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Non-HLA type 1 diabetes genes modulate disease risk together with HLA-DQ and islet autoantibodies

机译:非HLA 1型糖尿病基因与HLA-DQ和胰岛自身抗体一起调节疾病风险

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摘要

The possible interrelations between HLA-DQ, non-HLA single nucleotide polymorphisms (SNPs) and islet autoantibodies were investigated at clinical onset in 1-34 year old type 1 diabetes (T1D) patients (n=305) and controls (n=203). Among the non-HLA SNPs reported by the Type 1 Diabetes Genetics Consortium, 24% were supported in this Swedish replication set including that the increased risk of minor PTPN22 allele and high risk HLA was modified by GAD65 autoantibodies. The association between T1D and the minor AA+AC genotype in ERBB3 gene was stronger among IA-2 autoantibody-positive patients (comparison p=0.047). The association between T1D and the common insulin (AA) genotype was stronger among insulin autoantibody (IAA)-positive patients (comparison p=0.008). In contrast, the association between T1D and unidentified 26471 gene was stronger among IAA-negative (comparison p=0.049) and IA-2 autoantibody-negative (comparison p=0.052) patients. Finally, the association between IL2RA and T1D was stronger among IAA-positive than among IAA-negative patients (comparison p=0.028). These results suggest that the increased risk of T1D by non-HLA genes is often modified by both islet autoantibodies and HLA-DQ. The interactions between non-HLA genes, islet autoantibodies and HLA-DQ should be taken into account in T1D prediction studies as well as in prevention trials aimed at inducing immunological tolerance to islet autoantigens.
机译:在临床发病时研究了1-34岁1型糖尿病(T1D)患者(n = 305)和对照组(n = 203)的HLA-DQ,非HLA单核苷酸多态性(SNP)与胰岛自身抗体之间可能的相关性。在1型糖尿病遗传学协会报告的非HLA SNP中,有24%在该瑞典复制集中得到支持,包括GAD65自身抗体可改善次要PTPN22等位基因和高危HLA的风险增加。在IA-2自身抗体阳性患者中,T1D与ERBB3基因中较小的AA + AC基因型之间的关联更强(比较p = 0.047)。胰岛素自身抗体(IAA)阳性患者中T1D与常见胰岛素(AA)基因型之间的关联更强(比较p = 0.008)。相反,IAA阴性(比较p = 0.049)和IA-2自身抗体阴性(比较p = 0.052)的患者中T1D与26471基因之间的关联更强。最后,IAA阳性患者中IL2RA与T1D之间的关联强于IAA阴性患者(比较p = 0.028)。这些结果表明,非HLA基因导致的T1D风险增加经常被胰岛自身抗体和HLA-DQ所修饰。在T1D预测研究以及旨在诱导对胰岛自身抗原的免疫耐受性的预防试验中,应考虑非HLA基因,胰岛自身抗体和HLA-DQ之间的相互作用。

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