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工程化血管化骨:鼠骨膜细胞的成骨和成血管潜能。

Engineering vascularized bone: osteogenic and proangiogenic potential of murine periosteal cells.

机构信息

Laboratory of Clinical and Experimental Endocrinology, Division of Skeletal Tissue Engineering, KU Leuven, Leuven, Belgium.

出版信息

Stem Cells. 2012 Nov;30(11):2460-71. doi: 10.1002/stem.1210.

DOI:10.1002/stem.1210
PMID:22911908
Abstract

One of the key challenges in bone tissue engineering is the timely formation of blood vessels that promote the survival of the implanted cells in the construct. Fracture healing largely depends on the presence of an intact periosteum but it is still unknown whether periosteum-derived cells (PDC) are critical for bone repair only by promoting bone formation or also by inducing neovascularization. We first established a protocol to specifically isolate murine PDC (mPDC) from long bones of adult mice. Mesenchymal stem cells were abundantly present in this cell population as more than 50% of the mPDC expressed mesenchymal markers (CD73, CD90, CD105, and stem cell antigen-1) and the cells exhibited trilineage differentiation potential (chondrogenic, osteogenic, and adipogenic). When transplanted on a collagen-calcium phosphate scaffold in vivo, mPDC attracted numerous blood vessels and formed mature bone which comprises a hematopoiesis-supportive stroma. We explored the proangiogenic properties of mPDC using in vitro culture systems and showed that mPDC promote the survival and proliferation of endothelial cells through the production of vascular endothelial growth factor. Coimplantation with endothelial cells demonstrated that mPDC can enhance vasculogenesis by adapting a pericyte-like phenotype, in addition to their ability to stimulate blood vessel ingrowth from the host. In conclusion, these findings demonstrate that periosteal cells contribute to fracture repair, not only through their strong osteogenic potential but also through their proangiogenic features and thus provide an ideal cell source for bone regeneration therapies.

摘要

在骨组织工程学中,一个关键的挑战是及时形成血管,以促进植入细胞在构建体中的存活。骨折愈合在很大程度上取决于完整的骨膜的存在,但目前尚不清楚骨膜来源的细胞(PDC)是否仅通过促进骨形成,还是通过诱导血管新生,对骨修复至关重要。我们首先建立了一个从成年小鼠长骨中特异性分离小鼠 PDC(mPDC)的方案。间充质干细胞在该细胞群体中大量存在,因为超过 50%的 mPDC 表达间充质标记物(CD73、CD90、CD105 和干细胞抗原-1),并且细胞表现出三系分化潜能(软骨形成、成骨和脂肪形成)。当在体内移植到胶原-磷酸钙支架上时,mPDC 吸引了大量的血管,并形成了成熟的骨骼,其中包含造血支持的基质。我们使用体外培养系统探索了 mPDC 的促血管生成特性,并表明 mPDC 通过产生血管内皮生长因子促进内皮细胞的存活和增殖。与内皮细胞共植入表明,mPDC 除了能够刺激宿主血管向内生长之外,还可以通过适应周细胞样表型来增强血管生成。总之,这些发现表明,骨膜细胞不仅通过其强大的成骨潜能,而且还通过其促血管生成特性,有助于骨折修复,因此为骨再生治疗提供了理想的细胞来源。

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