Simulation of the Effects of Extracellular Calcium Changes Leads to a Novel Computational Model of Human Ventricular Action Potential With a Revised Calcium Handling.

Front Physiol

Computational Physiopathology Unit, Department of Electrical, Electronic and Information Engineering "Guglielmo Marconi", University of Bologna, Cesena, Italy.

Published: April 2020

AI Article Synopsis

  • Electrolyte concentrations are crucial for proper cardiac function, as variations can trigger arrhythmias through their role in action potential generation and cell stability.
  • Most existing human action potential models, including the widely used O'Hara-Rudy model, assume constant electrolyte levels and don't account for physiological changes in electrolyte concentrations, particularly calcium.
  • The new BPS2020 model builds on ORd, allowing for simulations of how extracellular calcium affects action potential duration and can examine repolarization issues, variability, and other potentially dangerous conditions related to electrolyte changes and current block.

Article Abstract

The importance of electrolyte concentrations for cardiac function is well established. Electrolyte variations can lead to arrhythmias onset, due to their important role in the action potential (AP) genesis and in maintaining cell homeostasis. However, most of the human AP computer models available in literature were developed with constant electrolyte concentrations, and fail to simulate physiological changes induced by electrolyte variations. This is especially true for Ca, even in the O'Hara-Rudy model (ORd), one of the most widely used models in cardiac electrophysiology. Therefore, the present work develops a new human ventricular model (BPS2020), based on ORd, able to simulate the inverse dependence of AP duration (APD) on extracellular Ca concentration ([Ca]), and APD rate dependence at 4 mM extracellular K. The main changes needed with respect to ORd are: (i) an increased sensitivity of L-type Ca current inactivation to [Ca]; (ii) a single compartment description of the sarcoplasmic reticulum; iii) the replacement of Ca release. BPS2020 is able to simulate the physiological APD-[Ca] relationship, while also retaining the well-reproduced properties of ORd (APD rate dependence, restitution, accommodation and current block effects). We also used BPS2020 to generate an experimentally-calibrated population of models to investigate: (i) the occurrence of repolarization abnormalities in response to hERG current block; (ii) the rate adaptation variability; (iii) the occurrence of alternans and delayed after-depolarizations at fast pacing. Our results indicate that we successfully developed an improved version of ORd, which can be used to investigate electrophysiological changes and pro-arrhythmic abnormalities induced by electrolyte variations and current block at multiple rates and at the population level.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7174690PMC
http://dx.doi.org/10.3389/fphys.2020.00314DOI Listing

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