A study of Italian pediatric celiac disease patients confirms that the primary HLA association is to the DQ(α1 ∗0501, β1 ∗0201) heterodimer

Celiac disease (CD) has been recently reported to be primarily associated with the DQ(α1 ∗0501, β1 ∗0201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5, 7 heterozygous individuals. The high incidence of DR5, 7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy,...

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Published in	Human immunology Vol. 33; no. 2; pp. 133 - 139
Main Authors	Mazzilli, Maria Cristina, Ferrante, Paola, Mariani, Paolo, Martone, Emma, Petronzelli, Fiorella, Triglione, Paola, Bonamico, Margherita
Format	Journal Article
Language	English
Published	New York, NY Elsevier Inc 01.02.1992 Elsevier Science
Subjects	Base Sequence Biological and medical sciences celiac disease Celiac Disease - genetics Celiac Disease - immunology Child Child, Preschool DNA Probes, HLA - genetics Gastroenterology. Liver. Pancreas. Abdomen HLA-DQ Antigens - genetics HLA-DQ Antigens - immunology HLA-DR Antigens - genetics HLA-DR Antigens - immunology Humans Italy Medical sciences Molecular Sequence Data Oligodeoxyribonucleotides - genetics Other diseases. Semiology Polymerase Chain Reaction Risk Stomach. Duodenum. Small intestine. Colon. Rectum. Anus Italy Europe RR CD HTC ESPGAN LD PCR SSO Human HLA-DQ-Locus HLA-System Immunogenetics Allele Gene Major histocompatibility system Class II histocompatibility antigen Inheritance Risk factor Digestive diseases Coeliac disease
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ISSN	0198-8859 1879-1166
DOI	10.1016/0198-8859(92)90064-T

