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生物活性物质在具有有序形貌的细胞上的纳米级电压驱动应用。

Nanoscale, Voltage-Driven Application of Bioactive Substances onto Cells with Organized Topography.

作者信息

Schobesberger Sophie, Jönsson Peter, Buzuk Andrey, Korchev Yuri, Siggers Jennifer, Gorelik Julia

机构信息

Department of Medicine, Imperial College London, London, United Kingdom.

Department of Chemistry, Lund University, Lund, Sweden.

出版信息

Biophys J. 2016 Jan 5;110(1):141-6. doi: 10.1016/j.bpj.2015.11.017.

Abstract

With scanning ion conductance microscopy (SICM), a noncontact scanning probe technique, it is possible both to obtain information about the surface topography of live cells and to apply molecules onto specific nanoscale structures. The technique is therefore widely used to apply chemical compounds and to study the properties of molecules on the surfaces of various cell types. The heart muscle cells, i.e., the cardiomyocytes, possess a highly elaborate, unique surface topography including transverse-tubule (T-tubule) openings leading into a cell internal system that exclusively harbors many proteins necessary for the cell's physiological function. Here, we applied isoproterenol into these surface openings by changing the applied voltage over the SICM nanopipette. To determine the grade of precision of our application we used finite-element simulations to investigate how the concentration profile varies over the cell surface. We first obtained topography scans of the cardiomyocytes using SICM and then determined the electrophoretic mobility of isoproterenol in a high ion solution to be -7 × 10(-9) m(2)/V s. The simulations showed that the delivery to the T-tubule opening is highly confined to the underlying Z-groove, and especially to the first T-tubule opening, where the concentration is ∼6.5 times higher compared to on a flat surface under the same delivery settings. Delivery to the crest, instead of the T-tubule opening, resulted in a much lower concentration, emphasizing the importance of topography in agonist delivery. In conclusion, SICM, unlike other techniques, can reliably deliver precise quantities of compounds to the T-tubules of cardiomyocytes.

摘要

扫描离子电导显微镜(SICM)作为一种非接触式扫描探针技术,既能获取活细胞表面形貌信息,又能将分子应用于特定的纳米级结构。因此,该技术被广泛用于施加化合物以及研究各种细胞类型表面分子的性质。心肌细胞,即cardiomyocytes,具有高度精细、独特的表面形貌,包括通向细胞内部系统的横管(T管)开口,该系统专门容纳许多细胞生理功能所需的蛋白质。在此,我们通过改变SICM纳米移液器上施加的电压,将异丙肾上腺素施加到这些表面开口中。为了确定我们施加的精度等级,我们使用有限元模拟来研究浓度分布在细胞表面如何变化。我们首先使用SICM获得心肌细胞的形貌扫描图,然后确定异丙肾上腺素在高离子溶液中的电泳迁移率为-7×10(-9)m(2)/V s。模拟结果表明,向T管开口的递送高度局限于下方的Z沟,特别是第一个T管开口,在相同递送设置下,此处的浓度比平坦表面上的浓度高约6.5倍。向嵴而不是T管开口递送导致浓度低得多,这强调了形貌在激动剂递送中的重要性。总之,与其他技术不同,SICM能够可靠地将精确数量的化合物递送至心肌细胞的T管。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8b85/4805872/eff2d92903e3/gr1.jpg

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