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The placenta as a cell source in fetal tissue engineering

Authors
 Amir Kaviani  ;  Tjörvi E. Perry  ;  Carmen M. Barnes  ;  Jung-Tak Oh  ;  Moritz M. Ziegler  ;  Steven J. Fishman  ;  Dario O. Fauza 
Citation
 JOURNAL OF PEDIATRIC SURGERY, Vol.37(7) : 995-999, 2002 
Journal Title
JOURNAL OF PEDIATRIC SURGERY
ISSN
 0022-3468 
Issue Date
2002
MeSH
Cells, Cultured ; Female ; Fetus/chemistry ; Fetus/cytology* ; Fetus/ultrastructure ; Humans ; Immunohistochemistry ; Microscopy, Electron, Scanning ; Placenta/cytology* ; Placentation ; Pregnancy ; TissueEngineering
Keywords
Fetal surgery ; tissue engineering ; placenta ; chorionic villus sampling ; congenital anomalies ; birth defects ; fetus ; prenatal ; neonate ; transplantation
Abstract
Purpose: This study was aimed at determining whether fetal tissue constructs can be engineered from cells derived from the placenta. Methods: A subpopulation of morphologically distinct cells was isolated mechanically from specimens of human placenta (n = 6) and selectively expanded. The lineage of these cells was determined by immunofluorescent staining against multiple intermediate filaments and surface antigens. Cell proliferation rates were determined by oxidation assays and compared with those of immunocytochemically identical cells derived from human amniotic fluid samples (n = 6). Statistical analysis was by analysis of variance (ANOVA). After expansion, the cells were seeded onto a polyglycolic acid polymer/poly-4-hydroxybutyrate scaffold. The resulting construct was analyzed by both optical and scanning electron microscopy. Results: The immunocytochemical profile of expanded placental cells was consistent with a nontrophoblastic, mesenchymal origin. Their proliferation rate in culture was not significantly different when compared with mesenchymal fetal cells isolated from human amniotic fluid; however, it was greater than previously reported rates for similar cells obtained from postnatal or adult tissues. Construct analysis showed dense layers of cells firmly attached to the scaffold without evidence of cell death. Conclusions: Subpopulations of nontrophoblastic, mesenchymal cells can be isolated consistently from the human placenta. These cells proliferate as rapidly as fetal mesenchymal amniocytes in vitro and attach firmly to polyglycolic acid scaffolds. The placenta can be a valuable and practical source of cells for the engineering of select fetal tissue constructs
Full Text
http://www.sciencedirect.com/science/article/pii/S0022346802000118
DOI
10.1053/jpsu.2002.33828
Appears in Collections:
1. College of Medicine (의과대학) > Dept. of Surgery (외과학교실) > 1. Journal Papers
Yonsei Authors
Oh, Jung Tak(오정탁)
URI
https://ir.ymlib.yonsei.ac.kr/handle/22282913/144112
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