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仿生矿化促进灌流生物反应器中人骨髓间充质干细胞的存活和分化。

Biomimetic Mineralization Promotes Viability and Differentiation of Human Mesenchymal Stem Cells in a Perfusion Bioreactor.

机构信息

BioNanoMet Group, Department of Inorganic Chemistry, University of Granada, 18071 Granada, Spain.

IZKF Group Tissue Regeneration in Musculoskeletal Diseases, University Hospital Wuerzburg, 97070 Wuerzburg, Germany.

出版信息

Int J Mol Sci. 2021 Feb 1;22(3):1447. doi: 10.3390/ijms22031447.

Abstract

In bone tissue engineering, the design of 3D systems capable of recreating composition, architecture and micromechanical environment of the native extracellular matrix (ECM) is still a challenge. While perfusion bioreactors have been proposed as potential tool to apply biomechanical stimuli, its use has been limited to a low number of biomaterials. In this work, we propose the culture of human mesenchymal stem cells (hMSC) in biomimetic mineralized recombinant collagen scaffolds with a perfusion bioreactor to simultaneously provide biochemical and biophysical cues guiding stem cell fate. The scaffolds were fabricated by mineralization of recombinant collagen in the presence of magnesium (RCP.MgAp). The organic matrix was homogeneously mineralized with apatite nanocrystals, similar in composition to those found in bone. X-Ray microtomography images revealed isotropic porous structure with optimum porosity for cell ingrowth. In fact, an optimal cell repopulation through the entire scaffolds was obtained after 1 day of dynamic seeding in the bioreactor. Remarkably, RCP.MgAp scaffolds exhibited higher cell viability and a clear trend of up-regulation of osteogenic genes than control (non-mineralized) scaffolds. Results demonstrate the potential of the combination of biomimetic mineralization of recombinant collagen in presence of magnesium and dynamic culture of hMSC as a promising strategy to closely mimic bone ECM.

摘要

在骨组织工程中,设计能够重现天然细胞外基质 (ECM) 的组成、结构和微机械环境的 3D 系统仍然是一个挑战。虽然灌注生物反应器已被提议作为施加生物力学刺激的潜在工具,但它的使用仅限于少数几种生物材料。在这项工作中,我们提出了在灌注生物反应器中培养人骨髓间充质干细胞 (hMSC) 仿生矿化重组胶原支架,以同时提供指导干细胞命运的生化和生物物理线索。支架通过在镁存在下对重组胶原蛋白进行矿化来制备(RCP.MgAp)。有机基质均匀矿化为与骨中相似的磷灰石纳米晶体。X 射线微断层扫描图像显示具有适合细胞生长的最佳孔隙率的各向同性多孔结构。事实上,在生物反应器中进行 1 天的动态接种后,整个支架中获得了最佳的细胞再定植。值得注意的是,RCP.MgAp 支架的细胞活力更高,且成骨基因的上调趋势明显高于对照(未矿化)支架。结果表明,在镁存在下仿生矿化重组胶原蛋白与 hMSC 动态培养的结合具有作为一种很有前途的策略来紧密模拟骨 ECM。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/795d/7867135/36154aec3c2e/ijms-22-01447-g001.jpg

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