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首页> 外文期刊>Frontiers in Bioengineering and Biotechnology >Integration of Hydrogel Microparticles With Three-Dimensional Liver Progenitor Cell Spheroids
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Integration of Hydrogel Microparticles With Three-Dimensional Liver Progenitor Cell Spheroids

机译:用三维肝祖细胞球体与三维肝祖细胞球体的整合水凝胶微粒

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The study of the liver progenitor cell microenvironment has demonstrated the important roles of both biochemical and biomechanical signals in regulating the progenitor cell functions that underlie liver morphogenesis and regeneration. While controllable two-dimensional in vitro culture systems have provided key insights into the effects of growth factors and extracellular matrix composition and mechanics on liver differentiation, it remains unclear how microenvironmental signals may differentially affect liver progenitor cell responses in a three-dimensional (3D) culture context. In addition, there has only been limited efforts to engineer 3D culture models of liver progenitor cells with the tunable presentation of microenvironmental stimuli. We present an in vitro model of 3D liver progenitor spheroidal cultures with integrated polyethylene glycol (PEG) hydrogel microparticles for the internal presentation of modular microenvironmental cues and the examination of the combinatorial effects with exogenous soluble factor. In particular, treatment with the growth factor TGF?1 directs differentiation of the spheroidal liver progenitor cells to a biliary phenotype, a behavior which was further enhanced in the presence of hydrogel microparticles. We further demonstrate that surface modification of the hydrogel microparticles with heparin influences the behavior of liver progenitor cells towards biliary differentiation. Taken together, this liver progenitor cell culture system represents an approach for controlling the presentation of microenvironmental cues internalized within 3D spheroidal aggregate cultures. Overall, this strategy could be applied towards the engineering of instructive microenvironments that control stem and progenitor cell differentiation within a 3D context for tissue engineering, drug testing, and metabolic studies.
机译:肝祖细胞微环境的研究表明了生物化学和生物力学信号在调节肝脏形态发生和再生的祖细胞功能方面的重要作用。虽然可控的二维体外培养系统提供了对生长因子和细胞外基质组成和机制对肝脏分化的影响的关键见解,但仍然不明确于微环境信号如何差异地影响三维(3D)中的肝祖细胞应答文化背景。此外,通过微环境刺激的可调谐呈现,仅努力工程到肝祖细胞3D培养模型的努力。我们向3D肝祖细胞培养物的体外模型与集成聚乙二醇(PEG)水凝胶微粒进行模块化微环境提示的内部呈递,并与外源可溶性因子检查组合效应。特别地,用生长因子TGFβ1的处理将球形肝祖细胞的分化指向胆道表型,在水凝胶微粒存在下进一步增强的行为。我们进一步证明,水凝胶微粒与肝素的表面改性会影响肝祖细胞对胆道分化的行为。携带在一起,该肝祖细胞培养系统代表了一种控制在3D球体聚集培养物内部内化的微环境提示呈现的方法。总的来说,这种策略可以应用于控制茎和祖细胞分化的指导微环境的工程,用于组织工程,药物检测和代谢研究的3D背景下。

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