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Thymic crosstalk restrains the pool of cortical thymic epithelial cells with progenitor properties

机译:胸腺串扰抑制皮质的池胸腺上皮细胞与祖属性

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Cortical (cTEC) and medullary (mTEC) thymic epithelial cells establish key microenvironments for T-cell differentiation and arise from thymic epithelial cell progenitors (TEP). However, the nature of TEPs and the mechanism controlling their stemness in the postnatal thymus remain poorly defined. Using TEC clonogenic assays as a surrogate to survey TEP activity, we found that a fraction of cTECs generates specialized clonal-derived colonies, which contain cells with sustained colony-forming capacity (ClonoTECs). These ClonoTECs are EpCAM+MHCII-Foxn1lo cells that lack traits of mature cTECs or mTECs but co-express stem-cell markers, including CD24 and Sca-1. Supportive of their progenitor identity, ClonoTECs reintegrate within native thymic microenvironments and generate cTECs or mTECs in vivo. Strikingly, the frequency of cTECs with the potential to generate ClonoTECs wanes between the postnatal and young adult immunocompetent thymus, but it is sustained in alymphoid Rag2-/-Il2rg-/- counterparts. Conversely, transplantation of wild-type bone marrow hematopoietic progenitors into Rag2-/-Il2rg-/- mice and consequent restoration of thymocyte-mediated TEC differentiation diminishes the frequency of colony-forming units within cTECs. Our findings provide evidence that the cortical epithelium contains a reservoir of epithelial progenitors whose abundance is dynamically controlled by continual interactions with developing thymocytes across lifespan.
机译:大脑皮层(cTEC)和髓(mTEC)胸腺上皮细胞建立关键的微环境从胸腺t细胞分化而产生上皮细胞祖细胞(TEP)。tep中的性质和控制机制他们在产后胸腺仍然具备干细胞差的定义。代理TEP调查活动,我们发现一个一部分cTECs生成专业clonal-derived殖民地,含有细胞持续的克隆形成能力(ClonoTECs)。这些ClonoTECs EpCAM + MHCII-Foxn1lo细胞缺乏成熟的cTECs特征或mTECs但co-express干细胞标记,包括CD24和本来。在本机胸腺ClonoTECs重建微环境并生成cTECs或mTECsvivo之间可能产生ClonoTECs减弱产后和年轻成人免疫活性的胸腺,但它持续在alymphoid Rag2 - / -Il2rg - / -同行。野生型骨髓造血祖细胞Rag2——/ -Il2rg - / -小鼠和结果恢复thymocyte-mediated TEC差异化的频率减少在cTECs菌落。提供证据表明皮层上皮包含一个储层上皮细胞的祖细胞丰富的动态控制的吗持续与发展中胸腺细胞的相互作用在寿命。

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