CLASS-III ALLELES AND HIGH-RISK MHC HAPLOTYPES IN TYPE-I DIABETES-MELLITUS, GRAVES-DISEASE AND HASHIMOTOS-THYROIDITIS

  • 1 April 1986
    • journal article
    • research article
    • Vol. 3  (2) , 143-157
Abstract
By typing a large quantity of family-based material for HLA-B, HLA-DR, C4, C2 and factor B, were were able to derive four-gene complement haplotypes (C4A, C4B, C2, BF) and six-gene MHC haplotypes (HLA-B, complement, HLA-DR). Fourteen six-gene MHC haplotypes showed linkage disequilibrium but exact frequencies could not be determined because it was not always possible to assign null C4 alleles in familes where null genes were not clearly seen to segregate. Comparison of unrelated type I diabetes, Graves'' disease and Hashimoto''s thyroiditis patients with healthy unrelated controls revealed the following MHC allele associations: C4B*3, HLA-DR3 and HLA-DR4 with type I diabetes; BF*F1 and HLA-DR3 with Graves'' disease: HLA-DR4 with Hashimoto''s thyroiditis. By typing families of type I diabetes and Graves'' disease patients we were able to derive two high-risk DR3+ haplotypes for both type I diabetes and Graves'' disease. These are HLA-B8 C4A*Q0 C4B*1 BF*S HLA-DR3 and HLA-B18 C4A*3 C4B*Q0 BF*F1 HLA-DR3, and these haplotypes account for most of the associations between these diseases and HLA-DR3. The MHC haplotype HLA-B15 C4A* 3 C4B*3 BF*S HLA-DR4 also carries high risk for type I diabetes in this group of patients. Our data suggest that other DR4+ haplotypes, probably containing C4A*3 C4B*1, carry increased risk for type I diabetes whereas haplotypes containing DR4 and C4 C4A*3 C4B*Q0 do not. Our phenotype data suggest that DR4 in Hashimoto''s thyroiditis is frequently associated with HLA-B44, C4A*3, C4B*1 and BF*S.

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