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Intrinsic Epithelial Cells Repair the Kidney After Injury

Overview
Journal Cell Stem Cell
Publisher Cell Press
Specialty Cell Biology
Date 2008 Mar 29
PMID 18371453
Citations 424
Authors
Benjamin D Humphreys
M Todd Valerius
Akio Kobayashi
Joshua W Mugford
Savuth Soeung
Jeremy S Duffield
Andrew P McMahon
Joseph V Bonventre
Affiliations
Soon will be listed here.
Abstract

Understanding the mechanisms of nephron repair is critical for the design of new therapeutic approaches to treat kidney disease. The kidney can repair after even a severe insult, but whether adult stem or progenitor cells contribute to epithelial renewal after injury and the cellular origin of regenerating cells remain controversial. Using genetic fate-mapping techniques, we generated transgenic mice in which 94%-95% of tubular epithelial cells, but no interstitial cells, were labeled with either beta-galactosidase (lacZ) or red fluorescent protein (RFP). Two days after ischemia-reperfusion injury (IRI), 50.5% of outer medullary epithelial cells coexpress Ki67 and RFP, indicating that differentiated epithelial cells that survived injury undergo proliferative expansion. After repair was complete, 66.9% of epithelial cells had incorporated BrdU, compared to only 3.5% of cells in the uninjured kidney. Despite this extensive cell proliferation, no dilution of either cell-fate marker was observed after repair. These results indicate that regeneration by surviving tubular epithelial cells is the predominant mechanism of repair after ischemic tubular injury in the adult mammalian kidney.

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