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Obtaining regulatory T cells from uraemic patients awaiting kidney transplantation for use in clinical trials

机译:从等待肾脏移植的尿毒症患者中获得调节性T细胞用于临床试验

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摘要

Adoptive transfer of regulatory T cells (Tregs) has been proposed for use as a cellular therapy to induce transplantation tolerance. Preclinical data are encouraging, and clinical trials with Treg therapy are anticipated. In this study, we investigate different strategies for the isolation and expansion of CD4+CD25highCD127low Tregs from uraemic patients. We use allogeneic dendritic cells (DCs) as feeder cells for the expansion and compare Treg preparations isolated by either fluorescence activated cell sorting (FACS) or magnetic activated cell sorting (MACS) that have been expanded subsequently with either mature or tolerogenic DCs. Expanded Treg preparations have been characterized by their purity, cytokine production and in-vitro suppressive ability. The results show that Treg preparations can be isolated from uraemic patients by both FACS and MACS. Also, the type of feeder cells used in the expansion affects both the purity and the functional properties of the Treg preparations. In particular, FACS-sorted Treg preparations expanded with mature DCs secrete more interleukin (IL)-10 and granzyme B than FACS-sorted Treg preparations expanded with tolerogenic DCs. This is a direct comparison between different isolation techniques and expansion protocols with Tregs from uraemic patients that may guide future efforts to produce clinical-grade Tregs for use in kidney transplantation.
机译:已经提出调节性T细胞(Tregs)的过继转移用作诱导移植耐受的细胞疗法。临床前数据令人鼓舞,并且预期使用Treg治疗的临床试验。在这项研究中,我们研究了从尿毒症患者中分离和扩增CD4 + CD25 CD127 Treg的不同策略。我们使用同种异体树突状细胞(DCs)作为饲养细胞进行扩增,并比较通过荧光激活细胞分选(FACS)或磁性激活细胞分选(MACS)分离的Treg制剂,这些细胞随后被成熟或耐受性DC扩展。扩展的Treg制剂的特征在于它们的纯度,细胞因子的产生和体外抑制能力。结果表明,可以通过FACS和MACS从尿毒症患者中分离Treg制剂。同样,用于扩增的饲养细胞的类型影响Treg制品的纯度和功能性质。特别是,用FACS分选的Treg制剂与成熟的DC一起扩增的分泌的白介素(IL)-10和颗粒酶B比用耐受性DC的FACS分选的Treg制剂分泌更多。这是尿毒症患者使用Treg的不同分离技术和扩增方案之间的直接比较,这可能会指导将来生产用于肾脏移植的临床级Treg的努力。

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