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Rapamycin Conditioning of Dendritic Cells Differentiated from Human ES Cells Promotes a Tolerogenic Phenotype

机译:雷帕霉素调节人胚胎干细胞分化的树突状细胞促进耐受性表型

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摘要

While human embryonic stem cells (hESCs) may one day facilitate the treatment of degenerative diseases requiring cell replacement therapy, the success of regenerative medicine is predicated on overcoming the rejection of replacement tissues. Given the role played by dendritic cells (DCs) in the establishment of immunological tolerance, we have proposed that DC, rendered tolerogenic during their differentiation from hESC, might predispose recipients to accept replacement tissues. As a first step towards this goal, we demonstrate that DC differentiated from H1 hESCs (H1-DCs) are particularly responsive to the immunosuppressive agent rapamycin compared to monocyte-derived DC (moDC). While rapamycin had only modest impact on the phenotype and function of moDC, H1-DC failed to upregulate CD40 upon maturation and displayed reduced immunostimulatory capacity. Furthermore, coculture of naïve allogeneic T cells with rapamycin-treated H1-DC promoted an increased appearance of CD25hi Foxp3+ regulatory T cells, compared to moDC. Our findings suggest that conditioning of hESC-derived DC with rapamycin favours a tolerogenic phenotype.
机译:虽然人类胚胎干细胞(hESCs)有一天可能会促进需要细胞替代疗法的退行性疾病的治疗,但再生医学的成功取决于克服替代组织的排斥。鉴于树突状细胞(DC)在建立免疫耐受中所起的作用,我们提出DC在其与hESC分化过程中具有致耐受性,可能使受体容易接受替代组织。作为朝着这个目标迈出的第一步,我们证明了与单核细胞衍生DC(moDC)相比,从H1 hESCs(H1-DCs)分化出来的DC对免疫抑制剂雷帕霉素特别有反应。尽管雷帕霉素对moDC的表型和功能仅有中等程度的影响,但H1-DC在成熟时未能上调CD40并显示出降低的免疫刺激能力。此外,与moDC相比,将未经处理的同种异体T细胞与雷帕霉素处理的H1-DC共培养可促进CD25hi Foxp3 +调节性T细胞的出现。我们的研究结果表明,雷帕霉素对hESC衍生DC的调节有利于产生耐受性的表型。

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