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Spatiotemporal control and modeling of morphogen delivery to induce gradient patterning of stem cell differentiation using fluidic channels

机译:使用流体通道诱导干细胞分化梯度图案化的时性对照和模拟

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摘要

The process of cell differentiation in a developing embryo is influenced by numerous factors, including various biological molecules whose presentation varies dramatically over space and time. These morphogens regulate cell fate based on concentration profiles, thus creating discrete populations of cells and ultimately generating large, complex tissues and organs. Recently, several in vitro platforms have attempted to recapitulate the complex presentation of extrinsic signals found in nature. However, it has been a challenge to design versatile platforms that can dynamically control morphogen gradients over extended periods of time. To address some of these issues, we introduce a platform using channels patterned in hydrogels to deliver multiple morphogens to cells in a 3D scaffold, thus creating a spectrum of cell phenotypes based on the resultant morphogen gradients. The diffusion coefficient of a common small molecule morphogen, retinoic acid (RA), was measured within our hydrogel platform using Raman spectroscopy and its diffusion in our platform's geometry was modeled using finite element analysis. The predictive model of spatial gradients was validated in a cell-free hydrogel, and temporal control of morphogen gradients was then demonstrated using a reporter cell line that expresses green fluorescent protein in the presence of RA. Finally, the utility of this approach for regulating cell phenotype was demonstrated by generating opposing morphogen gradients to create a spectrum of mesenchymal stem cell differentiation states.
机译:在发育胚胎中细胞分化的过程受到许多因素的影响,包括各种生物分子,其呈现在空间和时间上急剧变化。这些形态酚基根据浓度谱调节细胞命运,从而产生细胞的离散群体,最终产生大,复杂的组织和器官。最近,一些体外平台已经试图重新承载自然中发现的外部信号的复杂呈现。然而,设计多功能平台是一个挑战,这些平台可以在延长的时间段内动态控制形态学梯度。为了解决这些问题中的一些问题,我们使用水凝胶中图案化的通道介绍一个平台,以将多种变种子传递给3D支架中的细胞,从而基于所得的形态学梯度产生一种细胞表型。使用拉曼光谱法测量在我们的水凝胶平台中测量常见的小分子形态学,视黄酸(Ra)的扩散系数,并使用有限元分析模拟我们平台几何形状中的扩散。在无细胞水凝胶中验证了空间梯度的预测模型,然后使用在RA存在下表达绿色荧光蛋白的报告细胞系进行了化学梯度的时间控制。最后,通过产生相反的形态原梯度来制定这种调节细胞表型的这种方法的效用,以产生间充质干细胞分化态的光谱。

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  • 来源
    《Biomaterials Science》 |2019年第4期|共14页
  • 作者单位

    Vanderbilt Univ Dept Mech Engn Nashville TN 37235 USA;

    Vanderbilt Univ Dept Biomed Engn Nashville TN 37235 USA;

    Vanderbilt Univ Dept Biomed Engn Nashville TN 37235 USA;

    Vanderbilt Univ Dept Chem &

    Biomol Engn 221 Kirkland Hall Nashville TN 37235 USA;

    Vanderbilt Univ Dept Chem &

    Biomol Engn 221 Kirkland Hall Nashville TN 37235 USA;

    Vanderbilt Univ Dept Chem &

    Biomol Engn 221 Kirkland Hall Nashville TN 37235 USA;

    Vanderbilt Univ Dept Biomed Engn Nashville TN 37235 USA;

    Vanderbilt Univ Dept Mech Engn Nashville TN 37235 USA;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分子生物学;
  • 关键词

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