Inducing immune tolerance: a focus on Type 1 diabetes mellitus.

Dan Xu, Suchitra Prasad, Stephen D Miller
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引用次数: 24

Abstract

Tolerogenic strategies that specifically target diabetogenic immune cells in the absence of complications of immunosuppression are the desired treatment for the prevention or even reversal of Type 1 diabetes (T1D). Antigen (Ag)-based therapies must not only suppress disease-initiating diabetogenic T cells that are already activated, but, more importantly, prevent activation of naive auto-Ag-specific T cells that may become autoreactive through epitope spreading as a result of Ag liberation from damaged islet cells. Therefore, identification of auto-Ags relevant to T1D initiation and progression is critical to the design of effective Ag-specific therapies. Animal models of T1D have been successfully employed to identify potential diabetogenic Ags, and have further facilitated translation of Ag-specific tolerance strategies into human clinical trials. In this review, we highlight important advances using animal models in Ag-specific T1D immunotherapies, and the application of the preclinical findings to human subjects. We provide an up-to-date overview of the strengths and weaknesses of various tolerance-inducing strategies, including infusion of soluble Ags/peptides by various routes of delivery, genetic vaccinations, cell- and inert particle-based tolerogenic approaches, and various other strategies that target distinct tolerance-inducing pathways.

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诱导免疫耐受:1型糖尿病的焦点。
在没有免疫抑制并发症的情况下,特异性靶向糖尿病免疫细胞的耐受性策略是预防甚至逆转1型糖尿病(T1D)的理想治疗方法。以抗原(Ag)为基础的治疗不仅要抑制已经激活的引发疾病的糖尿病性T细胞,更重要的是,要防止原始的自体Ag特异性T细胞的激活,这些T细胞可能由于受损胰岛细胞中Ag的释放而通过表位扩散而产生自身反应。因此,识别与T1D发生和进展相关的auto-Ags对于设计有效的ag特异性治疗方法至关重要。T1D动物模型已被成功用于鉴定潜在的致糖尿病Ags,并进一步促进了将ag特异性耐受性策略转化为人类临床试验。在这篇综述中,我们重点介绍了利用动物模型进行ag特异性T1D免疫治疗的重要进展,以及临床前研究结果在人类受试者中的应用。我们提供了各种耐受性诱导策略的优点和缺点的最新概述,包括通过各种递送途径输注可溶性Ags/肽,遗传疫苗,基于细胞和惰性颗粒的耐受性方法,以及针对不同耐受性诱导途径的各种其他策略。
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