Literature DB >> 6932402

HLA and Graves' disease: an association with HLA-DRw3.

H Allannic, R Fauchet, Y Lorcy, J Heim, M Gueguen, A M Leguerrier, B Genetet.   

Abstract

HLA-A, -B, and -C antigens were tested by a standard lymphocyte microcytotoxicity technique in 86 Caucasians patients from western France with Graves' disease, and the data were compared with findings in 356 healthy controls. For HLA-DR antigen typing performed by lymphocyte microcytotoxicity testing using a long incubation time, the data were compared to findings in 100 healthy controls. An increase was found in the frequency of HLA-DRw3 [51.16% of patients vs. 20% of controls, corrected P (Pc) < 0.0003; relative risk (rr), 4.19) associated with an increased frequency of HLA-B8 (44.19% of patients vs. 22.47% of controls; Pc < 0.001; rr, 2.73) and HLA-A1 (40.7% of patients vs. 28.93% of controls; Pc < 0.03; rr, 1.71). In contrast, a diminished frequency was found for HLA-B12 (12.79% vs. 31.74%; Pc < 0.01). The antigen combination B8-DRw3 was noted in 37 of the 86 Graves' disease patients compared with 13 of 100 controls (Pc < 0.00003). No association was observed between HLA antigens and the different manifestations of the disease, such as the presence of goiter and/or exophthalmos, or the severity of clinical or biochemical signs. The present findings confirm the reported increase in the frequency of HLA-B8 in patients with Graves' disease. The most striking finding was the prevalence of HLA-DRw3, which, together with recent reports on lymphocyte-defined D locus determinants pointing to an increase frequency of HLA-Dw3, suggests that the gene or genes conferring susceptibility to Graves' disease may be located close to the HLA-D (DR) region of the sixth chromosome.

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Year:  1980        PMID: 6932402     DOI: 10.1210/jcem-51-4-863

Source DB:  PubMed          Journal:  J Clin Endocrinol Metab        ISSN: 0021-972X            Impact factor:   5.958


  14 in total

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Review 2.  Role of genetic and non-genetic factors in the etiology of Graves' disease.

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Journal:  J Endocrinol Invest       Date:  2014-11-25       Impact factor: 4.256

3.  Relative predispositional effects (RPEs) of marker alleles with disease: HLA-DR alleles and Graves disease.

Authors:  H Payami; S Joe; N R Farid; V Stenszky; S H Chan; P P Yeo; J S Cheah; G Thomson
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4.  Linkage analysis of "necessary" disease loci versus "susceptibility" loci.

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Journal:  Am J Hum Genet       Date:  1993-01       Impact factor: 11.025

5.  Combined segregation and linkage analysis of Graves disease with a thyroid autoantibody diathesis.

Authors:  D C Shields; S Ratanachaiyavong; A M McGregor; A Collins; N E Morton
Journal:  Am J Hum Genet       Date:  1994-09       Impact factor: 11.025

6.  HLA-DR4 associated response to corticosteroids in Graves' ophthalmopathy patients.

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7.  Graves' disease: immunological and immunogenetic indicators of relapse.

Authors:  T W de Bruin; J H Bolk; J K Bussemaker; T Stijnen; G M Schreuder; R R de Vries; D van der Heide
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8.  Mapping of thyroglobulin epitopes: presentation of a 9mer pathogenic peptide by different mouse MHC class II isotypes.

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10.  HLA antigens in Greek patients with thyrotoxicosis (Graves' disease and toxic nodular goiter).

Authors:  C Papasteriades; M N Alevizaki-Harhalaki; J Economidou; D G Ikkos
Journal:  J Endocrinol Invest       Date:  1984-08       Impact factor: 4.256

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