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Cross-platform single cell analysis of kidney development shows stromal cells express Gdnf

机译:肾脏发育的跨平台单细胞分析显示基质细胞表达Gdnf

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摘要

The developing kidney provides a useful model for study of the principles of organogenesis. In this report we use three independent platforms, Drop-Seq, Chromium 10x Genomics and Fluidigm C1, to carry out single cell RNA-Seq (scRNA-Seq) analysis of the E14.5 mouse kidney. Using the software AltAnalyze, in conjunction with the unsupervised approach ICGS, we were unable to identify and confirm the presence of 16 distinct cell populations during this stage of active nephrogenesis. Using a novel integrative supervised computational strategy, we were able to successfully harmonize and compare the cell profiles across all three technological platforms. Analysis of possible cross compartment receptor/ligand interactions identified the nephrogenic zone stroma as a source of GDNF. This was unexpected because the cap mesenchyme nephron progenitors had been thought to be the sole source of GDNF, which is a key driver of branching morphogenesis of the collecting duct system. The expression of Gdnf by stromal cells was validated in several ways, including Gdnf in situ hybridization combined with immunohistochemistry for SIX2, and marker of nephron progenitors, and MEIS1, a marker of stromal cells. Finally, the single cell gene expression profiles generated in this study confirmed and extended previous work showing the presence of multilineage priming during kidney development. Nephron progenitors showed stochastic expression of genes associated with multiple potential differentiation lineages.
机译:发育中的肾脏为研究器官发生原理提供了有用的模型。在本报告中,我们使用三个独立的平台Drop-Seq,Chromium 10x Genomics和Fluidigm C1对E14.5小鼠肾脏进行单细胞RNA-Seq(scRNA-Seq)分析。使用软件AltAnalyze结合无监督方法ICGS,我们无法在活跃的肾生成此阶段识别和确认16种不同细胞群的存在。使用一种新颖的集成监督计算策略,我们能够成功地协调和比较所有三个技术平台上的单元格概况。对可能的跨区受体/配体相互作用的分析确定了肾原性区基质是GDNF的来源。这是出乎意料的,因为帽间充质肾单位祖细胞被认为是GDNF的唯一来源,而GDNF是收集管系统分支形态发生的关键驱动力。用多种方法验证了基质细胞中Gdnf的表达,包括Gdnf原位杂交结合免疫组化的SIX2,肾单位祖细胞标志物和MEIS1(基质细胞标志物)。最后,在这项研究中产生的单细胞基因表达谱证实并扩展了先前的工作,显示了肾脏发育过程中多谱系引发的存在。 Nephron祖细胞显示与多种潜在分化谱系相关的基因的随机表达。

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