A numerical investigation of the electric and thermal cell kill distributions in electroporation-based therapies in tissue. Garcia, P. A., Davalos, R. V., & Miklavcic, D. PLoS One, 9(8):e103083, 2014. 1932-6203 Garcia, Paulo A Davalos, Rafael V Miklavcic, Damijan Journal Article Research Support, Non-U.S. Gov't United States 2014/08/15 PLoS One. 2014 Aug 12;9(8):e103083. doi: 10.1371/journal.pone.0103083. eCollection 2014.
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Electroporation-based therapies are powerful biotechnological tools for enhancing the delivery of exogeneous agents or killing tissue with pulsed electric fields (PEFs). Electrochemotherapy (ECT) and gene therapy based on gene electrotransfer (EGT) both use reversible electroporation to deliver chemotherapeutics or plasmid DNA into cells, respectively. In both ECT and EGT, the goal is to permeabilize the cell membrane while maintaining high cell viability in order to facilitate drug or gene transport into the cell cytoplasm and induce a therapeutic response. Irreversible electroporation (IRE) results in cell kill due to exposure to PEFs without drugs and is under clinical evaluation for treating otherwise unresectable tumors. These PEF therapies rely mainly on the electric field distributions and do not require changes in tissue temperature for their effectiveness. However, in immediate vicinity of the electrodes the treatment may results in cell kill due to thermal damage because of the inhomogeneous electric field distribution and high current density during the electroporation-based therapies. Therefore, the main objective of this numerical study is to evaluate the influence of pulse number and electrical conductivity in the predicted cell kill zone due to irreversible electroporation and thermal damage. Specifically, we simulated a typical IRE protocol that employs ninety 100-µs PEFs. Our results confirm that it is possible to achieve predominant cell kill due to electroporation if the PEF parameters are chosen carefully. However, if either the pulse number and/or the tissue conductivity are too high, there is also potential to achieve cell kill due to thermal damage in the immediate vicinity of the electrodes. Therefore, it is critical for physicians to be mindful of placement of electrodes with respect to critical tissue structures and treatment parameters in order to maintain the non-thermal benefits of electroporation and prevent unnecessary damage to surrounding healthy tissue, critical vascular structures, and/or adjacent organs.
@article{RN192,
   author = {Garcia, P. A. and Davalos, R. V. and Miklavcic, D.},
   title = {A numerical investigation of the electric and thermal cell kill distributions in electroporation-based therapies in tissue},
   journal = {PLoS One},
   volume = {9},
   number = {8},
   pages = {e103083},
   note = {1932-6203
Garcia, Paulo A
Davalos, Rafael V
Miklavcic, Damijan
Journal Article
Research Support, Non-U.S. Gov't
United States
2014/08/15
PLoS One. 2014 Aug 12;9(8):e103083. doi: 10.1371/journal.pone.0103083. eCollection 2014.},
   abstract = {Electroporation-based therapies are powerful biotechnological tools for enhancing the delivery of exogeneous agents or killing tissue with pulsed electric fields (PEFs). Electrochemotherapy (ECT) and gene therapy based on gene electrotransfer (EGT) both use reversible electroporation to deliver chemotherapeutics or plasmid DNA into cells, respectively. In both ECT and EGT, the goal is to permeabilize the cell membrane while maintaining high cell viability in order to facilitate drug or gene transport into the cell cytoplasm and induce a therapeutic response. Irreversible electroporation (IRE) results in cell kill due to exposure to PEFs without drugs and is under clinical evaluation for treating otherwise unresectable tumors. These PEF therapies rely mainly on the electric field distributions and do not require changes in tissue temperature for their effectiveness. However, in immediate vicinity of the electrodes the treatment may results in cell kill due to thermal damage because of the inhomogeneous electric field distribution and high current density during the electroporation-based therapies. Therefore, the main objective of this numerical study is to evaluate the influence of pulse number and electrical conductivity in the predicted cell kill zone due to irreversible electroporation and thermal damage. Specifically, we simulated a typical IRE protocol that employs ninety 100-µs PEFs. Our results confirm that it is possible to achieve predominant cell kill due to electroporation if the PEF parameters are chosen carefully. However, if either the pulse number and/or the tissue conductivity are too high, there is also potential to achieve cell kill due to thermal damage in the immediate vicinity of the electrodes. Therefore, it is critical for physicians to be mindful of placement of electrodes with respect to critical tissue structures and treatment parameters in order to maintain the non-thermal benefits of electroporation and prevent unnecessary damage to surrounding healthy tissue, critical vascular structures, and/or adjacent organs.},
   keywords = {Algorithms
Cell Survival
Electrochemotherapy/instrumentation/*methods
Electrodes
Electroporation/instrumentation/*methods
Gene Transfer Techniques
Humans
Liver
Models, Statistical
Temperature},
   ISSN = {1932-6203},
   DOI = {10.1371/journal.pone.0103083},
   year = {2014},
   type = {Journal Article}
}

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