生物
端粒酶
再生医学
诱导多能干细胞
脂肪组织
干细胞
细胞生物学
人口
端粒
遗传学
胚胎干细胞
基因
生物化学
社会学
人口学
作者
Fumitaka Ogura,Shohei Wakao,Yasumasa Kuroda,Kenichiro Tsuchiyama,Mozhdeh Bagheri,Saleh Heneidi,Gregorio D. Chazenbalk,Setsuya Aiba,Mari Dezawa
出处
期刊:Stem Cells and Development
[Mary Ann Liebert, Inc.]
日期:2013-11-20
卷期号:23 (7): 717-728
被引量:155
标识
DOI:10.1089/scd.2013.0473
摘要
In this study, we demonstrate that a small population of pluripotent stem cells, termed adipose multilineage-differentiating stress-enduring (adipose-Muse) cells, exist in adult human adipose tissue and adipose-derived mesenchymal stem cells (adipose-MSCs). They can be identified as cells positive for both MSC markers (CD105 and CD90) and human pluripotent stem cell marker SSEA-3. They intrinsically retain lineage plasticity and the ability to self-renew. They spontaneously generate cells representative of all three germ layers from a single cell and successfully differentiate into targeted cells by cytokine induction. Cells other than adipose-Muse cells exist in adipose-MSCs, however, do not exhibit these properties and are unable to cross the boundaries from mesodermal to ectodermal or endodermal lineages even under cytokine inductions. Importantly, adipose-Muse cells demonstrate low telomerase activity and transplants do not promote teratogenesis in vivo. When compared with bone marrow (BM)- and dermal-Muse cells, adipose-Muse cells have the tendency to exhibit higher expression in mesodermal lineage markers, while BM- and dermal-Muse cells were generally higher in those of ectodermal and endodermal lineages. Adipose-Muse cells distinguish themselves as both easily obtainable and versatile in their capacity for differentiation, while low telomerase activity and lack of teratoma formation make these cells a practical cell source for potential stem cell therapies. Further, they will promote the effectiveness of currently performed adipose-MSC transplantation, particularly for ectodermal and endodermal tissues where transplanted cells need to differentiate across the lineage from mesodermal to ectodermal or endodermal in order to replenish lost cells for tissue repair.
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