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T Cell Recognition of Autoantigens in Human Type 1 Diabetes: Clinical Perspectives

机译:人类1型糖尿病患者自身抗原的T细胞识别:临床观点

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Type 1 diabetes (T1D) is an autoimmune disease driven by the activation of lymphocytes against pancreatic β -cells. Among β -cell autoantigens, preproinsulin has been ascribed a key role in the T1D process. The successive steps that control the activation of autoreactive lymphocytes have been extensively studied in animal models of T1D, but remains ill defined in man. In man, T lymphocytes, especially CD8~(+)T cells, are predominant within insulitis. Developing T-cell assays in diabetes autoimmunity is, thus, a major challenge. It is expected to help defining autoantigens and epitopes that drive the disease process, to pinpoint key functional features of epitope-specific T lymphocytes along the natural history of diabetes and to pave the way towards therapeutic strategies to induce immune tolerance to β -cells. New T-cell technologies will allow defining autoreactive T-cell differentiation programs and characterizing autoimmune responses in comparison with physiologically appropriate immune responses. This may prove instrumental in the discovery of immune correlates of efficacy in clinical trials.
机译:1型糖尿病(T1D)是由针对胰腺β细胞的淋巴细胞活化引起的自身免疫性疾病。在β细胞自身抗原中,胰岛素原被认为是T1D过程中的关键作用。在T1D动物模型中已经广泛研究了控制自身反应性淋巴细胞激活的连续步骤,但在人类中仍然不清楚。在人类中,T淋巴细胞,特别是CD8〜(+)T细胞,在岛炎中占主导地位。因此,在糖尿病自身免疫中发展T细胞检测方法是一项重大挑战。有望帮助定义驱动疾病进程的自身抗原和抗原决定簇,沿着糖尿病的自然病程查明抗原决定簇特异性T淋巴细胞的关键功能特征,并为诱导对β细胞的免疫耐受的治疗策略铺平道路。与生理上适当的免疫反应相比,新的T细胞技术将允许定义自身反应性T细胞分化程序并表征自身免疫反应。这可能被证明有助于临床试验中发现免疫相关功效。

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