Cell shape-dependent rectification of surface receptor transport in a sinusoidal electric field

In the presence of an extracellular electric field, transport dynamics of cell surface receptors represent a balance between electromigration and mutual diffusion. Because mutual diffusion is highly dependent on surface geometry, certain asymmetrical cell shapes effectively create an anisotropic resistance to receptor electromigration. If the resistance to receptor transport along a single axis is anisotropic, then an applied sinusoidal electric field will drive a net time-average receptor displacement, effectively rectifying receptor transport. To quantify the importance of this effect, a finite difference mathematical model was formulated and used to describe charged receptor transport in the plane of a plasma membrane. Representative values for receptor electromigration mobility and diffusivity were used. Model responses were examined for low frequency (10(-4)-10 Hz) 10-V/cm fields and compared with experimental measurements of receptor back-diffusion in human fibroblasts. It was found that receptor transport rectification behaved as a low-pass filter; at the tapered ends of cells, sinusoidal electric fields in the 10(-3) Hz frequency range caused a time-averaged accumulation of receptors as great as 2.5 times the initial uniform concentration. The extent of effective rectification of receptor transport was dependent on the rate of geometrical taper. Model studies also demonstrated that receptor crowding could alter transmembrane potential by an order of magnitude more than the transmembrane potential directly induced by the field. These studies suggest that cell shape is important in governing interactions between alternating current (ac) electric fields and cell surface receptors

Microfabrication of Individual 200μm Diameter Transdermal Microconduits Using High Voltage Pulsing in Salicylic Acid and Benzoic Acid

We describe an extension of semiconductor fabrication methods that creates individual ≈ 200;μm diameter aqueous pathways through human stratum corneum at predetermined sites. Our hypothesis is that spatially localized electroporation of the multilamellar lipid bilayer membranes provides rapid delivery of salicylic acid to the keratin within corneocytes, leading to localized keratin disruption and then to a microconduit. A microconduit penetrating the isolated stratum corneum supports a volumetric flow of order 0.01;ml per s with a pressure difference of only 0.01;atm (about 102;Pa). This study provides a method for rapidly microengineering a pathway in the skin to interface future devices for transdermal drug delivery and sampling of biologically relevant fluids