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骨髓间充质干细胞对聚己内酯、I 型胶原和纳米羟基磷灰石仿生电纺基质的反应。

Mesenchymal stem cell responses to bone-mimetic electrospun matrices composed of polycaprolactone, collagen I and nanoparticulate hydroxyapatite.

机构信息

Department of Physiology and Biophysics, University of Alabama at Birmingham, Birmingham, Alabama, United States of America.

出版信息

PLoS One. 2011 Feb 8;6(2):e16813. doi: 10.1371/journal.pone.0016813.

Abstract

The performance of biomaterials designed for bone repair depends, in part, on the ability of the material to support the adhesion and survival of mesenchymal stem cells (MSCs). In this study, a nanofibrous bone-mimicking scaffold was electrospun from a mixture of polycaprolactone (PCL), collagen I, and hydroxyapatite (HA) nanoparticles with a dry weight ratio of 50/30/20 respectively (PCL/col/HA). The cytocompatibility of this tri-component scaffold was compared with three other scaffold formulations: 100% PCL (PCL), 100% collagen I (col), and a bi-component scaffold containing 80% PCL/20% HA (PCL/HA). Scanning electron microscopy, fluorescent live cell imaging, and MTS assays showed that MSCs adhered to the PCL, PCL/HA and PCL/col/HA scaffolds, however more rapid cell spreading and significantly greater cell proliferation was observed for MSCs on the tri-component bone-mimetic scaffolds. In contrast, the col scaffolds did not support cell spreading or survival, possibly due to the low tensile modulus of this material. PCL/col/HA scaffolds adsorbed a substantially greater quantity of the adhesive proteins, fibronectin and vitronectin, than PCL or PCL/HA following in vitro exposure to serum, or placement into rat tibiae, which may have contributed to the favorable cell responses to the tri-component substrates. In addition, cells seeded onto PCL/col/HA scaffolds showed markedly increased levels of phosphorylated FAK, a marker of integrin activation and a signaling molecule known to be important for directing cell survival and osteoblastic differentiation. Collectively these results suggest that electrospun bone-mimetic matrices serve as promising degradable substrates for bone regenerative applications.

摘要

用于骨修复的生物材料的性能在一定程度上取决于材料支持间充质干细胞(MSCs)黏附和存活的能力。在这项研究中,通过静电纺丝将聚己内酯(PCL)、I 型胶原和纳米羟基磷灰石(HA)以干重比分别为 50/30/20 的比例混合制备出仿生骨纳米纤维支架(PCL/col/HA)。将该三组分支架的细胞相容性与其他三种支架配方进行比较:100%PCL(PCL)、100%胶原 I(col)和含有 80%PCL/20%HA 的双组分支架(PCL/HA)。扫描电子显微镜、荧光活细胞成像和 MTS 检测结果表明,MSCs 能够黏附在 PCL、PCL/HA 和 PCL/col/HA 支架上,但是三组分仿生骨支架上的 MSCs 表现出更快的细胞铺展和显著更高的细胞增殖。相比之下,col 支架不能支持细胞铺展或存活,这可能是由于该材料的拉伸模量较低。与 PCL 或 PCL/HA 相比,PCL/col/HA 支架在体外暴露于血清或植入大鼠胫骨后,能够吸附更多的黏附蛋白,如纤维连接蛋白和纤连蛋白,这可能有助于三组分底物产生有利的细胞反应。此外,接种在 PCL/col/HA 支架上的细胞表现出明显更高水平的磷酸化 FAK,FAK 是整合素激活的标志物,也是一种已知对细胞存活和成骨细胞分化具有重要作用的信号分子。综上所述,静电纺丝仿生基质有望成为用于骨再生应用的有前途的可降解底物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/388e/3035635/deaabd37ea14/pone.0016813.g001.jpg

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