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Lidské embryonální renální multipotentní progenitory mohou přispět k regeneraci u akutního selhání ledvin
[Regenerative potential of embryonic renal multipotent progenitors in acute renal failure]
Lazzeri E, Crescioli C, Ronconi E, et al.
Jazyk čeština Země Česko
- MeSH
- akutní nemoc MeSH
- antigen CD24 biosyntéza MeSH
- CD antigeny biosyntéza MeSH
- embryo savčí cytologie MeSH
- glykoproteiny biosyntéza MeSH
- kmenové buňky cytologie MeSH
- konfokální mikroskopie MeSH
- ledvinové kanálky metabolismus MeSH
- lidé MeSH
- myši SCID MeSH
- myši MeSH
- nefrony patologie MeSH
- peptidy MeSH
- regenerace MeSH
- renální insuficience metabolismus patologie MeSH
- rhabdomyolýza patologie terapie MeSH
- zvířata MeSH
- Check Tag
- lidé MeSH
- myši MeSH
- zvířata MeSH
Bone marrow-and adult kidney-derived stem/progenitor cells hold promise in the development of therapies for renal failure. Here is reported the identification and characterization of renal multipotent progenitors in human embryonic kidneys that share CD24 and CD133 surface expression with adult renal progenitors and have the capacity for self-renewal and multilineage differentiation. It was found that these CD24+CD133+ cells constitute the early primordial nephron but progressively disappear during nephron development until they become selectively localized to the urinary pole of Bowman's capsule. When isolated and injected into SCID mice with acute renal failure from glycerol-induced rhabdomyolysis, these cells regenerated different portions of the nephron, reduced tissue necrosis and fibrosis, and significantly improved renal function. No tumorigenic potential was observed. It is concluded that CD24+CD133+ cells represent a subset of multipotent embryonic progenitors that persist in human kidneys from early stages of nephrogenesis. The ability of these cells to repair renal damage, together with their apparent lack of tumorigenicity, suggests their potential in the treatment of renal failure.
Regenerative potential of embryonic renal multipotent progenitors in acute renal failure
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- $a Regenerative potential of embryonic renal multipotent progenitors in acute renal failure
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- $a Excellence Center for Research, Transfer and High Education for the Development of DE NOVO THERAPIES, University of Florence, Florence
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- $a Bone marrow-and adult kidney-derived stem/progenitor cells hold promise in the development of therapies for renal failure. Here is reported the identification and characterization of renal multipotent progenitors in human embryonic kidneys that share CD24 and CD133 surface expression with adult renal progenitors and have the capacity for self-renewal and multilineage differentiation. It was found that these CD24+CD133+ cells constitute the early primordial nephron but progressively disappear during nephron development until they become selectively localized to the urinary pole of Bowman's capsule. When isolated and injected into SCID mice with acute renal failure from glycerol-induced rhabdomyolysis, these cells regenerated different portions of the nephron, reduced tissue necrosis and fibrosis, and significantly improved renal function. No tumorigenic potential was observed. It is concluded that CD24+CD133+ cells represent a subset of multipotent embryonic progenitors that persist in human kidneys from early stages of nephrogenesis. The ability of these cells to repair renal damage, together with their apparent lack of tumorigenicity, suggests their potential in the treatment of renal failure.
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