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一种载有细胞的微流控水凝胶。

A cell-laden microfluidic hydrogel.

作者信息

Ling Yibo, Rubin Jamie, Deng Yuting, Huang Catherine, Demirci Utkan, Karp Jeffrey M, Khademhosseini Ali

机构信息

Harvard-MIT Division of Health Sciences and Technology, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.

出版信息

Lab Chip. 2007 Jun;7(6):756-62. doi: 10.1039/b615486g. Epub 2007 May 3.

Abstract

The encapsulation of mammalian cells within the bulk material of microfluidic channels may be beneficial for applications ranging from tissue engineering to cell-based diagnostic assays. In this work, we present a technique for fabricating microfluidic channels from cell-laden agarose hydrogels. Using standard soft lithographic techniques, molten agarose was molded against a SU-8 patterned silicon wafer. To generate sealed and water-tight microfluidic channels, the surface of the molded agarose was heated at 71 degrees C for 3 s and sealed to another surface-heated slab of agarose. Channels of different dimensions were generated and it was shown that agarose, though highly porous, is a suitable material for performing microfluidics. Cells embedded within the microfluidic molds were well distributed and media pumped through the channels allowed the exchange of nutrients and waste products. While most cells were found to be viable upon initial device fabrication, only those cells near the microfluidic channels remained viable after 3 days, demonstrating the importance of a perfused network of microchannels for delivering nutrients and oxygen to maintain cell viability in large hydrogels. Further development of this technique may lead to the generation of biomimetic synthetic vasculature for tissue engineering, diagnostics, and drug screening applications.

摘要

将哺乳动物细胞包裹在微流控通道的块状材料中,对于从组织工程到基于细胞的诊断分析等一系列应用可能是有益的。在这项工作中,我们展示了一种从载有细胞的琼脂糖水凝胶制造微流控通道的技术。使用标准的软光刻技术,将熔融的琼脂糖模制在SU-8图案化的硅晶片上。为了生成密封且防水的微流控通道,将模制琼脂糖的表面在71摄氏度下加热3秒,并与另一个表面加热的琼脂糖平板密封。生成了不同尺寸的通道,结果表明,琼脂糖虽然具有高度多孔性,但却是进行微流控的合适材料。嵌入微流控模具中的细胞分布良好,通过通道泵送的培养基允许营养物质和废物的交换。虽然在初始器件制造时发现大多数细胞是有活力的,但3天后只有那些靠近微流控通道的细胞仍然存活,这表明灌注微通道网络对于在大型水凝胶中输送营养物质和氧气以维持细胞活力的重要性。这项技术的进一步发展可能会导致用于组织工程、诊断和药物筛选应用的仿生合成脉管系统的产生。

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