首页> 外文期刊>Journal of Autoimmunity >21-Hydroxylase epitopes are targeted by CD8 T cells in autoimmune Addison's disease.
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21-Hydroxylase epitopes are targeted by CD8 T cells in autoimmune Addison's disease.

机译:在自身免疫性艾迪生氏病中,CD8 T细胞可靶向21-羟化酶表位。

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摘要

In autoimmune adrenal deficiency, autoantibodies target the 21-hydroxylase (21OH) protein. However, it is presumed that autoreactive T cells, rather than antibodies, are the main effectors of adrenal gland destruction, but their identification is still lacking. We performed a T-cell epitope mapping study using 49 overlapping 20mer peptides covering the 21OH sequence in patients with isolated Addison's disease, Autoimmune Polyendocrine Syndrome 1 and 2. IFNgamma ELISPOT responses against these peptides were stronger, broader and more prevalent among patients than in controls, whatever the disease presentation. Five peptides elicited T-cell responses in patients only (68% sensitivity, 100% specificity). Blocking experiments identified IFNgamma-producing cells as CD8 T lymphocytes, with two peptides frequently recognized in HLA-B8+ patients and a third one targeted in HLA-B35+ subjects. In particular, the 21OH(431-450) peptide was highly immunodominant, as it was recognized in more than 30% of patients, all carrying the HLA-B8 restriction element. This 21OH(431-450) region contained an EPLARLEL octamer (21OH(431-438)) predicted to bind to HLA-B8 with high affinity. Indeed, circulating EPLARLEL-specific CD8 T cells were detected at significant frequencies in HLA-B8+ patients but not in controls by HLA tetramer staining. This report enlightens disease-specific T-cell biomarkers and epitopes targeted in autoimmune adrenal deficiency.
机译:在自身免疫性肾上腺缺乏症中,自身抗体靶向21-羟化酶(21OH)蛋白。然而,推测自身反应性T细胞而不是抗体是肾上腺破坏的主要效应子,但仍缺乏鉴定。我们对49例重叠的20mer肽进行了T细胞表位作图研究,这些肽覆盖了患有独立性Addison病,自身免疫性多内分泌综合征1和2的患者的21OH序列。与对照组相比,IFNgamma ELISPOT对这些肽的反应更强,更广泛,更普遍,无论疾病表现如何。五种肽仅在患者中引起T细胞反应(敏感性为68%,特异性为100%)。阻断实验将产生IFNγ的细胞鉴定为CD8 T淋巴细胞,其中两种肽在HLA-B8 +患者中经常被识别,第三种在HLA-B35 +患者中被靶向。特别是,21OH(431-450)肽具有高度免疫优势,因为在30%以上的患者中都发现了该肽,所有患者均携带HLA-B8限制元件。该21OH(431-450)区包含一个EPLARLEL八聚体(21OH(431-438)),预计它会以高亲和力与HLA-B8结合。实际上,在HLA-B8 +患者中以显着频率检测到了循环的EPLARLEL特异性CD8 T细胞,但在HLA四聚体染色中未在对照中检测到。该报告启发了针对自身免疫性肾上腺缺乏症的疾病特异性T细胞生物标志物和表位。

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