

Sergio Crovella, V. Baldas, Michele Boniotto, Serena Vatta, Antonio Amoroso, Alessandro Ventura, Oriano Radillo, Francesco Tedesco, Laura Braida, S. Percopo, Tarcisio Not, Marcella Montico, Boniotto, M, Braida, L, Baldas, V, Not, Tarcisio, Ventura, Alessandro, Vatta, S, Radillo, O, Tedesco, F, Percopo, S, Montico, M, Amoroso, A, and Crovella, Sergio

Subjects

Adult, Male, Adolescent, Biopsy, Mannose binding lectin, Autoimmunity, Apoptosis, Human leukocyte antigen, Biology, medicine.disease_cause, Mannose-Binding Lectin, Coeliac disease, Autoimmune Diseases, Gene Frequency, HLA-DQ Antigens, Drug Discovery, Genotype, Celiac disease, Polymorphisms, medicine, Humans, Genetic Predisposition to Disease, Child, Genetics (clinical), Mannan-binding lectin, Autoimmune disease, Polymorphism, Genetic, medicine.diagnostic_test, nutritional and metabolic diseases, Infant, Middle Aged, medicine.disease, digestive system diseases, Genotype frequency, Intestines, Celiac Disease, Haplotypes, Italy, Case-Control Studies, Child, Preschool, Immunology, Molecular Medicine, Female

Abstract

Celiac disease is a multifactorial disorder caused, in genetically susceptible patients, by the ingestion of dietary gluten. Very little is known about the genetic factors, but there is a strong association of two HLA haplotypes (DQ2 or alpha1*05, beta1*02 and DQ8 or alpha1*0301, beta1*0302) with the disease. We investigated the relationship between polymorphisms in the first exon of the MBL2 gene, which encodes for mannose binding lectin (MBL) and celiac disease. Moreover we studied the MBL role by immunohistochemistry and TUNEL. Results were confirmed by clinical findings. We enrolled 149 Italian celiac patients; 116 were characterized by the presence of DQ2 or DQ8. The HLA haplotype was established by allelic specific PCR while the MBL2 genotype was resolved by melting temperature assay. Immunohistochemistry and TUNEL assays were performed on serial sections of biopsy specimens from celiac patients and healthy controls. MBL2 allele and genotype frequencies varied significantly between celiac patients and healthy controls. The frequencies of the 0 allele were 28% in DQ2 or DQ8 celiac patients, 36% in HLA atypical celiac patients, and 22% in healthy controls. Interestingly, the MBL2 0/0 genotype was present in 7 of 33 HLA atypical celiac patients (21%) and in 13 of 116 HLA typical celiac patients (13%) but in only 7 of 147 healthy controls (5%). Furthermore, we found that MBL2 genotype is strongly associated with the occurrence of secondary autoimmune diseases. Immunohistochemistry and TUNEL findings support a role of MBL2 in the clearance of apoptotic cells. In conclusion, MBL2 variants, responsible for lower MBL levels, are associated with celiac disease and higher risk of developing autoimmune diseases. Here we propose a role for MBL in the disease which could be easily applied to other autoimmune disorders.

Published

2004

10. In vitro-deranged intestinal immune response to gliadin in type 1 diabetes

Author

Francesco Paparo, S. Percopo, Francesca Lombardi, Luigi Greco, Riccardo Troncone, Gerardo Nardone, Renata Auricchio, Maria Maglio, Giuliana Valerio, Adriana Franzese, Auricchio, Renata, Paparo, F, Maglio, M, Franzese, Adriana, Lombardi, F, Valerio, G, Nardone, GERARDO ANTONIO PIO, Percopo, S, Greco, Luigi, and Troncone, R.

Subjects

Male, Adolescent, Endocrinology, Diabetes and Metabolism, Biopsy, Inflammation, digestive system, Gliadin, Immune system, Organ Culture Techniques, HLA Antigens, Immunopathology, Internal Medicine, medicine, Humans, IL-2 receptor, Intestinal Mucosa, Child, Autoimmune disease, Type 1 diabetes, Lamina propria, biology, business.industry, medicine.disease, Immunohistochemistry, digestive system diseases, medicine.anatomical_structure, Diabetes Mellitus, Type 1, Jejunum, Case-Control Studies, Immunology, Antibody Formation, biology.protein, Female, medicine.symptom, business

Abstract

Dietary gluten has been associated with an increased risk of type 1 diabetes. We have evaluated inflammation and the mucosal immune response to gliadin in the jejunum of patients with type 1 diabetes. Small intestinal biopsies from 17 children with type 1 diabetes without serological markers of celiac disease and from 50 age-matched control subjects were examined by immunohistochemistry. In addition, biopsies from 12 type 1 diabetic patients and 8 control subjects were cultured with gliadin or ovalbumin peptic-tryptic digest and examined for epithelial infiltration and lamina propria T-cell activation. The density of intraepithelial CD3(+) and gammadelta(+) cells and of lamina propria CD25(+) mononuclear cells was higher in jejunal biopsies from type 1 diabetic patients versus control subjects. In the patients' biopsies cultured with peptic-tryptic gliadin, there was epithelial infiltration by CD3(+) cells, a significant increase in lamina propria CD25(+) and CD80(+) cells and enhanced expression of lamina propria CD54 and crypt HLA-DR. No such phenomena were observed in control subjects, even those with celiac disease-associated HLA haplotypes. In conclusion, signs of mucosal inflammation were present in jejunal biopsies from type 1 diabetic patients, and organ culture studies indicate a deranged mucosal immune response to gliadin.

Published

2004

11. HLA-DQ relative risks for coeliac disease in European populations: a study of the European Genetics Cluster on Coeliac Disease

Author

S. Percopo, A.S. Louka, Patricia Margaritte-Jeannin, Françoise Clerget-Darpoux, Marie-Claude Babron, J.P. Hugot, F. Clot, Ludvig M. Sollid, Luigi Greco, Henry Ascher, Mathieu Bourgey, and Iolanda Coto

Subjects

Proband, Genetics, Risk, Genotype, Immunology, Haplotype, General Medicine, Biology, medicine.disease, Disease cluster, Biochemistry, Coeliac disease, Europe, Celiac Disease, Gene Frequency, Haplotypes, Relative risk, HLA-DQ Antigens, HLA-DQ, medicine, Immunology and Allergy, Genetic Predisposition to Disease, Allele frequency

Abstract

Coeliac disease is an enteropathy due to an intolerance to gluten. The association between HLA-DQ genes and CD is well established. The majority of patients carry the HLA-DQ heterodimer encoded by DQA1*05/DQB1*02, either in cis or in trans. The remaining patients carry either part of the DQ heterodimer or DQA1*03-DQB1*0302. The aim of the study was to estimate the risks associated with different DQ genotypes in European populations. HLA information was available for 470 trio families from four countries: France (117), Italy (128), and Norway and Sweden (225). Five DQA1-DQB1 haplotypes were considered and control haplotype frequencies were estimated from the set of parental haplotypes not transmitted to the affected child. The possible genotypes were grouped into five genotype groups, based on the hierarchy of risk reported in the literature. A north-south gradient in the genotype group frequencies is observed in probands: homogeneity is strongly rejected between all country pairs. For each country, the relative risks associated with each genotype group were computed taking into account the control haplotype frequencies. Homogeneity of relative risks between countries was tested pairwise by maximum likelihood ratio statistics. The hypothesis of homogeneity of relative risks is rejected (P is approximately 10(-6)) for all country pairs. In conclusion, the gradient in the genotype group frequencies in probands is not only due to differences in haplotype frequencies but also due to differences in genotype relative risks in the studied populations; the relative risks associated with each DQ genotype group are different between northern and southern European countries; neither are they ordered in the same way.