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Abstract	Celiac disease (CD) has been recently reported to be primarily associated with the DQ(α1 ∗0501, β1 ∗0201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5, 7 heterozygous individuals. The high incidence of DR5, 7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes detecting DQA1 ∗0101 + 0102 + 0103, DQA1 ∗0201, DQA1 ∗0301 + 0302, DQA1 ∗0401 + 0501 and DQA1 ∗0501 and a DQB1-sequence-specific oligonucleotide probe recognizing DQB1 ∗0201 allele. As expected by the DR-DQ disequilibria, DQA1 ∗0201 [62% in patients versus 26% in controls, relative risk (RR) = 5] and DQA1 ∗0501 (96% versus 56%, RR = 19) show positive association with the disease. Of CD patients, 92% (50% DR3 and 42% DR5,7) compared to 18% of the controls carry both DQA1 ∗0501 and DQB1 ∗0201 alleles, so that the combination confers an RR of 52, higher than both the risks of the single alleles ( DQA1 ∗0501 RR = 19, DQB1 ∗ 0201 RR = 30 ), confirming the primary role of the dimer in determining genetic predisposition to CD both in DR3 and in DR5, 7 subjects.
AbstractList	Celiac disease (CD) has been recently reported to be primarily associated with the DQ( alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5,7 heterozygous individuals. The high incidence of DR5,7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes. Celiac disease (CD) has been recently reported to be primarily associated with the DQ(alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5,7 heterozygous individuals. The high incidence of DR5,7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes detecting DQA10101 + 0102 + 0103, DQA10201, DQA10301 + 0302, DQA10401 + 0501 + 0601, and DQA10501 and a DQB1-sequence-specific oligonucleotide probe recognizing DQB10201 allele. As expected by the DR-DQ disequilibria, DQA10201 [62% in patients versus 26% in controls, relative risk (RR) = 5] and DQA10501 (96% versus 56%, RR = 19) show positive association with the disease. Of CD patients, 92% (50% DR3 and 42% DR5,7) compared to 18% of the controls carry both DQA10501 and DQB10201 alleles, so that the combination confers an RR of 52, higher than both the risks of the single alleles (DQA10501 RR = 19, DQB10201 RR = 30), confirming the primary role of the dimer in determining genetic predisposition to CD both in DR3 and in DR5,7 subjects.Celiac disease (CD) has been recently reported to be primarily associated with the DQ(alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5,7 heterozygous individuals. The high incidence of DR5,7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes detecting DQA10101 + 0102 + 0103, DQA10201, DQA10301 + 0302, DQA10401 + 0501 + 0601, and DQA10501 and a DQB1-sequence-specific oligonucleotide probe recognizing DQB10201 allele. As expected by the DR-DQ disequilibria, DQA10201 [62% in patients versus 26% in controls, relative risk (RR) = 5] and DQA10501 (96% versus 56%, RR = 19) show positive association with the disease. Of CD patients, 92% (50% DR3 and 42% DR5,7) compared to 18% of the controls carry both DQA10501 and DQB10201 alleles, so that the combination confers an RR of 52, higher than both the risks of the single alleles (DQA10501 RR = 19, DQB10201 RR = 30), confirming the primary role of the dimer in determining genetic predisposition to CD both in DR3 and in DR5,7 subjects. Celiac disease (CD) has been recently reported to be primarily associated with the DQ(alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5,7 heterozygous individuals. The high incidence of DR5,7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes detecting DQA10101 + 0102 + 0103, DQA10201, DQA10301 + 0302, DQA10401 + 0501 + 0601, and DQA10501 and a DQB1-sequence-specific oligonucleotide probe recognizing DQB10201 allele. As expected by the DR-DQ disequilibria, DQA10201 [62% in patients versus 26% in controls, relative risk (RR) = 5] and DQA10501 (96% versus 56%, RR = 19) show positive association with the disease. Of CD patients, 92% (50% DR3 and 42% DR5,7) compared to 18% of the controls carry both DQA10501 and DQB10201 alleles, so that the combination confers an RR of 52, higher than both the risks of the single alleles (DQA10501 RR = 19, DQB10201 RR = 30), confirming the primary role of the dimer in determining genetic predisposition to CD both in DR3 and in DR5,7 subjects. Celiac disease (CD) has been recently reported to be primarily associated with the DQ(α1 ∗0501, β1 ∗0201) heterodimer encoded in cis on DR3 haplotype and in trans in DR5, 7 heterozygous individuals. The high incidence of DR5, 7 heterozygotes, reflecting the high frequency of the DR5 allele in Italy, makes the analysis of the Italian CD patients critical. Polymerase chain reaction-amplified DNA from 50 CD patients and 50 controls, serologically typed for DR and DQw antigens, was hybridized with five DQA1-specific oligonucleotide probes detecting DQA1 ∗0101 + 0102 + 0103, DQA1 ∗0201, DQA1 ∗0301 + 0302, DQA1 ∗0401 + 0501 and DQA1 ∗0501 and a DQB1-sequence-specific oligonucleotide probe recognizing DQB1 ∗0201 allele. As expected by the DR-DQ disequilibria, DQA1 ∗0201 [62% in patients versus 26% in controls, relative risk (RR) = 5] and DQA1 ∗0501 (96% versus 56%, RR = 19) show positive association with the disease. Of CD patients, 92% (50% DR3 and 42% DR5,7) compared to 18% of the controls carry both DQA1 ∗0501 and DQB1 ∗0201 alleles, so that the combination confers an RR of 52, higher than both the risks of the single alleles ( DQA1 ∗0501 RR = 19, DQB1 ∗ 0201 RR = 30 ), confirming the primary role of the dimer in determining genetic predisposition to CD both in DR3 and in DR5, 7 subjects.
Author	Mariani, Paolo Martone, Emma Ferrante, Paola Petronzelli, Fiorella Triglione, Paola Bonamico, Margherita Mazzilli, Maria Cristina
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Keywords	RR CD HTC ESPGAN LD PCR SSO Human HLA-DQ-Locus HLA-System Immunogenetics Allele Gene Major histocompatibility system Class II histocompatibility antigen Inheritance Risk factor Digestive diseases Coeliac disease
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Snippet	Celiac disease (CD) has been recently reported to be primarily associated with the DQ(α1 ∗0501, β1 ∗0201) heterodimer encoded in cis on DR3 haplotype and in... Celiac disease (CD) has been recently reported to be primarily associated with the DQ(alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype... Celiac disease (CD) has been recently reported to be primarily associated with the DQ( alpha 10501, beta 10201) heterodimer encoded in cis on DR3 haplotype...
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SubjectTerms	Base Sequence Biological and medical sciences celiac disease Celiac Disease - genetics Celiac Disease - immunology Child Child, Preschool DNA Probes, HLA - genetics Gastroenterology. Liver. Pancreas. Abdomen HLA-DQ Antigens - genetics HLA-DQ Antigens - immunology HLA-DR Antigens - genetics HLA-DR Antigens - immunology Humans Italy Medical sciences Molecular Sequence Data Oligodeoxyribonucleotides - genetics Other diseases. Semiology Polymerase Chain Reaction Risk Stomach. Duodenum. Small intestine. Colon. Rectum. Anus
Title	A study of Italian pediatric celiac disease patients confirms that the primary HLA association is to the DQ(α1 ∗0501, β1 ∗0201) heterodimer
URI	https://dx.doi.org/10.1016/0198-8859(92)90064-T https://www.ncbi.nlm.nih.gov/pubmed/1563982 https://www.proquest.com/docview/16149212 https://www.proquest.com/docview/72893658
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