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Fate mapping using Cited1-CreERT2 mice demonstrates that the cap mesenchyme contains self-renewing progenitor cells and gives rise exclusively to nephronic epithelia

机译:使用Cited1-CreERT2小鼠的命运图谱显示帽间充质包含自我更新的祖细胞并且仅产生肾上皮

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摘要

Classic tissue recombination and in vitro lineage tracing studies suggest that condensed metanephric mesenchyme (MM) gives rise to nephronic epithelium of the adult kidney. However, these studies do not distinguish between cap mesenchyme and pre-tubular aggregates comprising the condensed MM, nor do they establish whether these cells have self-renewing capacity. To address these questions, we generated Cited1-CreERT2 BAC transgenic mice, which express tamoxifen-regulated Cre recombinase exclusively in the cap mesenchyme. Fate mapping was performed by crossing these mice with the Rosa26RLacZ reporter line and evaluating the location and cellular characteristics of LacZ positive cells at different time points following tamoxifen injection. These studies confirmed expected results from previous in vitro analysis of MM cell fate, and provide in vivo evidence that the cap mesenchyme does not contribute to collecting duct epithelium in the adult. Furthermore, by exploiting the temporally regulated Cre recombinase, these studies show that nephronic epithelium arising at different stages of nephrogenesis has distinct spatial distribution in the adult kidney, and demonstrate for the first time that the cap mesenchyme includes a population of self-renewing epithelial progenitor cells.
机译:经典的组织重组和体外谱系追踪研究表明,浓缩的后肾间质(MM)会引起成年肾的肾上皮。但是,这些研究没有区分帽间充质和构成浓缩MM的肾小管前聚集体,也没有确定这些细胞是否具有自我更新能力。为了解决这些问题,我们产生了Cited1-CreER T2 BAC转基因小鼠,该小鼠仅在帽间充质中表达他莫昔芬调节的Cre重组酶。通过将这些小鼠与Rosa26R LacZ 报告基因系杂交并评估他莫昔芬注射后不同时间点的LacZ阳性细胞的位置和细胞特性,进行命运作图。这些研究证实了先前对MM细胞命运的体外分析的预期结果,并提供了体内的证据,即帽间充质在成人中无助于收集导管上皮。此外,通过利用时间调控的Cre重组酶,这些研究表明,在肾生成的不同阶段出现的肾上皮在成年肾脏中具有独特的空间分布,并首次证明帽间充质包括自我更新的上皮祖细胞群。细胞。

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