HLA‐A, B, Cw and DRB1, DRB3/4/5, DQB1, DPB1 Frequencies in German Immunoglobulin A‐Deficient Individuals

Machulla, Helmut K.G.; Schönermarck, Ulf; Schaaf, Astrid; Müller, Lutz; Kloss, Christopher C.; Krüger, Jana; Kunze, Gerhard; Schönermarck, G; Langner, Jürgen

doi:10.1046/j.1365-3083.2000.00765.x

Cited by 25 publications

(24 citation statements)

References 18 publications

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“…Of 26 homozygous probands, only a single case exhibited homozygosity in the telomeric part of the class III region and not in the HLA-DQ/DR region. The frequencies of unaffected homozygous individuals (7.7% for 4-STRs and 5.9% for 5-STRs) were comparable to ϳ6 -8% homozygosity observed in large numbers of population controls typed for HLA-DR or -DQ specificities (38,39).…”

Section: Homozygosity At Hla-dq/drsupporting

confidence: 64%

“…Because previous association studies suggested an increase of homozygosity in affected individuals vs controls both for HLA-DQ/DR (38,39) and HLA STRs (21), we estimated the relative risk of IgAD/CVID conferred by homozygous stretches at adjacent STRs and examined which region was associated with the highest risk. We chose to test 4-and 5-STR sliding windows because the average probability of being homozygous by chance was sufficiently low (ϳ2 ϫ 10 Ϫ3 and 3 ϫ 10 Ϫ4 , respectively), minimizing random homozygosity at adjacent STRs.…”

Section: Homozygosity At Hla-dq/drmentioning

confidence: 99%

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Fine-Scale Mapping at IGAD1 and Genome-Wide Genetic Linkage Analysis Implicate HLA-DQ/DR as a Major Susceptibility Locus in Selective IgA Deficiency and Common Variable Immunodeficiency

Královičová

Hammarström

Plebani

et al. 2003

The Journal of Immunology

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Selective IgA deficiency (IgAD) and common variable immunodeficiency (CVID) are the most common primary immunodeficiencies in humans. A high degree of familial clustering, marked differences in the population prevalence among ethnic groups, association of IgAD and CVID in families, and a predominant inheritance pattern in multiple-case pedigrees have suggested a strong, shared genetic predisposition. Previous genetic linkage, case-control, and family-based association studies mapped an IgAD/CVID susceptibility locus, designated IGAD1, to the MHC, but its precise location within the MHC has been controversial. We have analyzed a sample of 101 multiple- and 110 single-case families using 36 markers at the IGAD1 candidate region and mapped homozygous stretches across the MHC shared by affected family members. Haplotype analysis, linkage disequilibrium, and homozygosity mapping indicated that HLA-DQ/DR is the major IGAD1 locus, strongly suggesting the autoimmune pathogenesis of IgAD/CVID. This is supported by the highest excess of allelic sharing at 6p in the genome-wide linkage analysis of 101 IgAD/CVID families using 383 marker loci, by previously reported restrictions of the T cell repertoires in CVID, the presence of autoantibodies, impaired T cell activation, and a dysregulation of a number of genes in the targeted immune system. IgAD/CVID may thus provide a useful model for the study of pathogenesis and novel therapeutic strategies in autoimmune diseases.

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Section: Homozygosity At Hla-dq/drsupporting

confidence: 64%

Section: Homozygosity At Hla-dq/drmentioning

confidence: 99%

Fine-Scale Mapping at IGAD1 and Genome-Wide Genetic Linkage Analysis Implicate HLA-DQ/DR as a Major Susceptibility Locus in Selective IgA Deficiency and Common Variable Immunodeficiency

Královičová

Hammarström

Plebani

et al. 2003

The Journal of Immunology

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“…Homozygosity for the ancestral 8.1 haplotype increases the risk of development of the disease even further (10). Other haplotypes, including HLA-DR7, DQ2 and DR1, DQ5 are also associated with IgAD (11). In contrast, the DR15, DQ6 haplotype has been shown to confer an almost complete protection against the disorder (12)(13)(14).…”

