Literature DB >> 21963425

Nephron formation adopts a novel spatial topology at cessation of nephrogenesis.

Bree A Rumballe1, Kylie M Georgas, Alexander N Combes, Adler L Ju, Thierry Gilbert, Melissa H Little.   

Abstract

Nephron number in the mammalian kidney is known to vary dramatically, with postnatal renal function directly influenced by nephron complement. What determines final nephron number is poorly understood but nephron formation in the mouse kidney ceases within the first few days after birth, presumably due to the loss of all remaining nephron progenitors via epithelial differentiation. What initiates this event is not known. Indeed, whether nephron formation occurs in the same way at this time as during embryonic development has also not been examined. In this study, we investigate the key cellular compartments involved in nephron formation; the ureteric tip, cap mesenchyme and early nephrons; from postnatal day (P) 0 to 6 in the mouse. High resolution analyses of gene and protein expression indicate that loss of nephron progenitors precedes loss of ureteric tip identity, but show spatial shifts in the expression of cap mesenchyme genes during this time. In addition, cap mesenchymal volume and rate of proliferation decline prior to birth. Section-based 3D modeling and Optical Projection Tomography revealed a burst of ectopic nephron induction, with the formation of multiple (up to 5) nephrons per ureteric tip evident from P2. While the distal-proximal patterning of these nephrons occurred normally, their spatial relationship with the ureteric compartment was altered. We propose that this phase of nephron formation represents an acceleration of differentiation within the cap mesenchyme due to a displacement of signals within the nephrogenic niche. Crown
Copyright © 2011. Published by Elsevier Inc. All rights reserved.

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Year:  2011        PMID: 21963425      PMCID: PMC6186757          DOI: 10.1016/j.ydbio.2011.09.011

Source DB:  PubMed          Journal:  Dev Biol        ISSN: 0012-1606            Impact factor:   3.582


  25 in total

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4.  Epithelial transformation of metanephric mesenchyme in the developing kidney regulated by Wnt-4.

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6.  Human intrauterine renal growth expressed in absolute number of glomeruli assessed by the disector method and Cavalieri principle.

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8.  Fate mapping using Cited1-CreERT2 mice demonstrates that the cap mesenchyme contains self-renewing progenitor cells and gives rise exclusively to nephronic epithelia.

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  78 in total

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Journal:  J Am Soc Nephrol       Date:  2018-12-05       Impact factor: 10.121

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Review 5.  Recreating kidney progenitors from pluripotent cells.

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6.  Directing human embryonic stem cell differentiation towards a renal lineage generates a self-organizing kidney.

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7.  Haploinsufficiency for the Six2 gene increases nephron progenitor proliferation promoting branching and nephron number.

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9.  The Fate of Nephrons in Congenital Obstructive Nephropathy: Adult Recovery is Limited by Nephron Number Despite Early Release of Obstruction.

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Review 10.  A strategy for generating kidney organoids: Recapitulating the development in human pluripotent stem cells.

Authors:  Minoru Takasato; Melissa H Little
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