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高表达水平的 EphrinB2 可促进人骨髓间充质干细胞的成骨分化,并在聚乙烯亚胺-EphrinB2 基因激活基质中促进增强的细胞介导矿化。

High levels of ephrinB2 over-expression increases the osteogenic differentiation of human mesenchymal stem cells and promotes enhanced cell mediated mineralisation in a polyethyleneimine-ephrinB2 gene-activated matrix.

机构信息

Tissue Engineering Research Group, Department of Anatomy, Royal College of Surgeons in Ireland, Dublin, Ireland.

出版信息

J Control Release. 2013 Feb 10;165(3):173-82. doi: 10.1016/j.jconrel.2012.11.013. Epub 2012 Nov 29.

DOI:10.1016/j.jconrel.2012.11.013
PMID:23201622
Abstract

Gene therapy can be combined with tissue engineering constructs to produce gene-activated matrices (GAMs) with enhanced capacity for repair. Polyethyleneimine (PEI), a non-viral vector, has previously been optimised for high efficiency gene transfer in rat mesenchymal stem cells (rMSCs). The use of PEI to transfect human MSCs (hMSCs) with ephrinB2 is assessed here. Recently a role for the ephrinB2 ligand and EphB4 receptor duo has been proposed in bone remodelling. Herein, over-expression of the ephrinB2 ligand resulted in increased osteogenic differentiation in hMSCs. As ephrinB2 is a cell surface anchored ligand which only interacts with cells expressing the cognate EphB4 receptor through direct contact, we have shown that direct cell-cell contact between two neighbouring cells is responsible for enhanced osteogenesis. In an effort to begin to elucidate the molecular mechanisms at play downstream of ephrinB2 over-expression, RT-PCR was performed on the GAMs which revealed no significant changes in runx2 or BMP2 expression but an upregulation of osterix (Osx) and Dlx5 expression prompting the belief that the mode of osteogenesis is independent of the BMP2 pathway. This select interaction, coupled with the transient gene expression profile of PEI, makes the PEI-ephrinB2 GAM an ideal candidate matrix for a bone targeted GAM.

摘要

基因治疗可以与组织工程构建体结合,以产生具有增强修复能力的基因激活基质(GAM)。聚乙烯亚胺(PEI)是一种非病毒载体,以前已经过优化,可实现大鼠间充质干细胞(rMSCs)中的高效基因转移。本文评估了使用 PEI 转染人骨髓间充质干细胞(hMSCs)的 EphrinB2。最近,EphrinB2 配体和 EphB4 受体对的作用已被提出在骨重塑中。在此,EphrinB2 配体的过表达导致 hMSCs 中成骨分化增加。由于 EphrinB2 是一种细胞表面锚定配体,只能通过直接接触与表达同源 EphB4 受体的细胞相互作用,我们已经表明,两个相邻细胞之间的直接细胞-细胞接触负责增强成骨作用。为了开始阐明 EphrinB2 过表达下游发挥作用的分子机制,对 GAMs 进行了 RT-PCR 分析,结果显示,Runx2 或 BMP2 的表达没有明显变化,但osterix(Osx)和 Dlx5 的表达上调提示我们相信成骨作用的模式独立于 BMP2 途径。这种选择性相互作用,加上 PEI 的瞬时基因表达谱,使得 PEI-EphrinB2 GAM 成为骨靶向 GAM 的理想候选基质。

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