Published

2004

12. Candidate gene region 2q33 in European families with coeliac disease

Author

Åsa Torinsson Naluai, Ludvig M. Sollid, Françoise Clerget-Darpoux, Iolanda Coto, Luigi Greco, P. Holopainen, Henry Ascher, S J Moodie, S. Percopo, Paul J. Ciclitira, Jukka Partanen, and F. Clot

Subjects

Antigens, Differentiation, T-Lymphocyte, Genetic Markers, Male, Candidate gene, Genetic Linkage, Immunology, Programmed Cell Death 1 Receptor, Biology, Biochemistry, White People, Inducible T-Cell Co-Stimulator Protein, CD28 Antigens, Gene Frequency, Genetic linkage, Antigens, CD, Genetics, Genetic predisposition, Immunology and Allergy, Humans, CTLA-4 Antigen, Genetic Predisposition to Disease, Allele, Allele frequency, Alleles, Genetic association, Polymorphism, Genetic, Haplotype, Chromosome Mapping, General Medicine, Antigens, Differentiation, Europe, Celiac Disease, Haplotypes, Genetic marker, Chromosomes, Human, Pair 2, Antigens, Surface, Female, Apoptosis Regulatory Proteins

Abstract

Chromosome region 2q33 harbours a cluster of genes, CTLA-4, CD28, ICOS and closely located PD-1, all related to immune activation and considered as promising candidate genes for susceptibility to coeliac disease (CD). We present here the results of a genetic linkage and association analysis of nine markers located in this gene region in a large combined European material of 796 families with CD from Finland, Sweden, Norway, UK, France and Italy. The joint analysis supports earlier findings that this susceptibility locus, assigned as CELIAC3, merits further studies. Nominally significant linkage to CD was found in 314 families including affected sib pairs. Each of the five populations showed weak associations to several marker alleles, but the analysis revealed, however, no conclusive evidence for a primary functional gene or gene variant present in the total set of families. The results suggest that the CD risk due to 2q33 gene region is complex and may involve more than one susceptibility allele, which possibly differ from other autoimmune diseases.

Published

2004

13. Additional factor in some HLA DR3/DQ2 haplotypes confers a fourfold increased genetic risk of celiac disease

Author

E, Bolognesi, K, Karell, S, Percopo, I, Coto, L, Greco, V, Mantovani, E, Suoraniemi, J, Partanen, K, Mustalahti, M, Mäki, and P, Momigliano-Richiardi

Subjects

Genetic Markers, Celiac Disease, HLA-DR3 Antigen, Haplotypes, Italy, HLA-DQ Antigens, Humans, Genetic Predisposition to Disease, Finland

Abstract

Although HLA-DQ genes are the major celiac disease (CD) susceptibility genes, results from Finnish families suggest that not all DQ2-encoding haplotypes confer equal susceptibility to CD, implying the effect of other gene(s) in the HLA region. The aim of the present work was to extend and confirm the aforementioned results in a southern European population ( Italian) and to better localize the additional risk factor/s. The association of nine loci spanning the HLA region from DR to HFE, 4.5-Mb telomeric of HLA-A, was tested. The analysis was performed by comparing marker frequencies in DR3-DQ2 haplotypes transmitted and non-transmitted to the affected offspring in 156 Italian CD families selected for having at least one DR3-positive parent. The same analysis was performed independently in 101 Finnish CD families selected with the same criteria. Three alleles, MICA-A5.1, MICB-CA24 and MIB-350, all characteristic of the B8-DR3 extended haplotype, showed a significantly increased frequency in DR3 transmitted haplotypes in the Italian families. DR3 haplotypes carrying the combination of these alleles conferred an approximate fourfold increased CD risk. B8-DR3 transmitted haplotypes were significantly more conserved telomerically down to the MIC-Class I region. Similar results were seen in the Finnish families. The major conclusion that holds true in both populations is that, while DQ2 is an absolute requirement for the development of CD, the presence of an additional genetic factor within the MIC-Class I region confers an approximate 4-fold increased risk of the disease.

Published

2003

14. Saturation of the 5q31-q33 candidate region for coeliac disease

Author

Françoise Clerget-Darpoux, Michael B. Whalen, F. Landolfo, Marie-Claude Babron, S. De Virgiliis, Luigi Greco, S. Percopo, Iolanda Coto, Percopo, S, Babron, Mc, Whalen, M, DE VIRGILIIS, S, Coto, I, Clergetdarpoux, F, Landolfo, F, and Greco, Luigi

Subjects

Genetic Markers, Genetics, Candidate gene, Human leukocyte antigen, Biology, medicine.disease, Genome, Coeliac disease, Intestinal malabsorption, Celiac Disease, Gene mapping, Genetic marker, medicine, Susceptibility locus, Chromosomes, Human, Pair 5, Humans, Genetic Predisposition to Disease, Genetics (clinical)

Abstract

The first genome wide screening performed on Italian affected sib-pair families (Greco et al. 1998) gave evidence for linkage with coeliac disease in the 5q region. This finding was replicated in a second independent dataset (Greco et al. 2001). Overall, pooling both samples, the highest MLS value (2.92) was found for the most centromeric marker tested, D5S640. In the present study, the 5q31-q33 region was saturated with 12 new markers around D5S640, in order to verify whether there would be a shift of the MLS position. This study allowed us to support our previous finding of linkage for the region 5q31-q33, with the most significant MLS value at D5S2014, very close to the marker D5S640. No evidence for interaction between this risk factor and the one in the HLA region was found. Furthermore, many different groups have independently obtained analogous results for this region, confirming the presence of a susceptibility locus in the region 5q31-q33. This region contains several interesting candidate genes for coeliac disease.

Published

2003

15. The IL12B gene does not confer susceptibility to coeliac disease

Author

A S, Louka, A, Torinsson Naluai, S, D'Alfonso, H, Ascher, I, Coto, J, Ek, M, Giordano, A H, Gudjónsdóttir, M, Mellai, P, Momigliano-Richiardi, S, Percopo, L, Samuelsson, J, Wahlström, L, Greco, and L M, Sollid

Subjects

Intestines, Celiac Disease, Polymorphism, Genetic, Italy, Interleukin-12 Subunit p40, HLA-DQ Antigens, HLA-DQ beta-Chains, Humans, Genetic Predisposition to Disease, Scandinavian and Nordic Countries, Interleukin-12, Alleles, HLA-DQ alpha-Chains

Abstract

Coeliac disease (CD) is a chronic inflammatory disorder where dietary gluten is not tolerated. In the lesion there are gluten reactive T cells predominantly secreting gamma-interferon. Both HLA and non-HLA genes contribute to CD susceptibility. Interleukin-12 (IL-12) regulates gamma-interferon production. The IL12B gene is located in a region (5q31.1-33.1) where there is evidence for linkage with CD. Allele 1 of an IL12B 3'UTR single-nucleotide polymorphism leads to increased expression of IL-12, and was recently implicated in susceptibility for type 1 diabetes (T1D). We found no evidence for association of allele 1 to CD by the transmission/disequilibrium test or case-control approach. No increased frequency was observed in patients belonging to families where the disease was linked to markers on chromosome 5q. Unlike T1D, allele 1 does not appear to confer susceptibility to CD.

Published

2002

16. Existence of a genetic risk factor on chromosome 5q in Italian coeliac disease families

Author

Patricia Momigliano-Richiardi, S. De Virgiliis, Giorgio Casari, F. Clot, Marie-Claude Babron, J.L. Serre, V. Mantovani, Luigi Greco, A. Lemainque, A. D'alfonso, S. Percopo, Gino Roberto Corazza, Paolo Gasparini, Hana Selinger-Leneman, M. C. Fulchignoni-Lataud, Giuseppe Iacono, Roberto Tosi, Patrizia Zavattari, Françoise Clerget-Darpoux, R. Sica, Greco, L, Babron, Mc, Corazza, Gr, Percopo, S, Sica, R, Clot, F, Fulchignoni Lataud, Mc, Zavattari, P, Momigliano Richiardi, P, Casari, GIORGIO NEVIO, Gasparini, P, Tosi, R, Mantovani, V, De Virgiliis, S, Iacono, G, D'Alfonso, A, Selinger Leneman, H, Lemainque, A, Serre, Jl, and Clerget Darpoux, F.

