Membrane polarization at the excitation threshold induced by external electric fields in cardiomyocytes of rats at different developmental stages

External electric fields ( E ), used for cardiac pacing and defibrillation/cardioversion, induce a spatially variable change in cardiomyocyte transmembrane potential (Δ V m ) that depends on cell geometry and E orientation. This study investigates E -induced Δ V m in cardiomyocytes from rats at diff...

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Published inMedical & biological engineering & computing Vol. 61; no. 10; pp. 2637 - 2647
Main Authors Milan, Hugo F. M., Almazloum, Ahmad A., Bassani, Rosana A., Bassani, José W. M.
Format Journal Article
LanguageEnglish
Published Berlin/Heidelberg Springer Berlin Heidelberg 01.10.2023
Springer Nature B.V
Subjects
Aging
Animal models
Biomedical and Life Sciences
Biomedical Engineering and Bioengineering
Biomedicine
Cardiac muscle
Cardiomyocytes
Cell size
Computer Applications
Developmental stages
Electric fields
Excitability
Excitation
Geometry
Heart
Human Physiology
Imaging
Mathematical analysis
Mathematical models
Membrane potential
Myocytes
Neonates
Original Article
Radiology
Ventricle
Weaning
Excitability
Development
Aging
Electric field
Membrane electromagnetic models
Membrane polarization
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Summary:External electric fields ( E ), used for cardiac pacing and defibrillation/cardioversion, induce a spatially variable change in cardiomyocyte transmembrane potential (Δ V m ) that depends on cell geometry and E orientation. This study investigates E -induced Δ V m in cardiomyocytes from rats at different ages, which show marked size/geometry variation. Using a tridimensional numerical electromagnetic model recently proposed (NM3D), it was possible: (a) to evaluate the suitability of the simpler, prolate spheroid analytical model (PSAM) to calculate amplitude and location of Δ V m maximum (Δ V max ) for E  = 1 V.cm −1 ; and (b) to estimate the Δ V max required for excitation (Δ V T ) from experimentally determined threshold E values ( E T ). Ventricular myocytes were isolated from neonatal, weaning, adult, and aging Wistar rats. NM3D was constructed as the extruded 2D microscopy cell image, while measured minor and major cell dimensions were used for PSAM. Acceptable Δ V m estimates can be obtained with PSAM from paralelepidal cells for small θ . E T , but not Δ V T , was higher for neonate cells. Δ V T was significantly greater in the cell from older animals, which indicate lower responsiveness to E associated with aging, rather than with altered cell geometry/dimensions. Δ V T might be used as a non-invasive indicator of cell excitability as it is little affected by cell geometry/size. Graphical Abstract
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ISSN:0140-0118
1741-0444
DOI:10.1007/s11517-023-02868-1