Isolation and Characterization of Multipotent Progenitor Cells from the Bowman’s Capsule of Adult Human Kidneys
Costanza Sagrinati,Giuseppe Stefano Netti,Benedetta Mazzinghi,Elena Lazzeri,Francesco Liotta,Francesca Frosali,Elisa Ronconi,Claudia Meini,Mauro Gacci,Roberta Squecco,Marco Carini,Loreto Gesualdo,Fabio Francini,Enrico Maggi,Francesco Annunziato,Laura Lasagni,Mario Serio,Sergio Romagnani,Paola Romagnani +18 more
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TL;DR: This study demonstrates the existence and provides the characterization of a population of resident multipotent progenitor cells in adult human glomeruli, potentially opening new avenues for the development of regenerative medicine in patients who have renal diseases.
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Abstract: Regenerative medicine represents a critical clinical goal for patients with ESRD, but the identification of renal adult multipotent progenitor cells has remained elusive. It is demonstrated that in human adult kidneys, a subset of parietal epithelial cells (PEC) in the Bowman’s capsule exhibit coexpression of the stem cell markers CD24 and CD133 and of the stem cell–specific transcription factors Oct-4 and BmI-1, in the absence of lineage-specific markers. This CD24 + CD133 + PEC population, which could be purified from cultured capsulated glomeruli, revealed self-renewal potential and a high cloning efficiency. Under appropriate culture conditions, individual clones of CD24 + CD133 + PEC could be induced to generate mature, functional, tubular cells with phenotypic features of proximal and/or distal tubules, osteogenic cells, adipocytes, and cells that exhibited phenotypic and functional features of neuronal cells. The injection of CD24 + CD133 + PEC but not of CD24 − CD133 − renal cells into SCID mice that had acute renal failure resulted in the regeneration of tubular structures of different portions of the nephron. More important, treatment of acute renal failure with CD24 + CD133 + PEC significantly ameliorated the morphologic and functional kidney damage. This study demonstrates the existence and provides the characterization of a population of resident multipotent progenitor cells in adult human glomeruli, potentially opening new avenues for the development of regenerative medicine in patients who have renal diseases.
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Citations
Molecular characterization of the regenerative response induced by intrarenal transplantation of selected renal cells in a rodent model of chronic kidney disease.
Christopher W. Genheimer,Roger M. Ilagan,Thomas E. Spencer,Rusty Kelley,Eric S. Werdin,Sumana Choudhury,Deepak Jain,John W. Ludlow,Joydeep Basu +8 more
TL;DR: Molecular assays that incorporate the assessment of SOX2 and the regenerative response index may prove to be valuable tools for the detection and monitoring of the tissue response after the delivery of regenerative treatments for CKD, thereby significantly shortening the developmental timelines associated with such therapies.
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The Regenerative Potential of the Kidney: What Can We Learn from Developmental Biology?
Franca Anglani,Federica Mezzabotta,Monica Ceol,Rosalba Cristofaro,Dorella Del Prete,Angela D'Angelo +5 more
TL;DR: Developmental biology suggests that this might be particularly true of the kidney and that the papilla might represent the perivascular renal stem cell niche, which fits well with the evolving concept of the stemcell niche as an entity of action.
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The Role of Renal Progenitors in Renal Regeneration
TL;DR: In this review, the existence of renal progenitor cells and their contribution for regeneration of the tubular and the glomerular compartment are discussed, highlighting landmark publications of recent years.
Origin and fate of the regenerating cells of the kidney.
Jennifer Eymael,Bart Smeets +1 more
TL;DR: This review summarises the recent and most important advances in identifying regenerating cell populations of the kidney, and highlights the existing controversies.
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Renal Injury Repair: How About the Role of Stem Cells.
Jian-Si Li,Bing Li +1 more
TL;DR: Stem cell therapy and mechanisms for renal injury repair, including mesenchymal stem cells, HSCs, induced pluripotent stem cells (iPSCs), and nephron progenitor cells (NPCs) are reviewed.
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