Subjects

Genetic Markers, Male, Human leukocyte antigen, Biology, Genome, Coeliac disease, Genetic determinism, Chromosomes, Risk Factors, Genetics, medicine, Genetic predisposition, Humans, Risk factor, Genetics (clinical), Linkage (software), Family Health, Chromosome, medicine.disease, Celiac Disease, Italy, Immunology, Chromosomes, Human, Pair 5, Female, Lod Score

Abstract

Coeliac disease (CD) is a malabsorptive disorder of the small intestine resulting from ingestion of gluten. The HLA risk factors involved in CD are well known but do not explain the whole genetic susceptibility. Several regions of potential linkage on chromosomes 3q, 5q, 10q, 11q, 15q and 19q have already been reported in the literature. These six regions were analyzed with the Maximum Lod Score method on a dense set of markers. A new sample of 89 Italian sibpairs was available for study. There was no evidence for linkage for any of the regions tested, except for chromosome 5q. For this region, our data, as well as a sample of 93 sibpairs from our first genome screen (Greco et al. 1998), are compatible with the presence of a risk factor for CD with a moderate effect.

Published

2000

17. Study of two ectopeptidases in the susceptibility to celiac disease: Two newly identified polymorphisms of dipeptidylpeptidase IV

Author

Marie-Claude Babron, Marie-Claude Fulchignoni-Lataud, Françoise Clerget-Darpoux, F. Bouguerra, F. Clot, Jean-Louis Serre, S. Percopo, Mara Giordano, L. Greco, Clot, Fabienne, Babron, Marie Claude, Percopo, Selvaggia, Giordano, Mara, Bouguerra, Faouzi, Clerget Darpoux, Francoise, Greco, Luigi, Serre, Jean Loui, and Fulchignoni Lataud, Marie Claude

Subjects

Adult, Male, Linkage disequilibrium, Tunisia, Histology, Dipeptidyl Peptidase 4, Medicine (miscellaneous), Disease, CD13 Antigens, Biology, Linkage Disequilibrium, Coeliac disease, Intestinal malabsorption, Dipeptidyl-dipeptidase, Immunopathology, Membrane alanyl aminopeptidase, medicine, Humans, Genetic Predisposition to Disease, Child, Dipeptidylpeptidase iv, Polymorphism, Genetic, Gastroenterology, medicine.disease, Celiac Disease, Italy, Immunology, Pediatrics, Perinatology and Child Health, Female, Food Science

Abstract

No abstract available

Published

2000

18. Linkage and association study of the CTLA-4 region in coeliac disease for Italian and Tunisian populations

Author

F, Clot, M C, Fulchignoni-Lataud, C, Renoux, S, Percopo, F, Bouguerra, M C, Babron, I, Djilali-Saiah, S, Caillat-Zucman, F, Clerget-Darpoux, L, Greco, and J L, Serre

Subjects

Adult, Family Health, Genetic Markers, Male, Immunoconjugates, Polymorphism, Genetic, Tunisia, Genetic Linkage, Antigens, Differentiation, Abatacept, Celiac Disease, Italy, Antigens, CD, Humans, CTLA-4 Antigen, Female, Genetic Predisposition to Disease, Child

Abstract

Coeliac disease (CD) is a multifactorial disease for which there is an intensive search for genetic risk factors. Some authors found an association between the CTLA-4 region and CD. In the present work, we investigate the possible implication of the CTLA-4 region as a genetic risk factor for CD, through two statistical approaches: the maximum likelihood score (MLS) test in a large Italian sample of affected sib-pairs using polymorphic genetic markers on chromosome 2, and the transmission disequilibrium test (TDT) in continental Italian and Tunisian families using the CTLA-4 exon 1 49 A/G polymorphism. None of these approaches provides evidence for linkage or association between the CTLA-4 region and CD. This might result from a difference in the CTLA-4 region from population to population, either in its involvement as a risk factor or in the strength of linkage disequilibrium.

Published

1999

19. HLA-DR53 molecules are associated with susceptibility to celiac disease and selectively bind gliadin-derived peptides

Author

Scott Southwood, Jean-François Eliaou, F. Bouguerra, Carmen Gianfrani, Marie-Claude Babron, S. Percopo, Alessandro Sette, Françoise Clerget-Darpoux, Martin F. Kagnoff, F. Clot, Luigi Greco, Riccardo Troncone, Clot, F, Gianfrani, C, Babron, M. C, Bouguerra, F, Southwood, S, Kagnoff, M. F, Troncone, Riccardo, Percopo, S, Eliaou, J. F, Clerget Darpoux, F, Sette, A, and Greco, Luigi

Subjects

Tunisia, Genotype, Immunology, Plasma protein binding, Binding, Competitive, Gliadin, Cohort Studies, Risk Factors, HLA-DQ Antigens, Genetics, Humans, Genetic Predisposition to Disease, IC50, Gene, biology, Risk Factor, HLA-DQ2, HLA-DQ Antigen, nutritional and metabolic diseases, HLA-DR Antigens, Molecular biology, HLA-DR Antigen, Human genetics, Celiac Disease, HLA-DR53, Italy, biology.protein, HLA-DRB4 Chain, Cohort Studie, Dimerization, HLA-DRB4 Chains, Human, Protein Binding

Abstract

Celiac disease (CD) patients usually express a DQ2 heterodimer, whose chains DQalpha1*0501/DQbeta1*0201, are encoded by the genes HLA-DQA1*0501 and DQB1*0201, respectively. Among the DQ2 carriers, the risk of developing disease was shown to correlate with the number of DQbeta1*0201 chains encoded. Studying two separate cohorts of Italian and Tunisian patients, we now show a significant association of celiac disease with expression of either the DQ2 or DR53 heterodimers. The risk is maximal for individuals that carry both DQ2 and DR53 heterodimers. When twenty synthetic peptides overlapping most of A-gliadin sequence were tested for the binding to various purified DR molecules, it was found that DR53 molecules bind selectively and with high affinity (IC50

Published

1999

20. Linkage disequilibrium between intra-locus variants in the aminopeptidase n gene and test of their association with coeliac disease

Author

S. Percopo, Patricia Momigliano-Richiardi, M. Lessi, Giorgio Casari, Roberto Tosi, G. Oderda, Luigi Greco, Mara Giordano, P. Zavattari, Elisabetta Bolognesi, F. Clot, Sandra D'Alfonso, Giordano, M, Bolognesi, E, D'Alfonso, S, Lessi, M, Zavattari, P, Oderda, G, Clot, F, Percopo, S, Casari, GIORGIO NEVIO, Greco, L, Tosi, R, Momigliano Richiardi, P., Zavattari, P., Odera, G., Clot, F., Percopo, S., Casari, G., Greco, Luigi, Tosi, R., and MOMIGLIANO RICCIARDI, P.

Subjects

Proband, Male, Linkage disequilibrium, DNA, Complementary, Genotype, Disequilibrium, DNA Mutational Analysis, Locus (genetics), Biology, CD13 Antigens, Genetic determinism, Linkage Disequilibrium, Gene Frequency, Genetics, medicine, Humans, Point Mutation, Genetics (clinical), Alleles, Polymorphism, Single-Stranded Conformational, Genetic association, Family Health, Polymorphism, Genetic, Genetic Variation, Transmission disequilibrium test, Celiac Disease, Amino Acid Substitution, Haplotypes, GenBank, Female, medicine.symptom

Abstract

Coeliac disease (CD) is a multigenic and multifactorial enteropathy triggered by gluten-composing proteins. A possible involvement of the intestinal Aminopeptidase N (APN) was investigated by an association analysis. SSCP analysis detected four variants at position 281, 378, 956 and 2957 (referred to no. g178535, GenBank) that were studied in 193 Italian CD families. The haplotypic combinations were determined from family segregation and pairwise linkage disequilibria (D' = D/Dmax) between the polymorphic sites were calculated. Significant D' values ranged between 0.78 and 0.31. Association with CD was tested by TDT (Transmission Disequilibrium Test) utilizing as markers the nucleotide substitutions and their haplotypic combinations. No statistically significant transmission distortion to the probands or to their clinically silent sibs was observed. Our data exclude an involvement in CD of the tested markers and of further undetected variation in strong linkage disequilibrium (D' approximately equal to 1) with them. The power of the test was not adequate to detect an association with an unknown polymorphism which is not in complete linkage disequilibrium with those analysed.

