[No authors listed]
CONTEXT:The genetic background of young-onset Graves disease (GD) remains largely unknown. An intronic variant in human leukocyte antigen (HLA) complex P5 (HCP5) has previously been associated with GD susceptibility and age of onset in a cohort of Polish patients. OBJECTIVE:We aimed to investigate the association of the HCP5 variant rs3094228 with GD susceptibility and age of onset in a UK cohort and conduct a meta-analysis of UK and Polish data. DESIGN AND PARTICIPANTS:rs3094228 was genotyped in 469 UK patients with GD using Taqman chemistry. Genotype frequencies were compared with genotypic data available from the Wellcome Trust case-control consortium using logistic regression analysis. To determine whether rs3094228 is independently associated with age of GD onset, the HLA DRB1*0301 tagging variant, rs535777, was also genotyped. RESULTS:The C allele of rs3094228 was overrepresented in the UK GD cohort compared with controls (Pâallele=5.08â Ãâ 10-9, odds ratio 1.76; [95% confidence interval, 1.46-2.13]). This association was more marked in young-onset GD (<30 years) (Pâallele=1.70â Ãâ 10-10 vs Pâallele=0.0008). The meta-analysis of UK and Polish data supported the association of the C allele with GD susceptibility (Pâallele=1.79â Ãâ 10-5) and age of onset (Pâallele=5.63â Ãâ 10-8). Haplotype analysis demonstrated that rs3094228 is associated with age of GD onset (Pâ =â 2.39â Ãâ 10-6) independent of linkage disequilibrium with HLA DRB1*0301. CONCLUSION:The rs3094228 HCP5 polymorphism is independently associated with GD susceptibility and age of onset in a UK GD cohort. Our findings indicate a potential role of long noncoding ribonucleic acids, including HCP5, in GD pathogenesis, particularly in the younger population.
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