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Embryonální kmenové buňky se množí a diferencují v ledvinách zbavených vlastních buněk - cesta k získání imunologicky shodných štěpů pro transplantaci ledviny?
[Embryonic stem cells proliferate and differentiate when seeded into kidney scaffolds]
Ross EA, Williams MJ, Hamazaki T, et al.
Jazyk čeština Země Česko
- MeSH
- buněčná diferenciace MeSH
- embryonální kmenové buňky cytologie MeSH
- financování organizované MeSH
- krysa rodu rattus MeSH
- kultivované buňky MeSH
- ledviny MeSH
- potkani Sprague-Dawley MeSH
- proliferace buněk MeSH
- tkáňové podpůrné struktury MeSH
- zvířata MeSH
- Check Tag
- krysa rodu rattus MeSH
- mužské pohlaví MeSH
- zvířata MeSH
The scarcity of transplant allografts for diseased organs has prompted efforts at tissue regeneration using seeded scaffolds, an approach hampered by the enormity of cell types and complex architectures. Our goal was to decellularize intact organs in a manner that retained the matrix signal for differentiating pluripotent cells. We decellularized intact rat kidneys in a manner that preserved the intricate architecture and seeded them with pluripotent murine embryonic stem cells antegrade through the artery or retrograde through the ureter. Primitive precursor cells populated and proliferated within the glomerular, vascular, and tubular structures. Cells lost their embryonic appearance and expressed immunohistochemical markers for differentiation. Cells not in contact with the basement membrane matrix became apoptotic, thereby forming lumens. These observations suggest that the extracellular matrix can direct regeneration of the kidney, and studies using seeded scaffolds may help define differentiation pathways.
Embryonic stem cells proliferate and differentiate when seeded into kidney scaffolds
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- $a Embryonic stem cells proliferate and differentiate when seeded into kidney scaffolds
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- $a Division of Nephrology, Hypertension and Transplantation, University of Florida, Gainesville
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- $a The scarcity of transplant allografts for diseased organs has prompted efforts at tissue regeneration using seeded scaffolds, an approach hampered by the enormity of cell types and complex architectures. Our goal was to decellularize intact organs in a manner that retained the matrix signal for differentiating pluripotent cells. We decellularized intact rat kidneys in a manner that preserved the intricate architecture and seeded them with pluripotent murine embryonic stem cells antegrade through the artery or retrograde through the ureter. Primitive precursor cells populated and proliferated within the glomerular, vascular, and tubular structures. Cells lost their embryonic appearance and expressed immunohistochemical markers for differentiation. Cells not in contact with the basement membrane matrix became apoptotic, thereby forming lumens. These observations suggest that the extracellular matrix can direct regeneration of the kidney, and studies using seeded scaffolds may help define differentiation pathways.
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