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CD8 + T细胞反应可识别人类1型糖尿病中的β细胞自身免疫。

CD8+ T-cell responses identify beta-cell autoimmunity in human type 1 diabetes.

作者信息

Mallone Roberto, Martinuzzi Emanuela, Blancou Philippe, Novelli Giulia, Afonso Georgia, Dolz Manuel, Bruno Graziella, Chaillous Lucy, Chatenoud Lucienne, Bach Jean-Marie, van Endert Peter

机构信息

INSERM U580, Hôpital Necker, 161 rue de Sèvres, 75743 Paris Cedex 15, France.

出版信息

Diabetes. 2007 Mar;56(3):613-21. doi: 10.2337/db06-1419.

DOI:10.2337/db06-1419
PMID:17327428
Abstract

Despite the understanding that type 1 diabetes pathogenesis is mediated by T-cells, detection of these rare lymphocytes remains largely elusive. Suitable T-cell assays are highly needed, since they could offer preclinical diagnoses and immune surrogate end points for clinical trials. Although CD4+ T-cell assays have met with limited success, CD8+ T-cells are increasingly recognized as key actors in the diabetes of the NOD mouse. CD8+ T-cells are likely to play a role also in humans and may provide new markers of beta-cell autoimmunity. Taking advantage of a panel of HLA-A2-restricted beta-cell epitopes derived from preproinsulin, GAD, and islet glucose-6-phosphatase catalytic subunit-related protein (IGRP), we have implemented an islet-specific CD8+ T-cell interferon-gamma enzyme-linked immunospot (ISL8Spot) assay. The ISL8Spot assay is capable of detecting and quantifying beta-cell-reactive CD8+ T-cells directly ex vivo, without any preliminary expansion, using either fresh or frozen samples. Positive ISL8Spot responses separate new-onset diabetic and healthy samples with high accuracy (86% sensitivity, 91% specificity), using as few as five immunodominant epitopes. Moreover, sensitivity reaches 100% when the ISL8Spot assay is complemented by antibody determinations. Combination of CD8+ T-cell measurements with immune intervention strategies may open new avenues toward type 1 diabetes prediction and prevention.

摘要

尽管人们已经认识到1型糖尿病的发病机制是由T细胞介导的,但检测这些罕见的淋巴细胞在很大程度上仍然难以实现。非常需要合适的T细胞检测方法,因为它们可以为临床试验提供临床前诊断和免疫替代终点。虽然CD4+ T细胞检测取得的成功有限,但CD8+ T细胞越来越被认为是NOD小鼠糖尿病中的关键因素。CD8+ T细胞在人类中可能也发挥作用,并可能提供β细胞自身免疫的新标志物。利用一组源自胰岛素原、谷氨酸脱羧酶(GAD)和胰岛葡萄糖-6-磷酸酶催化亚基相关蛋白(IGRP)的HLA-A2限制性β细胞表位,我们实施了一种胰岛特异性CD8+ T细胞干扰素-γ酶联免疫斑点(ISL8Spot)检测。ISL8Spot检测能够直接在体外检测和定量β细胞反应性CD8+ T细胞,无需任何预先扩增,可使用新鲜或冷冻样本。使用少至五个免疫显性表位,阳性ISL8Spot反应能以高精度区分新发糖尿病和健康样本(敏感性86%,特异性91%)。此外,当ISL8Spot检测辅以抗体测定时,敏感性可达100%。将CD8+ T细胞测量与免疫干预策略相结合可能为1型糖尿病的预测和预防开辟新途径。

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CD8+ T-cell responses identify beta-cell autoimmunity in human type 1 diabetes.CD8 + T细胞反应可识别人类1型糖尿病中的β细胞自身免疫。
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A new role for an old player: do B cells unleash the self-reactive CD8+ T cell storm necessary for the development of type 1 diabetes?老参与者的新角色:B细胞是否引发了1型糖尿病发展所需的自身反应性CD8 + T细胞风暴?
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"Humanized" HLA transgenic NOD mice to identify pancreatic beta cell autoantigens of potential clinical relevance to type 1 diabetes.“人源化” HLA转基因NOD小鼠,用于鉴定与1型糖尿病具有潜在临床相关性的胰腺β细胞自身抗原。
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CD8(+) T cells specific for beta cells encounter their cognate antigens in the islets of NOD mice.对β细胞具有特异性的CD8(+) T细胞在非肥胖糖尿病(NOD)小鼠的胰岛中遇到其同源抗原。
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