You are here
CHARACTERIZING THE PHYSICAL PROPERTIES OF LIVING CELLS THROUGH MICROFLUIDIC IMPEDANCE SENSING
- Date Issued:
- 2020
- Abstract/Description:
- The purpose of this research is to explore and investigate the biophysical properties of living cells using microfluidics based electrical impedance sensing (EIS) technique. It provides a non-invasive approach to detect label-free biological markers in the regulation of cellular activities even at a molecular level. We specifically focus on the development, testing, and theoretical modeling of electrical impedance spectroscopy for neuroblastoma cells and endothelial cells. First, we demonstrate that the EIS technique can be used to monitor the progressive mitochondrial fission/fusion modification in genetically modified human neuroblastoma cell lines. Our results characterize quantitatively the abnormal mitochondrial dynamics through the variations in cytoplasm conductivity. Secondly, we employ a real time EIS method to determine the biophysical properties of the junctions which join one endothelial cell with one another in a monolayer of endothelial cells. In particular, we examine the role of the protein, c-MYC oncogene, in the barrier function. Our results show that the downregulation of c-MYC oncogene enhances the endothelial barrier dysfunction associated with inflammation. Finally, we measure and find that the electrical admittance (the reciprocal of the impedance) of the monolayer of endothelial cellular networks exhibits an anomalous power law of the form, Y ∝ ωα, over a wide range of frequency, with the value of the exponent, α, depending on the severity of the inflammation. We attribute the power law to the changes of the intercellular electric permeability between neighboring endothelial cells. Thus, the inflammation gives rise to relatively smaller values of α compared to that of the no-inflammation group. Furthermore, we propose a simple percolation model of a large R-C network to confirm the emergent of power law scaling behavior of the complex admittance, suggesting that the endothelial network behaves as a complex microstructural network and its electrical properties may be simulated by a large R-C network.
Title: | CHARACTERIZING THE PHYSICAL PROPERTIES OF LIVING CELLS THROUGH MICROFLUIDIC IMPEDANCE SENSING. |
56 views
29 downloads |
---|---|---|
Name(s): |
Galpayage, Dona Kalpani Nisansala Udeni, author Lau, Andy W.C., Thesis advisor Du, Sarah E. , Thesis advisor Florida Atlantic University, Degree grantor Department of Physics Charles E. Schmidt College of Science |
|
Type of Resource: | text | |
Genre: | Electronic Thesis Or Dissertation | |
Date Created: | 2020 | |
Date Issued: | 2020 | |
Publisher: | Florida Atlantic University | |
Place of Publication: | Boca Raton, Fla. | |
Physical Form: | application/pdf | |
Extent: | 115 p. | |
Language(s): | English | |
Abstract/Description: | The purpose of this research is to explore and investigate the biophysical properties of living cells using microfluidics based electrical impedance sensing (EIS) technique. It provides a non-invasive approach to detect label-free biological markers in the regulation of cellular activities even at a molecular level. We specifically focus on the development, testing, and theoretical modeling of electrical impedance spectroscopy for neuroblastoma cells and endothelial cells. First, we demonstrate that the EIS technique can be used to monitor the progressive mitochondrial fission/fusion modification in genetically modified human neuroblastoma cell lines. Our results characterize quantitatively the abnormal mitochondrial dynamics through the variations in cytoplasm conductivity. Secondly, we employ a real time EIS method to determine the biophysical properties of the junctions which join one endothelial cell with one another in a monolayer of endothelial cells. In particular, we examine the role of the protein, c-MYC oncogene, in the barrier function. Our results show that the downregulation of c-MYC oncogene enhances the endothelial barrier dysfunction associated with inflammation. Finally, we measure and find that the electrical admittance (the reciprocal of the impedance) of the monolayer of endothelial cellular networks exhibits an anomalous power law of the form, Y ∝ ωα, over a wide range of frequency, with the value of the exponent, α, depending on the severity of the inflammation. We attribute the power law to the changes of the intercellular electric permeability between neighboring endothelial cells. Thus, the inflammation gives rise to relatively smaller values of α compared to that of the no-inflammation group. Furthermore, we propose a simple percolation model of a large R-C network to confirm the emergent of power law scaling behavior of the complex admittance, suggesting that the endothelial network behaves as a complex microstructural network and its electrical properties may be simulated by a large R-C network. | |
Identifier: | FA00013595 (IID) | |
Degree granted: | Dissertation (Ph.D.)--Florida Atlantic University, 2020. | |
Collection: | FAU Electronic Theses and Dissertations Collection | |
Note(s): | Includes bibliography. | |
Subject(s): |
Microfluidics Impedance spectroscopy Cells |
|
Held by: | Florida Atlantic University Libraries | |
Sublocation: | Digital Library | |
Persistent Link to This Record: | http://purl.flvc.org/fau/fd/FA00013595 | |
Use and Reproduction: | Copyright © is held by the author with permission granted to Florida Atlantic University to digitize, archive and distribute this item for non-profit research and educational purposes. Any reuse of this item in excess of fair use or other copyright exemptions requires permission of the copyright holder. | |
Use and Reproduction: | http://rightsstatements.org/vocab/InC/1.0/ | |
Host Institution: | FAU | |
Is Part of Series: | Florida Atlantic University Digital Library Collections. |