Affiliation:
1. Mechanical Engineering Department, Southern Methodist University, Dallas, TX 75275, USA
2. Department of Biological Sciences, University of Texas at Dallas, Dallas, TX 75080, USA
Abstract
The plasma membrane is a lipid bilayer that establishes the outer boundary of a living cell. The composition of the lipid bilayer influences the membrane’s biophysical properties, including fluidity, thickness, permeability, phase behavior, charge, elasticity, and formation of flat sheet or curved structures. Changes in the biophysical properties of the membrane can be occasioned when new entities, such as drug molecules, are partitioned in the bilayer. Therefore, assessing drugs for their effect on the biophysical properties of the lipid bilayer of a cell membrane is critical to understanding specific and non-specific drug action. Previously, we reported a non-invasive technique for real-time characterization of cellular dielectric properties, such as membrane capacitance and cytoplasmic conductivity. In this study, we discuss the potential application of the technique in assessing the biophysical properties of the cell membrane in response to interaction with amiodarone compared to aspirin/acetylsalicylic acid and glucose. Amiodarone is a potent drug used to treat cardiac arrhythmia, but it also exerts various non-specific effects. Compared to aspirin and glucose, we measured a rapid and higher magnitude increase in membrane capacitance on cells under amiodarone treatment. Increased membrane capacitance induced by aspirin and glucose quickly returned to baseline in 15 s, while amiodarone-induced increased capacitance sustained and decreased slowly, approaching baseline or another asymptotic limit in ~2.5 h. Because amiodarone has a strong lipid partitioning property, we reason that drug partitioning alters the lipid bilayer context and subsequently reduces bilayer thickness, leading to an increase in the electrical capacitance of the cell membrane. The presented microfluidic system promises a new approach to assess drug–membrane interactions and delineate specific and non-specific actions of the drug on cells.
Subject
Electrical and Electronic Engineering,Mechanical Engineering,Control and Systems Engineering
Reference38 articles.
1. NMR of peptides and proteins in oriented membranes;Marassi;Concepts Magn. Reson. Educ. J.,2002
2. Alberts, B., Johnson, A., Lewis, J., Raff, M., Roberts, K., and Walter, P. (2002). Molecular Biology of the Cell, Garland Science. [4th ed.].
3. The lipid bilayer concept and its experimental realization: From soap bubbles, kitchen sink, to bilayer lipid membranes;Tien;J. Membr. Sci.,2001
4. Stein, W. (2012). Transport and Diffusion Across Cell Membranes, Elsevier.
5. Lateral pressures in cell membranes: A mechanism for modulation of protein function;Cantor;J. Phys. Chem. B,1997
Cited by
8 articles.
订阅此论文施引文献
订阅此论文施引文献,注册后可以免费订阅5篇论文的施引文献,订阅后可以查看论文全部施引文献