Published

1999

21. Genome search in celiac disease

Author

S. Percopo, Alessandro Ventura, Giuseppe Iacono, Fiorella Balli, Salvatore Musumeci, Ettore Cardi, Giuliano Torre, Gino Roberto Corazza, Carlo Catassi, Wilma Mantavoni, Rosanna Gatti, Françoise Clerget-Darpoux, J.L. Serre, Roberto Tosi, Francesco Cataldo, Jean François Eliaou, Stefano De Virgiliis, Umberto Volta, F. Clot, Colette Dib, Francesco Perri, R. Lazzari, Gianluigi De Angelis, Roberto Ferrari, Marie Claude Fulchignoni-Lataud, Luigi Greco, Riccardo Troncone, Patrizia Zavattari, F. Bouguerra, Giuseppe Magazzù, Annamaria Giunta, Marie Claude Babron, Maria Teresa Bardella, Greco, L, Corazza, G, Babron, Mc, Clot, F, Fulchignonilataud, Mc, Percopo, S, Zavattari, P, Bouguerra, F, Dib, C, Tosi, R, Troncone, R, Ventura, Alessandro, Mantavoni, W, Magazzu, G, Gatti, R, Lazzari, R, Giunta, A, Perri, F, Iacono, G, Cardi, E, DE VIRGILIIS, S, Cataldo, F, DE ANGELIS, G, Musumeci, S, Clergetdarpoux, F., Greco, Luigi, Fulchignoni Lataud, Mc, Troncone, Riccardo, Ventura, A, Mantovani, W, Magazzù, G, de Virgiliis, S, De Angelis, G, Ferrari, R, Balli, F, Bardella, Mt, Volta, U, Catassi, C, Torre, G, Eliaou, Jf, Serre, Jl, and Clerget Darpoux, F.

Subjects

Genotype, Genetic Linkage, Human leukocyte antigen, Biology, Coeliac disease, Genetic determinism, Genome screening, Gene mapping, Genetic linkage, Genetics, Genetic predisposition, medicine, Humans, Genetics(clinical), Genetic Testing, Risk factor, Genetics (clinical), Genetic testing, medicine.diagnostic_test, Linkage, Genome, Human, medicine.disease, HLA, Celiac Disease, Research Article

Abstract

SummaryCeliac disease (CD), a malabsorption disorder of the small intestine, results from ingestion of gluten. The HLA risk factors involved in CD are well known but do not explain the entire genetic susceptibility. To determine the localization of other genetic risk factors, a systematic screening of the genome has been undertaken. The typing information of 281 markers on 110 affected sib pairs and their parents was used to test linkage. Systematic linkage analysis was first performed on 39 pairs in which both sibs had a symptomatic form of CD. Replication of the regions of interest was then carried out on 71 pairs in which one sib had a symptomatic form and the other a silent form of CD. In addition to the HLA loci, our study suggests that a risk factor in 5qter is involved in both forms of CD (symptomatic and silent). Furthermore, a factor on 11qter possibly differentiates the two forms. In contrast, none of the regions recently published was confirmed by the present screening.

Published

1998

22. Lack of correlation between genotype and phenotype in celiac disease

Author

F. Clot, Carlo Franzese, S. Percopo, Jean-François Eliaou, Riccardo Troncone, Luigi Greco, Marie-Claude Babron, F. Bouguerra, Françoise Clerget-Darpoux, Greco, Luigi, Percopo, Selvaggia, Clot, Fabienne, Bouguerra, Faouzi, Babron, Marie Claude, Eliaou, Jean Françoi, Franzese, Carlo, Troncone, Riccardo, and Clerget Darpoux, Françoise

Subjects

medicine.medical_specialty, Histology, Genotype, Gene Dosage, Medicine (miscellaneous), Physical examination, Growth, Human leukocyte antigen, Disease, HLA-DQ alpha-Chains, Coeliac disease, Genotype-phenotype distinction, HLA-DQ Antigens, Immunopathology, Internal medicine, medicine, HLA-DQ beta-Chains, Humans, Celiac disease, medicine.diagnostic_test, business.industry, Body Weight, Gastroenterology, HLA-DR Antigens, DQ-specific heterodimer, medicine.disease, Phenotype, Body Height, HLA genotype, Child, Preschool, Immunology, Pediatrics, Perinatology and Child Health, Female, business, Dimerization, Food Science

Abstract

Background Celiac disease has a wide range of clinical features. The goal of this study was to evaluate whether specific HLA genotypes are associated with particular clinical appearances. Methods One hundred forty-five patients with confirmed celiac disease were oligotyped for DR and DQ HLA genes. Clinical notes, physical examination, and a questionnaire provided their personal data. Patients were grouped into nine genotypic categories, according to the presence of the specific DQ heterodimer DQA1*0501-DQB1*0201 (hence termed alpha0beta0), in single or double dose, and the presence of the DRB4 antigen. Results Age at first symptoms and age at beginning of gluten-free diet were not significantly different in the nine groups. The initial symptoms of the disease had a similar distribution in all groups. In twenty-seven patients, disease was diagnosed by family screening: they shared a similar HLA genotype with those who had relevant symptoms. The actual growth status-evaluated by standardized height, percentage of median weight for age, and percentage of median weight for height--was not different in the nine groups. Presence of unusual health complaints was not associated with a specific genotype. Conclusions There is no evidence that clinical features of celiac disease are associated with different HLA genotypes. Genes outside the HLA may play a relevant role.

Published

1998

23. Response

Author

F. Clot, C. Gianfrani, M.-C. Babron, F. Bouguerra, S. Southwood, M. F. Kagnoff, R. Troncone, S. Percopo, A. Sette, L. Greco, J.-F. Eliaou, and F. Clerget-Darpoux

Subjects

Immunology, Genetics

Published

2000

24. 75 HLA-DRB4 IS THE MISSING SPECIFICITY IN COELLAC DISEASE

Author

S. Percopo, Riccardo Troncone, Jean-François Eliaou, Françoise Clerget-Darpoux, M C Barbron, F. Clot, Luigi Greco, and F. Bouguerra

Subjects

business.industry, Pediatrics, Perinatology and Child Health, Immunology, Gastroenterology, Medicine, Disease, business, HLA-DRB4

Published

1996

25. The first large population based twin study of coeliac disease.

Author

L, Greco, R, Romino, I, Coto, N, Di Cosmo, S, Percopo, M, Maglio, F, Paparo, V, Gasperi, G, Limongelli M, R, Cotichini, C, D'Agate, N, Tinto, L, Sacchetti, R, Tosi, and A, Stazi M

Abstract

BACKGROUND AND AIMS: The genetic load in coeliac disease has hitherto been inferred from case series or anecdotally referred twin pairs. We have evaluated the genetic component in coeliac disease by estimating the concordance rate for the disease among twin pairs in a large population based study. METHODS: The Italian Twin Registry was matched with the membership lists of a patient support group. Forty seven twin pairs were recruited and screened for antiendomysial (EMA) and antihuman-tissue transglutaminase (anti-tTG) antibodies; zygosity was verified by DNA fingerprinting and twins were typed for HLA class II DRB1 and DQB1 molecules. RESULTS: Concordance rates for coeliac disease differ significantly between monozygotic (MZ) (0.86 probandwise and 0.75 pairwise) and dizygotic (DZ) (0.20 probandwise and 0.11 pairwise) twins. This is the highest concordance so far reported for a multifactorial disease. A logistic regression model, adjusted for age, sex, number of shared HLA haplotypes, and zygosity, showed that genotypes DQA1*0501/DQB1*0201 and DQA1*0301/DQB1*0302 (encoding for heterodimers DQ2 and DQ8, respectively) conferred to the non-index twin a risk of contracting the disease of 3.3 and 1.4, respectively. The risk of being concordant for coeliac disease estimated for the non-index twin of MZ pairs was 17 (95% confidence interval 2.1-134), independent of the DQ at risk genotype. CONCLUSION: This study provides substantial evidence for a very strong genetic component in coeliac disease, which is only partially due to the HLA region.

