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Evaluation of Cellular Adhesion and Organization in Different Microporous Polymeric Scaffolds

机译:不同微孔聚合物支架中细胞粘附和组织的评价

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摘要

The lack of prediction accuracy during drug development and screening risks complications during human trials, such as drug-induced liver injury (DILI), and has led to a demand for robust, human cell-based, in vitro assays for drug discovery. Microporous polymer-based scaffolds offer an alternative to the gold standard flat tissue culture plastic (2D TCPS) and other 3D cell culture platforms as the porous material entraps cells, making it advantageous for automated liquid handlers and high-throughput screening (HTS). In this study, we optimized the surface treatment, pore size, and choice of scaffold material with respect to cellular adhesion, tissue organization, and expression of complex physiologically relevant (CPR) outcomes such as the presence of bile canaliculi-like structures. Poly-l-lysine and fibronectin (FN) coatings have been shown to encourage cell attachment to the underlying substrate. Treatment of the scaffold surface with NaOH followed with a coating of FN improved cell attachment and penetration into pores. Of the two pore sizes we investigated (A: 104 +/- 4 m; B: 175 +/- 6 m), the larger pore size better promoted cell penetration while limiting tissue growth from reaching the hypoxia threshold. Finally, polystyrene (PS) proved to be conducive to cell growth, penetration into the scaffold, and yielded CPR outcomes while being a cost-effective choice for HTS applications. These observations provide a foundation for optimizing microporous polymer-based scaffolds suitable for drug discovery. (C) 2018 American Institute of Chemical Engineers
机译:在药物开发期间缺乏预测准确性和筛选人类试验期间的风险并发症,例如药物诱导的肝损伤(DILI),并导致了对药物发现的稳健的需求,用于药物发现的体外测定。微孔聚合物基支架提供了金标准扁平组织培养塑料(2D TCP)和其他3D细胞培养平台作为多孔材料嵌入细胞的替代方案,使其可用于自动液体处理器和高通量筛选(HTS)。在这项研究中,我们优化了对细胞粘附,组织组织和复杂生理学相关(CPR)结果的表达等蜂窝粘附,组织组织等表面处理,孔径和选择性的表面处理,孔径和选择,例如胆汁Canaliculi样结构的存在。已经证明了聚-L-赖氨酸和纤连蛋白(FN)涂层促使细胞附着在下面的基底上。用NaOH处理支架表面,然后用FN改进的细胞附着涂层并渗透到孔中。我们调查的两种孔径(A:104 +/- 4M; B:175 +/- 6米),孔径较大,更好地促进细胞渗透,同时限制了组织生长达到缺氧阈值。最后,通过聚苯乙烯(PS)被证明有利于细胞生长,渗透到支架中,并产生CPR结果,同时是HTS应用的成本效益选择。这些观察结果提供了优化适用于药物发现的微孔聚合物的支架的基础。 (c)2018美国化学工程研究所

著录项

  • 来源
    《Biotechnology Progress 》 |2018年第2期| 共10页
  • 作者单位

    Univ Georgia Driftmier Engn Ctr Coll Engn Sch Chem Mat &

    Biomed Engn Cellular Bioengn Lab Athens GA 30602 USA;

    Univ Georgia Driftmier Engn Ctr Coll Engn Sch Chem Mat &

    Biomed Engn Cellular Bioengn Lab Athens GA 30602 USA;

    Univ Georgia Driftmier Engn Ctr Coll Engn Sch Chem Mat &

    Biomed Engn Cellular Bioengn Lab Athens GA 30602 USA;

    Univ Georgia Driftmier Engn Ctr Coll Engn Sch Chem Mat &

    Biomed Engn Cellular Bioengn Lab Athens GA 30602 USA;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 生物科学 ;
  • 关键词

    cell-based assay; HTS; hepatic; scaffold; 3D culture;

    机译:基于细胞的测定;HTS;肝脏;脚手架;3D文化;

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