Genetic algorithm-based personalized models of human cardiac action potential
We present a novel modification of genetic algorithm (GA) which determines personalized parameters of cardiomyocyte electrophysiology model based on set of experimental human action potential (AP) recorded at different heart rates. In order to find the steady state solution, the optimized algorithm...
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| Published in | PloS one Vol. 15; no. 5; p. e0231695 |
|---|---|
| Main Authors | , , , , , , , , |
| Format | Journal Article |
| Language | English |
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United States
Public Library of Science
11.05.2020
Public Library of Science (PLoS) |
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| Online Access | Get full text |
| ISSN | 1932-6203 1932-6203 |
| DOI | 10.1371/journal.pone.0231695 |
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| Abstract | We present a novel modification of genetic algorithm (GA) which determines personalized parameters of cardiomyocyte electrophysiology model based on set of experimental human action potential (AP) recorded at different heart rates. In order to find the steady state solution, the optimized algorithm performs simultaneous search in the parametric and slow variables spaces. We demonstrate that several GA modifications are required for effective convergence. Firstly, we used Cauchy mutation along a random direction in the parametric space. Secondly, relatively large number of elite organisms (6-10% of the population passed on to new generation) was required for effective convergence. Test runs with synthetic AP as input data indicate that algorithm error is low for high amplitude ionic currents (1.6±1.6% for IKr, 3.2±3.5% for IK1, 3.9±3.5% for INa, 8.2±6.3% for ICaL). Experimental signal-to-noise ratio above 28 dB was required for high quality GA performance. GA was validated against optical mapping recordings of human ventricular AP and mRNA expression profile of donor hearts. In particular, GA output parameters were rescaled proportionally to mRNA levels ratio between patients. We have demonstrated that mRNA-based models predict the AP waveform dependence on heart rate with high precision. The latter also provides a novel technique of model personalization that makes it possible to map gene expression profile to cardiac function. |
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| AbstractList | We present a novel modification of genetic algorithm (GA) which determines personalized parameters of cardiomyocyte electrophysiology model based on set of experimental human action potential (AP) recorded at different heart rates. In order to find the steady state solution, the optimized algorithm performs simultaneous search in the parametric and slow variables spaces. We demonstrate that several GA modifications are required for effective convergence. Firstly, we used Cauchy mutation along a random direction in the parametric space. Secondly, relatively large number of elite organisms (6-10% of the population passed on to new generation) was required for effective convergence. Test runs with synthetic AP as input data indicate that algorithm error is low for high amplitude ionic currents (1.6±1.6% for IKr, 3.2±3.5% for IK1, 3.9±3.5% for INa, 8.2±6.3% for ICaL). Experimental signal-to-noise ratio above 28 dB was required for high quality GA performance. GA was validated against optical mapping recordings of human ventricular AP and mRNA expression profile of donor hearts. In particular, GA output parameters were rescaled proportionally to mRNA levels ratio between patients. We have demonstrated that mRNA-based models predict the AP waveform dependence on heart rate with high precision. The latter also provides a novel technique of model personalization that makes it possible to map gene expression profile to cardiac function. We present a novel modification of genetic algorithm (GA) which determines personalized parameters of cardiomyocyte electrophysiology model based on set of experimental human action potential (AP) recorded at different heart rates. In order to find the steady state solution, the optimized algorithm performs simultaneous search in the parametric and slow variables spaces. We demonstrate that several GA modifications are required for effective convergence. Firstly, we used Cauchy mutation along a random direction in the parametric space. Secondly, relatively large number of elite organisms (6-10% of the population passed on to new generation) was required for effective convergence. Test runs with synthetic AP as input data indicate that algorithm error is low for high amplitude ionic currents (1.6±1.6% for IKr, 3.2±3.5% for IK1, 3.9±3.5% for INa, 8.2±6.3% for ICaL). Experimental signal-to-noise ratio above 28 dB was required for high quality GA performance. GA was validated against optical mapping recordings of human ventricular AP and mRNA expression profile of donor hearts. In particular, GA output parameters were rescaled proportionally to mRNA levels ratio between patients. We have demonstrated that mRNA-based models predict the AP waveform dependence on heart rate with high precision. The latter also provides a novel technique of model personalization that makes