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成脂预分化的人骨髓间充质干细胞的成骨潜能在骨组织工程中的应用。

Osteogenic potential of adipogenic predifferentiated human bone marrow-derived multipotent stromal cells for bone tissue-engineering.

机构信息

UMR 7052 CNRS University Paris Diderot, Sorbonne Paris Cité, Paris, France.

出版信息

J Tissue Eng Regen Med. 2018 Mar;12(3):e1511-e1524. doi: 10.1002/term.2571. Epub 2017 Nov 28.

DOI:10.1002/term.2571
PMID:28875591
Abstract

In the present study, we evaluated the benefits of an adipogenic predifferentiation, the pathway most closely related to osteoblastogenesis, on the pro-osteogenic potential of human adult multipotent bone marrow stromal cells (hBMSCs), both in vitro and in vivo. Adipogenic differentiation of hBMSCs for 14 days resulted in a heterogeneous cell population from which the most adipogenic-committed cells were eliminated by their lack of readhesion ability. Our results provided evidence that the select adherent adipogenic differentiated hBMSCs (sAD+ cells) express a gene profile characteristic of both adipogenic and osteogenic lineages. In vitro, when cultured in osteogenic medium, sAD+ differentiated along the osteogenic lineage faster than undifferentiated hBMSCs. In vivo, in an ectopic mouse model, sAD+ exhibited a significantly higher bone formation capability compared with undifferentiated hBMSCs. We sought, then, to investigate the underlying mechanisms responsible for such beneficial effects of adipogenic predifferentiation on bone formation and found that this outcome was not linked to a better cell survival post-implantation. The secretome of sAD+ was both proangiogenic and chemoattractant, but its potential did not supersede the one of undifferentiated hBMSCs. However, using co-culture systems, we observed that the sAD+ paracrine factors were pro-osteogenic on undifferentiated hBMSCs. In conclusion, adipogenic priming endows hBMSCs with high osteogenic potential as well as pro-osteogenic paracrine-mediated activity. This preconditioning appears as a promising strategy for bone tissue engineering technology in order to improve the hBMSC osteogenic potency in vivo.

摘要

在本研究中,我们评估了脂肪形成预分化(与成骨细胞形成最密切相关的途径)对人成年多能骨髓基质细胞(hBMSCs)体外和体内前成骨潜能的益处。hBMSCs 经过 14 天的脂肪分化,形成了一个异质细胞群体,其中最具脂肪分化潜能的细胞由于缺乏黏附能力而被淘汰。我们的结果表明,选择黏附的脂肪分化 hBMSCs(sAD+细胞)表达了具有成脂和成骨谱系特征的基因谱。在体外,当在成骨培养基中培养时,sAD+细胞比未分化的 hBMSCs 更快地沿着成骨谱系分化。在体内,在异位小鼠模型中,sAD+细胞的骨形成能力明显高于未分化的 hBMSCs。因此,我们试图研究脂肪形成预分化对骨形成有益影响的潜在机制,发现这种结果与植入后细胞的更好存活无关。sAD+的分泌组具有促血管生成和趋化作用,但它的潜力并没有超过未分化的 hBMSCs。然而,使用共培养系统,我们观察到 sAD+的旁分泌因子对未分化的 hBMSCs 具有促成骨作用。总之,脂肪形成预分化赋予了 hBMSCs 高成骨潜能和促成骨旁分泌介导的活性。这种预处理似乎是一种很有前途的骨组织工程技术策略,可提高 hBMSC 在体内的成骨潜能。

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