4.5 Article

Actin networks regulate the cell membrane permeability during electroporation

Journal

BIOCHIMICA ET BIOPHYSICA ACTA-BIOMEMBRANES
Volume 1863, Issue 1, Pages -

Publisher

ELSEVIER
DOI: 10.1016/j.bbamem.2020.183468

Keywords

Electroporation; Electropermeabilization; Actin networks; Energy barrier; Temperature dependent kinetics of electroporation

Funding

  1. European Research Council (ERC) under European Union [819424]
  2. European Research Council (ERC) [819424] Funding Source: European Research Council (ERC)

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In electroporation, disruption of actin networks influences cell membrane permeability, leading to increased uptake of membrane-impermeable molecules with higher temperatures. This suggests a potential lowering of the activation energy barrier for electroporation when actin networks are disrupted, emphasizing the importance of cytoskeletal networks in understanding cell membrane permeability during the delivery of exogenous substances.
Transient physical disruption of cell membranes by electric pulses (or electroporation) has significance in biomedical and biological applications requiring the delivery of exogenous (bio)molecules to living cells. We demonstrate that actin networks regulate the cell membrane permeability during electroporation. Disruption of actin networks increases the uptake of membrane-impermeable molecules such as propidium iodide during electroporation. Our experiments at different temperatures ranging from 11 degrees C to 37 degrees C show that molecular uptake during electroporation increases with temperature. Furthermore, by examining the temperature-dependent kinetics of propidium iodide uptake, we infer that the activation energy barrier of electroporation is lowered when the actin networks are disrupted. Our numerical calculations of transmembrane voltage show that the reduced activation energy barrier for the cells with disrupted actin is not a consequence of the changes in transmembrane voltage associated with changes in the cell shape due to the disruption of actin, indicating that this could be due to changes in membrane mechanical properties. Our results suggest that the current theoretical models of electroporation should be advanced further by including the contributions of the cytoskeletal networks on the cell membrane permeability during the delivery of exogenous materials.

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