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评估骨髓和基质中的氧气张力对于二维和三维仿生层状支架中 MSC 分化的影响。

Evaluating Oxygen Tensions Related to Bone Marrow and Matrix for MSC Differentiation in 2D and 3D Biomimetic Lamellar Scaffolds.

机构信息

Department of Biotechnology, Middle East Technical University, 06800 Ankara, Turkey.

Department of Tissue Engineering, University of Health Sciences, 34668 Istanbul, Turkey.

出版信息

Int J Mol Sci. 2021 Apr 13;22(8):4010. doi: 10.3390/ijms22084010.

Abstract

The physiological O microenvironment of mesenchymal stem cells (MSCs) and osteoblasts and the dimensionality of a substrate are known to be important in regulating cell phenotype and function. By providing the physiologically normoxic environments of bone marrow (5%) and matrix (12%), we assessed their potential to maintain stemness, induce osteogenic differentiation, and enhance the material properties in the micropatterned collagen/silk fibroin scaffolds that were produced in 2D or 3D. Expression of osterix (OSX) and vascular endothelial growth factor A (VEGFA) was significantly enhanced in the 3D scaffold in all oxygen environments. At 21% O, OSX and VEGFA expressions in the 3D scaffold were respectively 13,200 and 270 times higher than those of the 2D scaffold. Markers for assessing stemness were significantly more pronounced on tissue culture polystyrene and 2D scaffold incubated at 5% O. At 21% O, we measured significant increases in ultimate tensile strength ( < 0.0001) and Young's modulus ( = 0.003) of the 3D scaffold compared to the 2D scaffold, whilst 5% O hindered the positive effect of cell seeding on tensile strength. In conclusion, we demonstrated that the 3D culture of MSCs in collagen/silk fibroin scaffolds provided biomimetic cues for bone progenitor cells toward differentiation and enhanced the tensile mechanical properties.

摘要

骨髓(5%)和基质(12%)的生理低氧环境以及基质的维度已知可调节细胞表型和功能。我们通过提供这些生理低氧环境来评估它们在维持干细胞特性、诱导成骨分化以及增强 2D 或 3D 微图案胶原/丝素纤维支架材料性能方面的潜力。在所有氧气环境中,3D 支架中的osterix(OSX)和血管内皮生长因子 A(VEGFA)的表达均显著增强。在 21%O 下,3D 支架中 OSX 和 VEGFA 的表达分别比 2D 支架高 13200 倍和 270 倍。在 5%O 下孵育的组织培养聚苯乙烯和 2D 支架上,用于评估干细胞特性的标志物更为明显。与 2D 支架相比,3D 支架的极限拉伸强度(<0.0001)和杨氏模量(=0.003)在 21%O 下显著增加,而 5%O 则阻碍了细胞接种对拉伸强度的积极影响。总之,我们证明了 MSC 在胶原/丝素纤维支架中的 3D 培养为成骨前体细胞提供了向分化的仿生线索,并增强了拉伸力学性能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ab45/8068918/fae64fedea12/ijms-22-04010-g001.jpg

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