AI Article Synopsis
- The kidney consists of over 30 specialized cell types essential for maintaining various bodily functions, and defects in its development can lead to chronic kidney disease in children, potentially requiring dialysis or transplants.
- A study investigated gene expression in developing mouse kidneys at a specific embryonic stage, identifying distinct cell types and major compartments through single-cell analysis.
- Findings revealed that specific cell cycle-related genes are differentially expressed in nephron progenitors and immature distal tubules, hinting at their critical roles in nephron patterning and early kidney development processes.
Article Abstract
The kidney is a complex organ composed of more than 30 terminally differentiated cell types that all are required to perform its numerous homeostatic functions. Defects in kidney development are a significant cause of chronic kidney disease in children, which can lead to kidney failure that can only be treated by transplant or dialysis. A better understanding of molecular mechanisms that drive kidney development is important for designing strategies to enhance renal repair and regeneration. In this study, we profiled gene expression in the developing mouse kidney at embryonic day 14.5 at single-cell resolution. Consistent with previous studies, clusters with distinct transcriptional signatures clearly identify major compartments and cell types of the developing kidney. Cell cycle activity distinguishes between the "primed" and "self-renewing" sub-populations of nephron progenitors, with increased expression of the cell cycle-related genes Birc5, Cdca3, Smc2 and Smc4 in "primed" nephron progenitors. In addition, augmented expression of cell cycle related genes Birc5, Cks2, Ccnb1, Ccnd1 and Tuba1a/b was detected in immature distal tubules, suggesting cell cycle regulation may be required for early events of nephron patterning and tubular fusion between the distal nephron and collecting duct epithelia.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8599654 | PMC |
| http://dx.doi.org/10.1038/s41598-021-01790-6 | DOI Listing |
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