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KIR in Type 1 Diabetes: Disparate Distribution of Activating and Inhibitory Natural Killer Cell Receptors in Patients Versus HLA-Matched Control Subjects

机译:1型糖尿病的KIR:患者与HLA匹配的对照受试者中活化和抑制性自然杀伤细胞受体的分布不同

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Killer cell immunoglobulin-like receptors (KIRs) modulate natural killer cell and T-cell function by interacting with HLA class 1 ligands on target cells. Both KIR and HLA are highly polymorphic. We studied the influence of KIR and HLA class 1 genes on the susceptibility to develop type 1 diabetes. The results showed increased numbers of activating KIR genes in patients compared with control subjects (P = 0.049). The combination of the activating KIR2DS2 gene, together with its putative HLA ligand, was present more frequently in patients than in diabetes high-risk HLA-matched control subjects (P = 0.030). Moreover, our results imply that an increase in activating KIR2DS2-HLA ligand pairs combined with a lack of inhibitory KIR-HLA ligand pairs is associated with an additional risk to develop type 1 diabetes in individuals with diabetes high-risk HLA alleles (P = 0.035). We propose that the genetic imbalance between KIR and their HLA class 1 ligands may enhance the activation of T-cells with a low affinity for pancreatic self-antigens, thereby contributing to the pathogenesis of type 1 diabetes.
机译:杀伤细胞免疫球蛋白样受体(KIR)通过与靶细胞上的HLA 1类配体相互作用来调节自然杀伤细胞和T细胞功能。 KIR和HLA都是高度多态的。我们研究了KIR和HLA 1类基因对发展1型糖尿病的易感性的影响。结果显示,与对照组相比,患者的激活KIR基因数目增加(P = 0.049)。与糖尿病高危HLA匹配对照组相比,KIR2DS2激活基因及其推定的HLA配体的组合在患者中的出现频率更高(P = 0.030)。此外,我们的结果表明,在患有高风险HLA等位基因的个体中,激活KIR2DS2-HLA配体对的增加与缺乏抑制性KIR-HLA配体对的组合会增加患1型糖尿病的风险(P = 0.035) )。我们建议,KIR及其HLA 1类配体之间的遗传失衡可能会增强对胰腺自身抗原的低亲和力的T细胞的活化,从而促进1型糖尿病的发病机理。

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