HLA genotype of patients with severe haemophilia A due to intron 22 inversion with and without inhibitors of factor VIII

Molecular genetic studies have shown that development of antibodies to factor VIII (inhibitors) occurs most frequently in patients with severe haemophilia due to major gene lesions including inversions, stop codons and large deletions. Previous studies of HLA type were performed on inhibitor and non...

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Bibliographic Details
Published inThrombosis and haemostasis Vol. 77; no. 2; p. 238
Main Authors Oldenburg, J, Picard, J K, Schwaab, R, Brackmann, H H, Tuddenham, E G, Simpson, E
Format Journal Article
LanguageEnglish
Published Germany 01.02.1997
Subjects
Alleles
Chromosome Inversion
Disease Susceptibility
Factor VIII - immunology
Factor VIII - therapeutic use
Genes, MHC Class II
Genotype
Germany - epidemiology
Haplotypes
Hemophilia A - epidemiology
Hemophilia A - immunology
Hemophilia A - therapy
HLA-D Antigens - genetics
HLA-D Antigens - immunology
Humans
Introns - genetics
Isoantibodies - genetics
Isoantibodies - immunology
Male
Risk Factors
Germany
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Summary:Molecular genetic studies have shown that development of antibodies to factor VIII (inhibitors) occurs most frequently in patients with severe haemophilia due to major gene lesions including inversions, stop codons and large deletions. Previous studies of HLA type were performed on inhibitor and non-inhibitor patients with diverse uncharacterized mutations which may have confounded detection of significant associations. We therefore selected a group of patients with a single mutation type, the prevalent intron 22 inversion, with or without inhibitors, to determine HLA genotype. Seventy-one such patients, 42 without and 29 with inhibitors (13 high, 9 low and 7 transient responders) were genotyped for MHC Class I HLA-A, -B, -C and Class II HLA-DQA, -DQB and -DRB loci. No strong correlation of any HLA-allele to inhibitor or non-inhibitor status was found. However, alleles of the haplotype HLA-A3, HLA-B7, HLA-C7, HLA-DQA0102, HLA-DQB0602, HLA-DR15 occurred more often in inhibitor patients. Since the alleles of this extended haplotype are common in the North European population only a very strong association would achieve statistical significance. Further studies of groups of patients similar to those studied here will be needed to confirm or exclude this association.
ISSN:0340-6245
DOI:10.1055/s-0038-1655945