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New strategy for testing efficacy of immunotherapeutic compounds for diabetes in vitro

机译:体外测试免疫治疗化合物对糖尿病疗效的新策略

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摘要

BackgroundThe valuable role of immunotherapy in treating autoimmune diseases is increasingly recognized by those involved in the research and clinical application of new biopharmaceuticals products. However, many aspects related to the mechanisms of immune-modulated therapies remain to be elucidated in order to explore fully the emerging opportunities. The non-obese diabetic NOD mouse develops insulin-dependent diabetes mellitus spontaneously as a consequence of an autoimmune process in the presence of pathogenic CD4+ T cells that typically exhibit Th17 cell phenotypes. The change of a Th17 phenotype into a pattern of regulatory T cells (Treg) is extremely important in controlling autoimmune diseases. Heat shock proteins (HSPs) are stress-induced proteins with immunoregulatory properties. In the current study, the capacity of Hsp65 and Hsp70 mycobacterial HSPs and a constructed DNA encoded Hsp65 (DNAhsp65) to transform the pattern of the immune response from Th17 into Treg cells has been studied in vitro using co-cultures of antigen presenting cells (APCs) and T cells in NOD mice.
机译:背景技术免疫疗法在治疗自身免疫性疾病中的重要作用已被参与新生物制药产品研究和临床应用的人们越来越认识到。然而,与免疫调节疗法的机制有关的许多方面仍有待阐明,以便充分探索新出现的机会。非肥胖型糖尿病NOD小鼠在存在通常表现出Th17细胞表型的致病性CD4 + T细胞的情况下,由于自身免疫过程而自发发展为胰岛素依赖型糖尿病。 Th17表型转变为调节性T细胞(Treg)的模式在控制自身免疫性疾病中极为重要。热激蛋白(HSP)是具有免疫调节特性的应激诱导蛋白。在当前的研究中,使用抗原呈递细胞(APC)的共培养物体外研究了Hsp65和Hsp70分枝杆菌HSP的能力以及构建的DNA编码的Hsp65(DNAhsp65)将Th17免疫应答模式转化为Treg细胞的能力。 )和NOD小鼠的T细胞。

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