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动态三维培养方法可增强间充质干细胞特性并提高治疗潜力。

Dynamic three-dimensional culture methods enhance mesenchymal stem cell properties and increase therapeutic potential.

机构信息

Department of Biology, University of York, Heslington, York, United Kingdom.

出版信息

Tissue Eng Part C Methods. 2010 Aug;16(4):735-49. doi: 10.1089/ten.TEC.2009.0432.

Abstract

Mesenchymal stem cells (MSCs) are capable of self-renewal and differentiation along the osteogenic, chondrogenic, and adipogenic lineages and have potential applications in a range of therapies. MSCs can be cultured as monolayers on tissue culture plastic, but there are indications that they lose cell-specific properties with time in vitro and so poorly reflect in vivo MSC behavior. We developed dynamic three-dimensional (3D) techniques for in vitro MSC culture using spinner flasks and a rotating wall vessel bioreactor. We characterized the two methods for dynamic 3D MSC culture and compared the properties of these cultures with monolayer MSCs. Our results showed that under optimal conditions, MSCs form compact cellular spheroids and remain viable in dynamic 3D culture. We demonstrated altered cell size and surface antigen expression together with enhanced osteogenic and adipogenic differentiation potential in MSCs from dynamic 3D conditions. By microarray analysis of monolayer and spinner flask MSCs, we identified many differences in gene expression, including those confirming widespread changes to the cellular architecture and extracellular matrix. The upregulation of interleukin 24 in dynamic 3D cultures was shown to selectively impair the viability of prostate cancer cells cultured in medium conditioned by dynamic 3D MSCs. Overall, this work suggests a novel therapeutic application for dynamic 3D MSCs and demonstrates that these methods are a viable alternative to monolayer techniques and may prove beneficial for retaining MSC properties in vitro.

摘要

间充质干细胞(MSCs)具有自我更新和沿着成骨、软骨和成脂谱系分化的能力,并在多种治疗中有潜在的应用。MSCs 可以在组织培养塑料上培养成单层,但有迹象表明,它们在体外随着时间的推移会失去细胞特异性特性,因此很难反映体内 MSC 的行为。我们开发了使用旋转瓶和旋转壁式生物反应器的体外 MSC 培养的动态三维(3D)技术。我们对这两种动态 3D MSC 培养方法进行了表征,并将这些培养物的特性与单层 MSC 进行了比较。我们的结果表明,在最佳条件下,MSCs 形成紧密的细胞球体,并在动态 3D 培养中保持存活。我们证明了细胞大小和表面抗原表达的改变,以及在动态 3D 条件下 MSC 的成骨和成脂分化潜能增强。通过单层和旋转瓶 MSC 的微阵列分析,我们确定了基因表达的许多差异,包括那些证实细胞结构和细胞外基质广泛改变的差异。在动态 3D 培养中白细胞介素 24 的上调被证明选择性地损害了在由动态 3D MSC 条件培养基培养的前列腺癌细胞的活力。总的来说,这项工作表明动态 3D MSC 具有新的治疗应用,并证明这些方法是单层技术的可行替代方法,可能有助于在体外保留 MSC 特性。

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