Published

2002

26. Promoter polymorphisms of the CD14 gene in Italian patients with coeliac disease

Author

Laura Braida, Antonio Amoroso, Alessandro Ventura, S Percopo, S. Crovella, Michele Boniotto, Boniotto, M, Braida, L, Ventura, Alessandro, Percopo, S, Amoroso, A, and Crovella, Sergio

Subjects

Candidate gene, Genotype, CD14, Lipopolysaccharide Receptors, Human leukocyte antigen, Biology, Autoimmune enteropathy, Major histocompatibility complex, Coeliac disease, Promoter Regions, Gene Frequency, Genetic, Genetic linkage, HLA Antigens, Genetics, medicine, Humans, Polymorphism, Promoter Regions, Genetic, Genetics (clinical), Alleles, Polymorphism, Genetic, Celiac Disease, DNA, Italy, Polymorphism, Restriction Fragment Length, Haplotype, medicine.disease, Restriction Fragment Length, Immunology, biology.protein, Online Mutation Report

Abstract

Coeliac disease (CD) is an autoimmune enteropathy triggered by ingestion of wheat gluten or related protein from rye and barley, and is one of the most frequently occurring, treatable, lifelong disorders.1,2 Undetected or untreated CD may cause other, more severe, complications later, such as autoimmune diseases, osteoporosis, neurological disorders, and infertility.3,4 Several studies have shown CD clusters in families with a sibling relative risk of 20–60 and high concordance between monozygotic twins (75%),5–8 which indicates a strong genetic component to coeliac disease. As expected in complex autoimmune diseases, human leukocyte antigen (HLA) linked genes are the main genetic factor involved in CD. More than 90% of patients suffering from CD share the major histocompatibility complex II class HLA-DQ2 haplotype. Most of the remainder present HLA-DQ8. However, there are patients who present neither HLA-DQ8 nor HLA-DQ2 on their antigen-presenting cells. These genetic findings strongly indicate the involvement of other genes in the pathogenesis of coeliac disease. So far, various genome-wide linkage analyses have been performed in order to identify non-HLA linked genes responsible for CD. A recent study by Greco et al. 9 on Italian coeliac families demonstrated the existence of a genetic risk factor on chromosome 5 (5q31–33), which has been reported in other linkage studies in different populations.10,11 This genomic region contains several candidate genes for CD, including the interleukin ( IL12B ) gene, the polymorphisms of which do not seem to be associated with CD,12 and the gene encoding for CD14.13 CD14 is a multifunctional receptor involved in the innate immune response. In fact, it is thought to be one of the most important receptors for lipopolysaccharide and other bacterial wall-derived components.14–16 However it is well known that CD14 has several other functions,17,18 including the clearance …

27. Concordance, disease progression, and heritability of coeliac disease in Italian twins.

Author

Nisticò L, Fagnani C, Coto I, Percopo S, Cotichini R, Limongelli MG, Paparo F, D'Alfonso S, Giordano M, Sferlazzas C, Magazzù G, Momigliano-Richiardi P, Greco L, and Stazi MA

Subjects

Adolescent, Adult, Celiac Disease etiology, DNA Fingerprinting, Disease Progression, Diseases in Twins etiology, Environment, Female, Genetic Predisposition to Disease, HLA-DQ Antigens analysis, HLA-DR Antigens analysis, Histocompatibility Testing, Humans, Italy, Male, Registries, Survival Analysis, Twins, Dizygotic, Twins, Monozygotic, Celiac Disease genetics, Diseases in Twins genetics

Abstract

Background and Aims: We adopted the twin method to disentangle the genetic and environmental components of susceptibility to coeliac disease (CD). We estimated disease concordance rate by zygosity and HLA genotypes, discordance times, progression rates to disease, and heritability., Methods: We crosslinked the Italian Twin Registry with the membership lists of the Italian Coeliac Disease Association and recruited 23 monozygotic (MZ) and 50 dizygotic (DZ) twin pairs with at least one affected member. Zygosity was assigned by DNA fingerprinting, and HLA-DQ and DR alleles were genotyped. Disease status was ascertained by antiendomysial, anti-human tissue transglutaminase antibodies, and bowel biopsy., Results: Concordance was significantly higher in MZ (83.3% probandwise, 71.4% pairwise) than in DZ (16.7% probandwise, 9.1% pairwise) pairs. Concordance was not affected by sex or HLA genotype of the co-twin and being MZ was significantly associated with the occurrence of CD (Cox adjusted hazard ratio 14.3 (95% confidence interval 4.0-50.3)). In 90% of concordant pairs the discordance time was

Published

2006

28. Evidence of a correlation between mannose binding lectin and celiac disease: a model for other autoimmune diseases.

Author

Boniotto M, Braida L, Baldas V, Not T, Ventura A, Vatta S, Radillo O, Tedesco F, Percopo S, Montico M, Amoroso A, and Crovella S

Subjects

Adolescent, Adult, Apoptosis genetics, Autoimmune Diseases genetics, Biopsy, Case-Control Studies, Celiac Disease pathology, Child, Child, Preschool, Female, Gene Frequency, Genetic Predisposition to Disease, HLA-DQ Antigens genetics, Haplotypes genetics, Humans, Infant, Intestines pathology, Intestines physiology, Italy, Male, Mannose-Binding Lectin metabolism, Middle Aged, Celiac Disease genetics, Mannose-Binding Lectin genetics, Polymorphism, Genetic

Abstract

Celiac disease is a multifactorial disorder caused, in genetically susceptible patients, by the ingestion of dietary gluten. Very little is known about the genetic factors, but there is a strong association of two HLA haplotypes (DQ2 or alpha1*05, beta1*02 and DQ8 or alpha1*0301, beta1*0302) with the disease. We investigated the relationship between polymorphisms in the first exon of the MBL2 gene, which encodes for mannose binding lectin (MBL) and celiac disease. Moreover we studied the MBL role by immunohistochemistry and TUNEL. Results were confirmed by clinical findings. We enrolled 149 Italian celiac patients; 116 were characterized by the presence of DQ2 or DQ8. The HLA haplotype was established by allelic specific PCR while the MBL2 genotype was resolved by melting temperature assay. Immunohistochemistry and TUNEL assays were performed on serial sections of biopsy specimens from celiac patients and healthy controls. MBL2 allele and genotype frequencies varied significantly between celiac patients and healthy controls. The frequencies of the 0 allele were 28% in DQ2 or DQ8 celiac patients, 36% in HLA atypical celiac patients, and 22% in healthy controls. Interestingly, the MBL2 0/0 genotype was present in 7 of 33 HLA atypical celiac patients (21%) and in 13 of 116 HLA typical celiac patients (13%) but in only 7 of 147 healthy controls (5%). Furthermore, we found that MBL2 genotype is strongly associated with the occurrence of secondary autoimmune diseases. Immunohistochemistry and TUNEL findings support a role of MBL2 in the clearance of apoptotic cells. In conclusion, MBL2 variants, responsible for lower MBL levels, are associated with celiac disease and higher risk of developing autoimmune diseases. Here we propose a role for MBL in the disease which could be easily applied to other autoimmune disorders.

