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High-resolution gene expression analysis of the developing mouse kidney defines novel cellular compartments within the nephron progenitor population.

机译:发育中的小鼠肾脏的高分辨率基因表达分析定义了肾单位祖细胞内的新型细胞区室。

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摘要

The functional unit of the kidney is the nephron. During its organogenesis, the mammalian metanephric kidney generates thousands of nephrons over a protracted period of fetal life. All nephrons are derived from a population of self-renewing multi-potent progenitor cells, termed the cap mesenchyme. However, our understanding of the molecular and cellular mechanisms underlying nephron development is at an early stage. In order to identify factors involved in nephrogenesis, we performed a high-resolution, spatial profiling of a number of transcriptional regulators expressed within the cap mesenchyme and early developing nephron. Our results demonstrate novel, stereotypic, spatially defined cellular sub-domains within the cap mesenchyme, which may, in part, reflect induction of nephron precursors. These results suggest a hitherto unappreciated complexity of cell states that accompany the assembly of the metanephric kidney, likely reflecting diverse regulatory actions such as the maintenance and induction of nephron progenitors.
机译:肾脏的功能单位是肾单位。在其器官发生过程中,哺乳动物后肾在胎儿生命的延长期内会产生数千个肾单位。所有肾单位均来自自我更新的多能祖细胞群,称为帽间充质。但是,我们对肾单位发展的分子和细胞机制的了解还处于早期阶段。为了鉴定参与肾发生的因素,我们对帽间充质和早期发展的肾单位内表达的许多转录调节子进行了高分辨率的空间分析。我们的研究结果表明帽间充质内新颖,刻板,空间定义的细胞亚域,这可能部分反映肾单位前体的诱导。这些结果表明,迄今为止,未认识到的后肾肾脏组装所伴随的细胞状态复杂性,可能反映了多种调节作用,例如维持和诱导肾单位祖细胞。

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