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一种基于钙和磷酸根离子诱导人间充质干细胞球状体矿化的模型系统。

An model system based on calcium- and phosphate ion-induced hMSC spheroid mineralization.

作者信息

Vermeulen Steven, Knoops Kèvin, Duimel Hans, Parvizifard Maryam, van Beurden Denis, López-Iglesias Carmen, Giselbrecht Stefan, Truckenmüller Roman, Habibović Pamela, Tahmasebi Birgani Zeinab

机构信息

Department of Instructive Biomaterials Engineering, MERLN Institute for Technology-Inspired Regenerative Medicine, Maastricht University, Maastricht, the Netherlands.

Microscopy CORE Lab, M4I Faculty of Health, Medicine and Life Sciences, Maastricht University, Maastricht, the Netherlands.

出版信息

Mater Today Bio. 2023 Nov 7;23:100844. doi: 10.1016/j.mtbio.2023.100844. eCollection 2023 Dec.

Abstract

A challenge in regenerative medicine is creating the three-dimensional organic and inorganic microenvironment of bone, which would allow the study of musculoskeletal disorders and the generation of building blocks for bone regeneration. This study presents a microwell-based platform for creating spheroids of human mesenchymal stromal cells, which are then mineralized using ionic calcium and phosphate supplementation. The resulting mineralized spheroids promote an osteogenic gene expression profile through the influence of the spheroids' biophysical environment and inorganic signaling and require less calcium or phosphate to achieve mineralization compared to a monolayer culture. We found that mineralized spheroids represent an model for studying small molecule perturbations and extracellular mediated calcification. Furthermore, we demonstrate that understanding pathway signaling elicited by the spheroid environment allows mimicking these pathways in traditional monolayer culture, enabling similar rapid mineralization events. In sum, this study demonstrates the rapid generation and employment of a mineralized cell model system for regenerative medicine applications.

摘要

再生医学面临的一个挑战是创建骨骼的三维有机和无机微环境,这将有助于研究肌肉骨骼疾病并生成用于骨再生的构建模块。本研究提出了一种基于微孔的平台,用于创建人骨髓间充质基质细胞球体,然后通过补充离子钙和磷酸盐使其矿化。所得的矿化球体通过球体的生物物理环境和无机信号传导的影响促进成骨基因表达谱,并且与单层培养相比,实现矿化所需的钙或磷酸盐更少。我们发现矿化球体代表了一种研究小分子扰动和细胞外介导钙化的模型。此外,我们证明,了解球体环境引发的信号通路可以在传统单层培养中模拟这些通路,从而实现类似的快速矿化事件。总之,本研究展示了一种用于再生医学应用的矿化细胞模型系统的快速生成和应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8a3e/10682137/b3ff58c52849/ga1.jpg

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