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Permeation Studies across Symmetric and Asymmetric Membranes in Microdroplet Arrays

机译:微型阵列中对称和不对称膜的渗透研究

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摘要

We investigated the permeation of molecules across lipid membranes on an open microfluidic platform. An array of droplet pairs was created by spotting aqueous droplets, dispersed in a lipid oil solution, onto a plate with cavities surrounded by a hydrophobic substrate. Droplets in two adjacent cavities come in contact and form an artificial lipid bilayer, called a droplet interface bilayer (DIB). The method allows for monitoring permeation of fluorescently tagged compounds from a donor droplet to an acceptor droplet. A mathematical model was applied to describe the kinetics and determine the permeation coefficient. We also demonstrate that permeation kinetics can be followed over a series of droplets, all connected via DIBs. Moreover, by changing the lipid oil composition after spotting donor droplets, we were able to create asymmetric membranes that we used to mimic the asymmetry of the cellular plasma membrane. Finally, we developed a protocol to separate and extract the droplets for label-free analysis of permeating compounds by liquid chromatography–mass spectrometry. Our versatile platform has the potential to become a new tool for the screening of drug membrane permeability in the future.
机译:我们在一个开放的微流控平台上研究了分子在脂膜上的渗透。通过将分散在油脂溶液中的水滴点在一个有空腔的平板上,形成一组液滴对。两个相邻空腔中的液滴相互接触,形成人工脂质双层,称为液滴界面双层(DIB)。该方法允许监测荧光标记化合物从供体液滴到受体液滴的渗透。应用数学模型描述动力学并确定渗透系数。我们还证明,通过DIB连接的一系列液滴可以遵循渗透动力学。此外,通过在发现供体液滴后改变油脂成分,我们能够创造出不对称的膜,我们用来模拟细胞质膜的不对称性。最后,我们开发了一个协议,用于分离和提取液滴,通过液相色谱-质谱对渗透化合物进行无标签分析。我们的多功能平台有望成为未来筛选药物膜通透性的新工具。

著录项

  • 来源
    《Analytical chemistry》 |2021年第12期|共8页
  • 作者单位

    Department of Biosystems Science and Engineering ETH Zurich;

    Department of Biosystems Science and Engineering ETH Zurich;

    Institute of Pharmaceutical Sciences Department of Chemistry and Applied Biosciences ETH Zurich;

    Department of Biosystems Science and Engineering ETH Zurich;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 分析化学;
  • 关键词

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