Published

2005

29. Variable phenotype associated with SP-C gene mutations: fatal case with the I73T mutation.

Author

Percopo S, Cameron HS, Nogee LM, Pettinato G, Montella S, and Santamaria F

Subjects

Base Sequence, Biopsy, Needle, Blotting, Western, Fatal Outcome, Genetic Testing, Humans, Immunohistochemistry, Infant, Infant, Newborn, Male, Molecular Sequence Data, Polymerase Chain Reaction, Prognosis, Sensitivity and Specificity, Genetic Predisposition to Disease, Lung Diseases, Interstitial genetics, Lung Diseases, Interstitial pathology, Mutation, Missense, Protein C genetics

Published

2004

30. In vitro-deranged intestinal immune response to gliadin in type 1 diabetes.

Author

Auricchio R, Paparo F, Maglio M, Franzese A, Lombardi F, Valerio G, Nardone G, Percopo S, Greco L, and Troncone R

Subjects

Adolescent, Antibody Formation, Biopsy, Case-Control Studies, Child, Female, HLA Antigens analysis, HLA Antigens classification, Humans, Immunohistochemistry, Jejunum immunology, Jejunum pathology, Male, Organ Culture Techniques, Diabetes Mellitus, Type 1 immunology, Gliadin immunology, Intestinal Mucosa immunology

Abstract

Dietary gluten has been associated with an increased risk of type 1 diabetes. We have evaluated inflammation and the mucosal immune response to gliadin in the jejunum of patients with type 1 diabetes. Small intestinal biopsies from 17 children with type 1 diabetes without serological markers of celiac disease and from 50 age-matched control subjects were examined by immunohistochemistry. In addition, biopsies from 12 type 1 diabetic patients and 8 control subjects were cultured with gliadin or ovalbumin peptic-tryptic digest and examined for epithelial infiltration and lamina propria T-cell activation. The density of intraepithelial CD3(+) and gammadelta(+) cells and of lamina propria CD25(+) mononuclear cells was higher in jejunal biopsies from type 1 diabetic patients versus control subjects. In the patients' biopsies cultured with peptic-tryptic gliadin, there was epithelial infiltration by CD3(+) cells, a significant increase in lamina propria CD25(+) and CD80(+) cells and enhanced expression of lamina propria CD54 and crypt HLA-DR. No such phenomena were observed in control subjects, even those with celiac disease-associated HLA haplotypes. In conclusion, signs of mucosal inflammation were present in jejunal biopsies from type 1 diabetic patients, and organ culture studies indicate a deranged mucosal immune response to gliadin.

Published

2004

31. HLA-DQ relative risks for coeliac disease in European populations: a study of the European Genetics Cluster on Coeliac Disease.

Author

Margaritte-Jeannin P, Babron MC, Bourgey M, Louka AS, Clot F, Percopo S, Coto I, Hugot JP, Ascher H, Sollid LM, Greco L, and Clerget-Darpoux F

Subjects

Celiac Disease metabolism, Europe epidemiology, Gene Frequency, Genotype, HLA-DQ Antigens metabolism, Haplotypes, Risk, Celiac Disease genetics, Genetic Predisposition to Disease, HLA-DQ Antigens genetics

Abstract

Coeliac disease is an enteropathy due to an intolerance to gluten. The association between HLA-DQ genes and CD is well established. The majority of patients carry the HLA-DQ heterodimer encoded by DQA1*05/DQB1*02, either in cis or in trans. The remaining patients carry either part of the DQ heterodimer or DQA1*03-DQB1*0302. The aim of the study was to estimate the risks associated with different DQ genotypes in European populations. HLA information was available for 470 trio families from four countries: France (117), Italy (128), and Norway and Sweden (225). Five DQA1-DQB1 haplotypes were considered and control haplotype frequencies were estimated from the set of parental haplotypes not transmitted to the affected child. The possible genotypes were grouped into five genotype groups, based on the hierarchy of risk reported in the literature. A north-south gradient in the genotype group frequencies is observed in probands: homogeneity is strongly rejected between all country pairs. For each country, the relative risks associated with each genotype group were computed taking into account the control haplotype frequencies. Homogeneity of relative risks between countries was tested pairwise by maximum likelihood ratio statistics. The hypothesis of homogeneity of relative risks is rejected (P is approximately 10(-6)) for all country pairs. In conclusion, the gradient in the genotype group frequencies in probands is not only due to differences in haplotype frequencies but also due to differences in genotype relative risks in the studied populations; the relative risks associated with each DQ genotype group are different between northern and southern European countries; neither are they ordered in the same way., (Copyright 2004 Blackwell Munksgaard)

Published

2004

32. Candidate gene region 2q33 in European families with coeliac disease.

Author

Holopainen P, Naluai AT, Moodie S, Percopo S, Coto I, Clot F, Ascher H, Sollid L, Ciclitira P, Greco L, Clerget-Darpoux F, and Partanen J

Subjects

Alleles, Antigens, CD, Apoptosis Regulatory Proteins, CTLA-4 Antigen, Chromosome Mapping, Europe, Female, Gene Frequency, Genetic Linkage, Genetic Markers, Genetic Predisposition to Disease, Haplotypes genetics, Humans, Inducible T-Cell Co-Stimulator Protein, Male, Polymorphism, Genetic, Programmed Cell Death 1 Receptor, White People genetics, Antigens, Differentiation genetics, Antigens, Differentiation, T-Lymphocyte genetics, Antigens, Surface genetics, CD28 Antigens genetics, Celiac Disease genetics, Chromosomes, Human, Pair 2 genetics

Abstract

Chromosome region 2q33 harbours a cluster of genes, CTLA-4, CD28, ICOS and closely located PD-1, all related to immune activation and considered as promising candidate genes for susceptibility to coeliac disease (CD). We present here the results of a genetic linkage and association analysis of nine markers located in this gene region in a large combined European material of 796 families with CD from Finland, Sweden, Norway, UK, France and Italy. The joint analysis supports earlier findings that this susceptibility locus, assigned as CELIAC3, merits further studies. Nominally significant linkage to CD was found in 314 families including affected sib pairs. Each of the five populations showed weak associations to several marker alleles, but the analysis revealed, however, no conclusive evidence for a primary functional gene or gene variant present in the total set of families. The results suggest that the CD risk due to 2q33 gene region is complex and may involve more than one susceptibility allele, which possibly differ from other autoimmune diseases.

Published

2004

33. Promoter polymorphisms of the CD14 gene in Italian patients with coeliac disease.

Author

Boniotto M, Braida L, Ventura A, Percopo S, Amoroso A, and Crovella S

Subjects

Alleles, DNA genetics, Gene Frequency, Genotype, HLA Antigens genetics, Humans, Italy, Polymorphism, Genetic, Polymorphism, Restriction Fragment Length, Celiac Disease genetics, Lipopolysaccharide Receptors genetics, Promoter Regions, Genetic genetics

Published

2003

34. Saturation of the 5q31-q33 candidate region for coeliac disease.

Author

Percopo S, Babron MC, Whalen M, De Virgiliis S, Coto I, Clerget-Darpoux F, Landolfo F, and Greco L

Subjects

Genetic Markers, Genetic Predisposition to Disease, Humans, Celiac Disease genetics, Chromosomes, Human, Pair 5

Abstract

The first genome wide screening performed on Italian affected sib-pair families (Greco et al. 1998) gave evidence for linkage with coeliac disease in the 5q region. This finding was replicated in a second independent dataset (Greco et al. 2001). Overall, pooling both samples, the highest MLS value (2.92) was found for the most centromeric marker tested, D5S640. In the present study, the 5q31-q33 region was saturated with 12 new markers around D5S640, in order to verify whether there would be a shift of the MLS position. This study allowed us to support our previous finding of linkage for the region 5q31-q33, with the most significant MLS value at D5S2014, very close to the marker D5S640. No evidence for interaction between this risk factor and the one in the HLA region was found. Furthermore, many different groups have independently obtained analogous results for this region, confirming the presence of a susceptibility locus in the region 5q31-q33. This region contains several interesting candidate genes for coeliac disease.

Published

2003

35. Additional factor in some HLA DR3/DQ2 haplotypes confers a fourfold increased genetic risk of celiac disease.

Author

Bolognesi E, Karell K, Percopo S, Coto I, Greco L, Mantovani V, Suoraniemi E, Partanen J, Mustalahti K, Mäki M, and Momigliano-Richiardi P

Subjects

Finland, Genetic Markers, Genetic Predisposition to Disease, Humans, Italy, Celiac Disease genetics, HLA-DQ Antigens genetics, HLA-DR3 Antigen genetics, Haplotypes

Abstract

Although HLA-DQ genes are the major celiac disease (CD) susceptibility genes, results from Finnish families suggest that not all DQ2-encoding haplotypes confer equal susceptibility to CD, implying the effect of other gene(s) in the HLA region. The aim of the present work was to extend and confirm the aforementioned results in a southern European population ( Italian) and to better localize the additional risk factor/s. The association of nine loci spanning the HLA region from DR to HFE, 4.5-Mb telomeric of HLA-A, was tested. The analysis was performed by comparing marker frequencies in DR3-DQ2 haplotypes transmitted and non-transmitted to the affected offspring in 156 Italian CD families selected for having at least one DR3-positive parent. The same analysis was performed independently in 101 Finnish CD families selected with the same criteria. Three alleles, MICA-A5.1, MICB-CA24 and MIB-350, all characteristic of the B8-DR3 extended haplotype, showed a significantly increased frequency in DR3 transmitted haplotypes in the Italian families. DR3 haplotypes carrying the combination of these alleles conferred an approximate fourfold increased CD risk. B8-DR3 transmitted haplotypes were significantly more conserved telomerically down to the MIC-Class I region. Similar results were seen in the Finnish families. The major conclusion that holds true in both populations is that, while DQ2 is an absolute requirement for the development of CD, the presence of an additional genetic factor within the MIC-Class I region confers an approximate 4-fold increased risk of the disease.

