Adipose-derived adult stromal cells heal critical-size mouse calvarial defects

被引:0
|
作者
Catherine M Cowan
Yun-Ying Shi
Oliver O Aalami
Yu-Fen Chou
Carina Mari
Romy Thomas
Natalina Quarto
Christopher H Contag
Benjamin Wu
Michael T Longaker
机构
[1] Stanford University School of Medicine,The Department of Surgery
[2] Stanford University,The Department of Bioengineering
[3] University of California,The Department of Radiology, Division of Nuclear Medicine
[4] Los Angeles,The Department of Pediatrics
[5] Stanford University School of Medicine,undefined
[6] Stanford University School of Medicine,undefined
[7] Stanford University,undefined
来源
Nature Biotechnology | 2004年 / 22卷
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摘要
In adults and children over two years of age, large cranial defects do not reossify successfully, posing a substantial biomedical burden. The osteogenic potential of bone marrow stromal (BMS) cells has been documented. This study investigates the in vivo osteogenic capability of adipose-derived adult stromal (ADAS) cells, BMS cells, calvarial-derived osteoblasts and dura mater cells to heal critical-size mouse calvarial defects. Implanted, apatite-coated, PLGA scaffolds seeded with ADAS or BMS cells produced significant intramembranous bone formation by 2 weeks and areas of complete bony bridging by 12 weeks as shown by X-ray analysis, histology and live micromolecular imaging. The contribution of implanted cells to new bone formation was 84–99% by chromosomal detection. These data show that ADAS cells heal critical-size skeletal defects without genetic manipulation or the addition of exogenous growth factors.
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页码:560 / 567
页数:7
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