| Literature DB >> 30257215 |
Ping Wang1, Yidong Chen2, Jun Yong3, Yueli Cui1, Rui Wang1, Lu Wen1, Jie Qiao4, Fuchou Tang5.
Abstract
Healthy renal function depends on normal nephrogenesis during embryonic development. However, a comprehensive gene expression profile of human fetal kidney development remains largely unexplored. Here, using a single-cell RNA-sequencing technique, we analyzed >3,000 human fetal renal cells spanning 4 months of development in utero. Unsupervised analysis identified two progenitor subtypes during cap mesenchyme development, suggesting a mechanism for sustaining their progenitor states. Furthermore, we identified critical transcriptional regulators and signaling pathways involved in the segmentation of nephron tubules. We explored the development of the highly heterogeneous collecting duct epithelia and dissected the metabolic gene repertoire and the extracellular matrix composition of the glomerular mesangium. The results provide insights on the molecular basis and regulatory events in human renal development. Moreover, the cell-type-specific expression features of causal genes in congenital renal diseases may be helpful in the treatment of these diseases.Entities:
Keywords: STRT; congenital renal diseases; human fetal kidney development; nephron progenitors; nephron tubule segmentation; single cell transcriptome analysis; single-cell RNA-seq
Year: 2018 PMID: 30257215 DOI: 10.1016/j.celrep.2018.08.056
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423