Section: Introductionmentioning

confidence: 99%

Selective IgA Deficiency in Autoimmune Diseases

Wang

Shen

Vyse

et al. 2011

Mol Med

174

118

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“…Most studies support a polygenic inheritance with a susceptibility locus (designated IGAD1) in the MHC. Associations of IgAD were first described with HLA class I alleles, most consistently with A1 and B8 (2-4) but also with A28, B14 (5-7), and B44 (8,9). Subsequently, an association with the class II allele HLA-DR3 was repeatedly observed (4, 9 -14), in addition to associations with DR1 (7, 9 -11) and DR7 (6,9,10,12).…”

mentioning

confidence: 95%

“…Associations of IgAD were first described with HLA class I alleles, most consistently with A1 and B8 (2-4) but also with A28, B14 (5-7), and B44 (8,9). Subsequently, an association with the class II allele HLA-DR3 was repeatedly observed (4, 9 -14), in addition to associations with DR1 (7, 9 -11) and DR7 (6,9,10,12). Some early studies already signaled that the association was with particular combinations of MHC alleles rather than with individual alleles per se (5,7) and that these combinations reflected extended, conserved, or "ancestral" haplotypes A1-B8-DR3, A28-B14-DR1, and B44-DR7 (7,8,11,15).…”

mentioning

confidence: 99%

MHC Susceptibility Genes to IgA Deficiency Are Located in Different Regions on Different HLA Haplotypes

Concha

Fernández‐Arquero

Gual

et al. 2002

The Journal of Immunology

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Familial predisposition to IgA deficiency (IgAD) suggests that genetic factors influence susceptibility. Most studies support a polygenic inheritance with a susceptibility locus (designated IGAD1) in the MHC, but its exact location is still controversial. This study aimed to map the predisposing IGAD1 locus (or loci) within the MHC by investigating the pattern of association of the disease with several markers in the region. DNA-based techniques were used to type individual alleles of four polymorphic HLA genes (HLA-DR, -DQA1, -DQB1, and HLA-B), six microsatellites (all located between HLA-DR and HLA-B), and three single nucleotide polymorphisms on the TNF gene. The frequencies of these alleles were compared among ethnically matched populations comprising 182 patients and 343 controls. Additionally, we investigated parents and siblings of 100 of these patients. All four parental haplotypes were established in each family (n = 400), and transmission disequilibrium tests were performed. Surprisingly, our results did not support the hypothesis of a unique susceptibility gene being shared by all MHC susceptibility haplotypes. On HLA-DR1 and -DR7-positive haplotypes IGAD1 mapped to the class II region, whereas on haplotypes carrying HLA-DR3 the susceptibility locus mapped to the telomeric end of the class III region, as reported previously. Our results show how, in complex diseases, individuals may be affected for different genetic reasons and a single linkage signal to a region of a chromosome may actually be the result of disease-predisposing alleles in different linked genes in different pedigrees.

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HLA‐A, B, Cw and DRB1, DRB3/4/5, DQB1, DPB1 Frequencies in German Immunoglobulin A‐Deficient Individuals

Cited by 25 publications

References 18 publications

Fine-Scale Mapping at IGAD1 and Genome-Wide Genetic Linkage Analysis Implicate HLA-DQ/DR as a Major Susceptibility Locus in Selective IgA Deficiency and Common Variable Immunodeficiency

Fine-Scale Mapping at IGAD1 and Genome-Wide Genetic Linkage Analysis Implicate HLA-DQ/DR as a Major Susceptibility Locus in Selective IgA Deficiency and Common Variable Immunodeficiency

Selective IgA Deficiency in Autoimmune Diseases

MHC Susceptibility Genes to IgA Deficiency Are Located in Different Regions on Different HLA Haplotypes

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