Published

2003

36. The first large population based twin study of coeliac disease.

Author

Greco L, Romino R, Coto I, Di Cosmo N, Percopo S, Maglio M, Paparo F, Gasperi V, Limongelli MG, Cotichini R, D'Agate C, Tinto N, Sacchetti L, Tosi R, and Stazi MA

Subjects

Adolescent, Adult, DNA Fingerprinting, Female, HLA-DQ Antigens analysis, HLA-DQ alpha-Chains, HLA-DQ beta-Chains, HLA-DR Antigens analysis, HLA-DRB1 Chains, Histocompatibility Testing, Humans, Logistic Models, Male, Odds Ratio, Celiac Disease genetics, Diseases in Twins genetics, Genetic Predisposition to Disease

Abstract

Background and Aims: The genetic load in coeliac disease has hitherto been inferred from case series or anecdotally referred twin pairs. We have evaluated the genetic component in coeliac disease by estimating the concordance rate for the disease among twin pairs in a large population based study., Methods: The Italian Twin Registry was matched with the membership lists of a patient support group. Forty seven twin pairs were recruited and screened for antiendomysial (EMA) and antihuman-tissue transglutaminase (anti-tTG) antibodies; zygosity was verified by DNA fingerprinting and twins were typed for HLA class II DRB1 and DQB1 molecules., Results: Concordance rates for coeliac disease differ significantly between monozygotic (MZ) (0.86 probandwise and 0.75 pairwise) and dizygotic (DZ) (0.20 probandwise and 0.11 pairwise) twins. This is the highest concordance so far reported for a multifactorial disease. A logistic regression model, adjusted for age, sex, number of shared HLA haplotypes, and zygosity, showed that genotypes DQA1*0501/DQB1*0201 and DQA1*0301/DQB1*0302 (encoding for heterodimers DQ2 and DQ8, respectively) conferred to the non-index twin a risk of contracting the disease of 3.3 and 1.4, respectively. The risk of being concordant for coeliac disease estimated for the non-index twin of MZ pairs was 17 (95% confidence interval 2.1-134), independent of the DQ at risk genotype., Conclusion: This study provides substantial evidence for a very strong genetic component in coeliac disease, which is only partially due to the HLA region.

Published

2002

37. The IL12B gene does not confer susceptibility to coeliac disease.

Author

Louka AS, Torinsson Naluai A, D'Alfonso S, Ascher H, Coto I, Ek J, Giordano M, Gudjónsdóttir AH, Mellai M, Momigliano-Richiardi P, Percopo S, Samuelsson L, Wahlström J, Greco L, and Sollid LM

Subjects

Alleles, Celiac Disease pathology, HLA-DQ Antigens genetics, HLA-DQ alpha-Chains, HLA-DQ beta-Chains, Humans, Interleukin-12 Subunit p40, Intestines pathology, Italy, Polymorphism, Genetic, Scandinavian and Nordic Countries, Celiac Disease genetics, Genetic Predisposition to Disease, Interleukin-12 genetics

Abstract

Coeliac disease (CD) is a chronic inflammatory disorder where dietary gluten is not tolerated. In the lesion there are gluten reactive T cells predominantly secreting gamma-interferon. Both HLA and non-HLA genes contribute to CD susceptibility. Interleukin-12 (IL-12) regulates gamma-interferon production. The IL12B gene is located in a region (5q31.1-33.1) where there is evidence for linkage with CD. Allele 1 of an IL12B 3'UTR single-nucleotide polymorphism leads to increased expression of IL-12, and was recently implicated in susceptibility for type 1 diabetes (T1D). We found no evidence for association of allele 1 to CD by the transmission/disequilibrium test or case-control approach. No increased frequency was observed in patients belonging to families where the disease was linked to markers on chromosome 5q. Unlike T1D, allele 1 does not appear to confer susceptibility to CD.

Published

2002

38. Existence of a genetic risk factor on chromosome 5q in Italian coeliac disease families.

Author

Greco L, Babron MC, Corazza GR, Percopo S, Sica R, Clot F, Fulchignoni-Lataud MC, Zavattari P, Momigliano-Richiardi P, Casari G, Gasparini P, Tosi R, Mantovani V, De Virgiliis S, Iacono G, D'Alfonso A, Selinger-Leneman H, Lemainque A, Serre JL, and Clerget-Darpoux F

Subjects

Celiac Disease ethnology, Chromosomes, Family Health, Female, Genetic Markers, Humans, Italy, Lod Score, Male, Risk Factors, Celiac Disease genetics, Chromosomes, Human, Pair 5

Abstract

Coeliac disease (CD) is a malabsorptive disorder of the small intestine resulting from ingestion of gluten. The HLA risk factors involved in CD are well known but do not explain the whole genetic susceptibility. Several regions of potential linkage on chromosomes 3q, 5q, 10q, 11q, 15q and 19q have already been reported in the literature. These six regions were analyzed with the Maximum Lod Score method on a dense set of markers. A new sample of 89 Italian sibpairs was available for study. There was no evidence for linkage for any of the regions tested, except for chromosome 5q. For this region, our data, as well as a sample of 93 sibpairs from our first genome screen (Greco et al. 1998), are compatible with the presence of a risk factor for CD with a moderate effect.

Published

2001

39. Study of two ectopeptidases in the susceptibility to celiac disease: two newly identified polymorphisms of dipeptidylpeptidase IV.

Author

Clot F, Babron MC, Percopo S, Giordano M, Bouguerra F, Clerget-Darpoux F, Greco L, Serre JL, and Fulchignoni-Lataud MC

Subjects

Adult, Child, Female, Humans, Italy, Linkage Disequilibrium, Male, Polymorphism, Genetic, Tunisia, CD13 Antigens genetics, Celiac Disease enzymology, Celiac Disease genetics, Dipeptidyl Peptidase 4 genetics, Genetic Predisposition to Disease

Published

2000

40. Linkage and association study of the CTLA-4 region in coeliac disease for Italian and Tunisian populations.

Author

Clot F, Fulchignoni-Lataud MC, Renoux C, Percopo S, Bouguerra F, Babron MC, Djilali-Saiah I, Caillat-Zucman S, Clerget-Darpoux F, Greco L, and Serre JL

Subjects

Abatacept, Adult, Antigens, CD, CTLA-4 Antigen, Child, Family Health, Female, Genetic Markers, Genetic Predisposition to Disease, Humans, Italy, Male, Tunisia, Antigens, Differentiation genetics, Celiac Disease genetics, Genetic Linkage, Immunoconjugates, Polymorphism, Genetic

Abstract

Coeliac disease (CD) is a multifactorial disease for which there is an intensive search for genetic risk factors. Some authors found an association between the CTLA-4 region and CD. In the present work, we investigate the possible implication of the CTLA-4 region as a genetic risk factor for CD, through two statistical approaches: the maximum likelihood score (MLS) test in a large Italian sample of affected sib-pairs using polymorphic genetic markers on chromosome 2, and the transmission disequilibrium test (TDT) in continental Italian and Tunisian families using the CTLA-4 exon 1 49 A/G polymorphism. None of these approaches provides evidence for linkage or association between the CTLA-4 region and CD. This might result from a difference in the CTLA-4 region from population to population, either in its involvement as a risk factor or in the strength of linkage disequilibrium.