it possible to map gene expression profile to cardiac function.We present a novel modification of genetic algorithm (GA) which determines personalized parameters of cardiomyocyte electrophysiology model based on set of experimental human action potential (AP) recorded at different heart rates. In order to find the steady state solution, the optimized algorithm performs simultaneous search in the parametric and slow variables spaces. We demonstrate that several GA modifications are required for effective convergence. Firstly, we used Cauchy mutation along a random direction in the parametric space. Secondly, relatively large number of elite organisms (6-10% of the population passed on to new generation) was required for effective convergence. Test runs with synthetic AP as input data indicate that algorithm error is low for high amplitude ionic currents (1.6±1.6% for IKr, 3.2±3.5% for IK1, 3.9±3.5% for INa, 8.2±6.3% for ICaL). Experimental signal-to-noise ratio above 28 dB was required for high quality GA performance. GA was validated against optical mapping recordings of human ventricular AP and mRNA expression profile of donor hearts. In particular, GA output parameters were rescaled proportionally to mRNA levels ratio between patients. We have demonstrated that mRNA-based models predict the AP waveform dependence on heart rate with high precision. The latter also provides a novel technique of model personalization that makes it possible to map gene expression profile to cardiac function. |
| Audience | Academic |
| Author | Efimov, Igor R. Gams, Anna Koppel, Aaron Gusev, Oleg Smirnov, Dmitrii Syunyaev, Roman Deviatiiarov, Ruslan Aras, Kedar Pikunov, Andrey |
| AuthorAffiliation | University of Oxford, UNITED KINGDOM 2 The George Washington University, Washington, DC, United States of America 1 Moscow Institute of Physics and Technology, Dolgoprudny, Russia 3 Sechenov University, Moscow, Russia 4 Kazan Federal University, Kazan, Russia |
| AuthorAffiliation_xml | – name: University of Oxford, UNITED KINGDOM – name: 3 Sechenov University, Moscow, Russia – name: 1 Moscow Institute of Physics and Technology, Dolgoprudny, Russia – name: 4 Kazan Federal University, Kazan, Russia – name: 2 The George Washington University, Washington, DC, United States of America |
| Author_xml | – sequence: 1 givenname: Dmitrii surname: Smirnov fullname: Smirnov, Dmitrii – sequence: 2 givenname: Andrey surname: Pikunov fullname: Pikunov, Andrey – sequence: 3 givenname: Roman orcidid: 0000-0001-9582-0199 surname: Syunyaev fullname: Syunyaev, Roman – sequence: 4 givenname: Ruslan surname: Deviatiiarov fullname: Deviatiiarov, Ruslan – sequence: 5 givenname: Oleg orcidid: 0000-0002-6203-9758 surname: Gusev fullname: Gusev, Oleg – sequence: 6 givenname: Kedar orcidid: 0000-0002-9898-1462 surname: Aras fullname: Aras, Kedar – sequence: 7 givenname: Anna orcidid: 0000-0002-3052-8469 surname: Gams fullname: Gams, Anna – sequence: 8 givenname: Aaron orcidid: 0000-0003-4887-2695 surname: Koppel fullname: Koppel, Aaron – sequence: 9 givenname: Igor R. surname: Efimov fullname: Efimov, Igor R. |
| BackLink | https://www.ncbi.nlm.nih.gov/pubmed/32392258$$D View this record in MEDLINE/PubMed |
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| CitedBy_id | crossref_primary_10_1371_journal_pone_0244687 crossref_primary_10_1177_14604582231203757 crossref_primary_10_3389_fsysb_2023_1102467 crossref_primary_10_1113_JP285162 crossref_primary_10_1113_JP284011 crossref_primary_10_1515_rnam_2023_0011 crossref_primary_10_24193_adn_15_2_3 crossref_primary_10_3389_fphys_2022_879035 crossref_primary_10_1038_s41598_020_77076_0 crossref_primary_10_3389_fphys_2021_675867 crossref_primary_10_3389_fphys_2021_681943 crossref_primary_10_1098_rsos_230668 |
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| Copyright | COPYRIGHT 2020 Public Library of Science 2020 Smirnov et al. This is an open access article distributed under the terms of the Creative Commons Attribution License: http://creativecommons.org/licenses/by/4.0/ (the “License”), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited. Notwithstanding the ProQuest Terms and Conditions, you may use this content in accordance with the terms of the License. 2020 Smirnov et al 2020 Smirnov et al |
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| SubjectTerms | Action potential Action Potentials - genetics Action Potentials - physiology Algorithms Biology and Life Sciences Cardiomyocytes Convergence Customization Electrophysiology Engineering and Technology Gene Expression Gene mapping Genes Genetic algorithms Heart Heart - physiology Heart conduction system Heart rate Heart Transplantation Heart Ventricles - metabolism Humans Mapping Mathematical models Medicine and Health Sciences Messenger RNA Methods Models, Biological Mutation Myocytes, Cardiac - physiology Noise levels Novels Organisms Parameter modification Patch-Clamp Techniques Physical Sciences Physics Precision medicine Research and Analysis Methods Restitution RNA RNA-Seq Signal to noise ratio Simulation Tissue Donors Ventricle Waveforms |
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| Title | Genetic algorithm-based personalized models of human cardiac action potential |
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