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首页> 外文期刊>Annals of anatomy =: Anatomischer Anzeiger : official organ of the Anatomische Gesellschaft >Effect of ascorbic and chondrogenic derived decellularized extracellular matrix from mesenchymal stem cells on their proliferation, viability and differentiation
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Effect of ascorbic and chondrogenic derived decellularized extracellular matrix from mesenchymal stem cells on their proliferation, viability and differentiation

机译:间充质干细胞抗坏血酸和软骨源性脱皮细胞外基质对其增殖,活力与分化的影响

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BackgroundThe development and application of biomaterials to promote stem cell proliferation and differentiation has undergone major expansion over the last few years. Decellularized stem cell matrix (DSCMs) represent bioactive and biocompatible materials which achieve similar characteristics of native extracellular matrix. DSCMs have given promising outcomes in generating novel cell culture substrates mimicking specific niche microenvironments in tissue engineering. AimsThis research aims at producing two different DSCMs obtained from adipose derived mesenchymal stem cells and bone marrow mesenchymal stem cells, characterize them and evaluate the DSCMs bioactivity on mesenchymal stem cells. MethodsDSCMs were produced using ascorbic or chondrogenic medium, which were then used as a scaffold for adipose derived mesenchymal stem cells and bone marrow mesenchymal stem cells, respectively. The biological characteristics of both types of DSCMs, including cell attachment, morphology, proliferation, viability, and chondrogenic and osteogenic differentiation were evaluated and compared. ResultsDifferences between ascorbic derived-DSCMs and chondrogenic derived DSCMs were found. Chondrogenic derived-DSCMs remained compact and stronger during extraction and this made their handling easier. Ascorbic derived-DSCMs showed a different protein composition to chondrogenic-DSCMs. Bioactive characteristics analyzed were different depending on the cellular origin of DSCM and the method used to produce them. ConclusionsThe DSCMs obtained in this work constitutes favorable structure- and growth factors providing a microenvironment which is very similar to that of native ECM, which results in enhanced biological potential of the MSCs and responsiveness to the induction of differentiation. We found differences between ascorbic derived-DSCMs and chondrogenic derived DSCMs. Our results suggest that the cell source used to produce DSCMs is highly related to the bioactive characteristics of DSCMs.
机译:背景技术生物材料以促进干细胞增殖和分化的发展和应用在过去几年中经历了重大扩张。脱细胞的干细胞基质(DSCMS)代表生物活性和生物相容性材料,其实现了天然细胞外基质的类似特征。 DSCMS在产生了在组织工程中模仿特异性Niche微环境的新细胞培养基材中具有有希望的结果。 AIMSTHIS研究旨在产生从脂肪衍生的间充质干细胞和骨髓间充质干细胞获得的两种不同的DSCM,表征并评估中间充质干细胞的DSCMS生物活性。方法使用抗坏血性或软骨培养基生产,然后用作脂肪衍生的间充质干细胞和骨髓间充质干细胞的支架。评估和比较两种类型DSCM的生物学特性,包括细胞附着,形态,增殖,活力和软骨内和骨质发生分化。发现抗坏血性衍生DSCM和软骨衍生DSCMS之间的结果。在提取过程中软骨衍生的-DSCM仍然紧凑,更强大,这使得它们的处理更容易。抗坏血性衍生DSCMS对软骨发生-DSCMS显示出不同的蛋白质组合物。分析的生物活性特性取决于DSCM的细胞来源和用于生产它们的方法。结论该工作中获得的DSCMS构成有利的结构和生长因子,提供了与本机ECM非常相似的微环境,这导致MSCs的生物潜力和对分化诱导的反应性。我们发现抗坏血性衍生DSCM和软骨生殖DSCM之间的差异。我们的研究结果表明,用于生产DSCM的细胞源与DSCM的生物活性特性高度相关。

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