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Directed differentiation of human embryonic stem cells into thymic epithelial progenitor-like cells reconstitutes the thymic microenvironment in vivo

机译:将人类胚胎干细胞定向分化为胸腺上皮祖细胞样细胞,可在体内重建胸腺微环境

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摘要

Thymus transplantation has great clinical potential for treating immunological disorders, but the shortage of transplant donors limits the progress of this therapy. Human embryonic stem cells (hESCs) are promising cell sources for generating thymic epithelial cells. Here, we report a stepwise protocol to direct the differentiation of hESCs into thymic epithelial progenitor-like cells (TEPLCs) by mimicking thymus organogenesis with sequential regulation of Activin, retinoic acid, BMP, and WNT signals. The hESC-derived TEPLCs expressed the key thymic marker gene FOXN1 and could further develop in vivo into thymic epithelium expressing the functional thymic markers MHC II and AIRE upon transplantation. Moreover, the TEPLC-derived thymic epithelium could support mouse thymopoiesis in T-cell-deficient mice and promote human T cell generation in NOD/SCID mice engrafted with human hematopoietic stem cells (hHSCs). These findings could facilitate hESC-based replacement therapy and provide a valuable in vitro platform for studying human thymus organogenesis and regeneration.
机译:胸腺移植在治疗免疫性疾病方面具有巨大的临床潜力,但移植供体的短缺限制了该疗法的进展。人类胚胎干细胞(hESCs)是产生胸腺上皮细胞的有希望的细胞来源。在这里,我们报告一个逐步的协议,通过模拟激活激活素,视黄酸,BMP和WNT信号的胸腺器官发生,指导hESC分化为胸腺上皮样祖细胞(TEPLCs)。源自hESC的TEPLC表达了关键的胸腺标记基因FOXN1,并且可以在体内进一步发展为在移植后表达功能性胸腺标记MHC II和AIRE的胸腺上皮。此外,TEPLC衍生的胸腺上皮细胞可以支持T细胞缺陷型小鼠的胸腺细胞生成,并在植入了人类造血干细胞(hHSC)的NOD / SCID小鼠体内促进人类T细胞的生成。这些发现可以促进基于hESC的替代疗法,并为研究人类胸腺器官发生和再生提供有价值的体外平台。

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