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人胚胎干细胞在人骨髓基质细胞微环境中发生成骨分化。

Human Embryonic Stem Cells Undergo Osteogenic Differentiation in Human Bone Marrow Stromal Cell Microenvironments.

作者信息

Tong Wilbur, Brown Shelley E, Krebsbach Paul H

机构信息

Biologic and Materials Sciences, University of Michigan School of Dentistry, Ann Arbor, MI 48109.

出版信息

J Stem Cells. 2007;2(3):139-147.

Abstract

Human embryonic stem cells (hESCs) may offer an unlimited supply of cells that can be directed to differentiate into all cell types within the body and used in regenerative medicine for tissue and cell replacement therapies. Previous work has shown that exposing hESCs to exogenous factors such as dexamethasone, ascorbic acid and β-glycerophosphate can induce osteogenesis. The specific factors that induce osteogenic differentiation of hESCs have not been identified yet, however, it is possible that differentiated human bone marrow stromal cells (hMBSCs) may secrete factors within the local microenvironment that promote osteogenesis. Here we report that the lineage progression of hESCs to osteoblasts is achieved in the presence of soluble signaling factors derived from differentiated hBMSCs. For 28 days, hESCs were grown in a transwell co-culture system with hBMSCs that had been previously differentiated in growth medium containing defined osteogenic supplements for 7-24 days. As a control. hESCs were co-cultured with undifferentiated hBMSCs and alone. Von Kossa and Alizarin Red staining as well as immunohistochemistry confirmed that the hESCs co-cultured with differentiated hBMSCs formed mineralized bone nodules and secreted extracellular matrix protein osteocalcin (OCN). Quantitative Alizarin Red assays showed increased mineralization as compared to the control with undifferentiated hBMSCs. RT-PCR revealed the loss of pluripotent hESC markers with the concomitant gain of osteoblastic markers such as collagen type I, runx2, and osterix. We demonstrate that osteogenic growth factors derived from differentiated hBMSCs within the local microenvironment may help to promote hESC osteogenic differentiation.

摘要

人胚胎干细胞(hESCs)可能提供无限的细胞供应,这些细胞可被定向分化为体内所有细胞类型,并用于再生医学中的组织和细胞替代疗法。先前的研究表明,将hESCs暴露于地塞米松、抗坏血酸和β-甘油磷酸等外源性因子可诱导成骨。然而,尚未确定诱导hESCs成骨分化的具体因子,不过,分化的人骨髓基质细胞(hMBSCs)可能在局部微环境中分泌促进成骨的因子。在此我们报告,在存在源自分化的hBMSCs的可溶性信号因子的情况下,hESCs可向成骨细胞进行谱系进展。hESCs在Transwell共培养系统中与先前在含有特定成骨补充剂的生长培养基中分化7 - 24天的hBMSCs一起培养28天。作为对照,hESCs与未分化的hBMSCs共培养以及单独培养。冯科萨染色和茜素红染色以及免疫组织化学证实,与分化的hBMSCs共培养的hESCs形成了矿化骨结节并分泌细胞外基质蛋白骨钙素(OCN)。定量茜素红测定显示,与未分化hBMSCs的对照相比,矿化增加。逆转录聚合酶链反应(RT-PCR)显示多能hESC标志物丢失,同时成骨标志物如I型胶原、runx2和osterix增加。我们证明,局部微环境中源自分化的hBMSCs的成骨生长因子可能有助于促进hESC成骨分化。

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