Association of the large multifunctional proteasome (LMP2) gene with Graves' disease is a result of linkage disequilibrium with the HLA haplotype DRB1*0304-DQB1*02-DQA1*0501

J M Heward; A Allahabadia; M C Sheppard; A H Barnett; J A Franklyn; S C Gough

doi:10.1046/j.1365-2265.1999.00755.x

Association of the large multifunctional proteasome (LMP2) gene with Graves' disease is a result of linkage disequilibrium with the HLA haplotype DRB10304-DQB102-DQA1*0501

Clin Endocrinol (Oxf). 1999 Jul;51(1):115-8. doi: 10.1046/j.1365-2265.1999.00755.x.

Authors

J M Heward¹, A Allahabadia, M C Sheppard, A H Barnett, J A Franklyn, S C Gough

Affiliation

¹ Department of Medicine, University of Birmingham, Queen Elizabeth Hospital, Birmingham, UK.

PMID: 10468973
DOI: 10.1046/j.1365-2265.1999.00755.x

Abstract

Objective: The large multifunctional proteasome (LMP) molecules are over expressed in thyrocytes, the target cells of Graves' disease, and the LMP genes are found within the MHC class II region. The LMP genes may therefore play a role in susceptibility to Graves' disease. The aim of this this study was to determine whether polymorphisms of the LMP genes, LMP 2 and LMP 7 are in linkage disequilibrium with Graves' disease.

Design: Target DNA was amplified using the polymerase chain reaction. The distribution of an Arg-His polymorphism in the LMP 2 gene and a G/T polymorphism in the LMP 7 gene, both of which lead to the presence of an HhaI restriction site, were investigated in a population based case control and family based study in patients with Graves' disease.

Patients: We obtained DNA from 306 patients with Graves' disease and 364 control subjects for the population based case-control study. In an independent family based study, DNA was obtained from 129 families including both parents, an affected sibling with Graves' disease and an unaffected sibling. All families, patients and control subjects were white caucasians.

Measurements: Frequencies of the alleles and genotypes of the LMP 2 and LMP 7 genes were compared between patients and control subjects using the chi2 test. Transmission of alleles from heterozygous parents to affected and unaffected offspring was assessed using the transmission disequilibrium test (TDT).

Results: In the case control study, no difference in allele or genotype frequency was seen between patients and control subjects at the LMP7 locus. At the LMP2 locus the R allele and the RH genotype were increased in subjects with Graves' disease when compared with control subjects (R allele: 36.3% vs. 29.5%, pc = 0. 0164; RH genotype: 56.5% vs. 45%, pc = 0.0102). However, the R allele was in linkage disequilibrium with the associated HLA DRB1*0304-DQB1*02-DQA1*0501 haplotype, delta = 0.102. Within the family based study, no preferential allelic transmission was seen from heterozygote parents to offspring at either loci.

Conclusion: These results show that association of the LMP 2 locus with Graves' disease is due to linkage disequilibrium with the associated HLA haplotype DRB1*0304-DQB1*02-DQA1*0501.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Case-Control Studies
Chi-Square Distribution
Cysteine Endopeptidases*
Genotype
Graves Disease / genetics*
HLA-DQ Antigens / genetics
HLA-DQ alpha-Chains
HLA-DR Antigens / genetics*
HLA-DRB1 Chains
Haplotypes
Humans
Linkage Disequilibrium*
Multienzyme Complexes*
Proteasome Endopeptidase Complex
Proteins / genetics*

Substances

HLA-DQ Antigens
HLA-DQ alpha-Chains
HLA-DQA1 antigen
HLA-DR Antigens
HLA-DRB1 Chains
Multienzyme Complexes
Proteins
LMP-2 protein
Cysteine Endopeptidases
LMP7 protein
Proteasome Endopeptidase Complex

Grants and funding

Wellcome Trust/United Kingdom