Published

1999

41. HLA-DR53 molecules are associated with susceptibility to celiac disease and selectively bind gliadin-derived peptides.

Author

Clot F, Gianfrani C, Babron MC, Bouguerra F, Southwood S, Kagnoff MF, Troncone R, Percopo S, Eliaou JF, Clerget-Darpoux F, Sette A, and Greco L

Subjects

Binding, Competitive, Cohort Studies, Dimerization, Genetic Predisposition to Disease, Genotype, HLA-DQ Antigens genetics, HLA-DR Antigens chemistry, HLA-DR Antigens isolation & purification, HLA-DRB4 Chains, Humans, Italy, Protein Binding, Risk Factors, Tunisia, Celiac Disease genetics, Gliadin metabolism, HLA-DR Antigens genetics

Abstract

Celiac disease (CD) patients usually express a DQ2 heterodimer, whose chains DQalpha1*0501/DQbeta1*0201, are encoded by the genes HLA-DQA1*0501 and DQB1*0201, respectively. Among the DQ2 carriers, the risk of developing disease was shown to correlate with the number of DQbeta1*0201 chains encoded. Studying two separate cohorts of Italian and Tunisian patients, we now show a significant association of celiac disease with expression of either the DQ2 or DR53 heterodimers. The risk is maximal for individuals that carry both DQ2 and DR53 heterodimers. When twenty synthetic peptides overlapping most of A-gliadin sequence were tested for the binding to various purified DR molecules, it was found that DR53 molecules bind selectively and with high affinity (IC50<1 microM) to A-gliadin-derived peptides. These data suggest that both HLA DQ2 and DR53 molecules are associated with increased genetic risk for CD, and provide a possible biochemical basis for this complex association.

Published

1999

42. Linkage disequilibrium between intra-locus variants in the aminopeptidase n gene and test of their association with coeliac disease.

Author

Giordano M, Bolognesi E, D'Alfonso S, Lessi M, Zavattari P, Oderda G, Clot F, Percopo S, Casari G, Greco L, Tosi R, and Momigliano-Richiardi P

Subjects

Alleles, Amino Acid Substitution, Celiac Disease enzymology, DNA Mutational Analysis, DNA, Complementary chemistry, DNA, Complementary genetics, Family Health, Female, Gene Frequency, Genetic Variation, Genotype, Haplotypes, Humans, Male, Point Mutation, Polymorphism, Genetic, Polymorphism, Single-Stranded Conformational, CD13 Antigens genetics, Celiac Disease genetics, Linkage Disequilibrium

Abstract

Coeliac disease (CD) is a multigenic and multifactorial enteropathy triggered by gluten-composing proteins. A possible involvement of the intestinal Aminopeptidase N (APN) was investigated by an association analysis. SSCP analysis detected four variants at position 281, 378, 956 and 2957 (referred to no. g178535, GenBank) that were studied in 193 Italian CD families. The haplotypic combinations were determined from family segregation and pairwise linkage disequilibria (D' = D/Dmax) between the polymorphic sites were calculated. Significant D' values ranged between 0.78 and 0.31. Association with CD was tested by TDT (Transmission Disequilibrium Test) utilizing as markers the nucleotide substitutions and their haplotypic combinations. No statistically significant transmission distortion to the probands or to their clinically silent sibs was observed. Our data exclude an involvement in CD of the tested markers and of further undetected variation in strong linkage disequilibrium (D' approximately equal to 1) with them. The power of the test was not adequate to detect an association with an unknown polymorphism which is not in complete linkage disequilibrium with those analysed.

Published

1999

43. Genome search in celiac disease.

Author

Greco L, Corazza G, Babron MC, Clot F, Fulchignoni-Lataud MC, Percopo S, Zavattari P, Bouguerra F, Dib C, Tosi R, Troncone R, Ventura A, Mantavoni W, Magazzù G, Gatti R, Lazzari R, Giunta A, Perri F, Iacono G, Cardi E, de Virgiliis S, Cataldo F, De Angelis G, Musumeci S, and Clerget-Darpoux F

Subjects

Genetic Linkage, Genetic Testing, Genotype, Humans, Celiac Disease genetics, Genome, Human

Abstract

Celiac disease (CD), a malabsorption disorder of the small intestine, results from ingestion of gluten. The HLA risk factors involved in CD are well known but do not explain the entire genetic susceptibility. To determine the localization of other genetic risk factors, a systematic screening of the genome has been undertaken. The typing information of 281 markers on 110 affected sib pairs and their parents was used to test linkage. Systematic linkage analysis was first performed on 39 pairs in which both sibs had a symptomatic form of CD. Replication of the regions of interest was then carried out on 71 pairs in which one sib had a symptomatic form and the other a silent form of CD. In addition to the HLA loci, our study suggests that a risk factor in 5qter is involved in both forms of CD (symptomatic and silent). Furthermore, a factor on 11qter possibly differentiates the two forms. In contrast, none of the regions recently published was confirmed by the present screening.

Published

1998

44. Lack of correlation between genotype and phenotype in celiac disease.

Author

Greco L, Percopo S, Clot F, Bouguerra F, Babron MC, Eliaou JF, Franzese C, Troncone R, and Clerget-Darpoux F

Subjects

Body Height, Body Weight, Celiac Disease physiopathology, Child, Preschool, Dimerization, Female, Gene Dosage, Growth, HLA-DQ alpha-Chains, HLA-DQ beta-Chains, Humans, Celiac Disease diagnosis, Celiac Disease genetics, Genotype, HLA-DQ Antigens genetics, HLA-DR Antigens genetics, Phenotype

Abstract

Background: Celiac disease has a wide range of clinical features. The goal of this study was to evaluate whether specific HLA genotypes are associated with particular clinical appearances., Methods: One hundred forty-five patients with confirmed celiac disease were oligotyped for DR and DQ HLA genes. Clinical notes, physical examination, and a questionnaire provided their personal data. Patients were grouped into nine genotypic categories, according to the presence of the specific DQ heterodimer DQA1*0501-DQB1*0201 (hence termed alpha0beta0), in single or double dose, and the presence of the DRB4 antigen., Results: Age at first symptoms and age at beginning of gluten-free diet were not significantly different in the nine groups. The initial symptoms of the disease had a similar distribution in all groups. In twenty-seven patients, disease was diagnosed by family screening: they shared a similar HLA genotype with those who had relevant symptoms. The actual growth status-evaluated by standardized height, percentage of median weight for age, and percentage of median weight for height--was not different in the nine groups. Presence of unusual health complaints was not associated with a specific genotype., Conclusions: There is no evidence that clinical features of celiac disease are associated with different HLA genotypes. Genes outside the HLA may play a relevant role.

Published

1998

45. The coeliac disease task force " Free from Gluten," " Improved knowledge to cure coeliac disease".

Author

Greco L and Percopo S

Subjects

Adult, Celiac Disease diet therapy, Celiac Disease economics, Celiac Disease epidemiology, Child, Cohort Effect, Cost of Illness, Disease Susceptibility, Food Hypersensitivity epidemiology, Food Hypersensitivity prevention & control, Fund Raising, Glutens administration & dosage, Humans, Incidence, Italy epidemiology, Mass Screening economics, Organizations economics, Patient Advocacy trends, Population Dynamics, Prevalence, Selection, Genetic, Celiac Disease prevention & control, Glutens adverse effects

Abstract

Gluten has recently been introduced into the diet of the Mediterranean and European population, but a considerable proportion has not adapted to this change and has developed intolerance to gluten. At least one million EEC citizens are gluten intolerant. In Italy each year 12 million ECU is spent in the diagnosis of uncomplicated gluten intolerance, 10 million ECU for complex diagnosis and 32 million ECU for long-term complications and malignancies. The total financial load of gluten intolerance, in its present state, is about 150 million ECU/year in Italy. Four million ECU is actually needed to develop a genetic probe, which may make the population screening feasible. A National Task Force "Free from Gluten" has been set up by the Italian Coeliac Society to stimulate fund-raising activities supporting genetic and basic research on gluten intolerance.

Published

1996