All-Optical Electrophysiology Refines Populations of In Silico Human iPSC-CMs for Drug Evaluation

Michelangelo Paci; Elisa Passini; Aleksandra Klimas; Stefano Severi; Jari Hyttinen; Blanca Rodriguez; Emilia Entcheva

doi:10.1016/j.bpj.2020.03.018

All-Optical Electrophysiology Refines Populations of In Silico Human iPSC-CMs for Drug Evaluation

Michelangelo Paci
, Elisa Passini
, Aleksandra Klimas
, Stefano Severi
, Jari Hyttinen
, Blanca Rodriguez
, Emilia Entcheva

Tutkimustuotos: Artikkeli › Tieteellinen › vertaisarvioitu

62 Sitaatiot (Scopus)

19 Lataukset (Pure)

Abstrakti

High-throughput in vitro drug assays have been impacted by recent advances in human induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) technology and by contact-free all-optical systems simultaneously measuring action potentials (APs) and Ca²⁺ transients (CaTrs). Parallel computational advances have shown that in silico simulations can predict drug effects with high accuracy. We combine these in vitro and in silico technologies and demonstrate the utility of high-throughput experimental data to refine in silico hiPSC-CM populations and to predict and explain drug action mechanisms. Optically obtained hiPSC-CM APs and CaTrs were used from spontaneous activity and under optical pacing in control and drug conditions at multiple doses. An updated version of the Paci2018 model was developed to refine the description of hiPSC-CM spontaneous electrical activity: a population of in silico hiPSC-CMs was constructed and calibrated using simultaneously recorded APs and CaTrs. We tested in silico five drugs (astemizole, dofetilide, ibutilide, bepridil, and diltiazem) and compared the outcomes to in vitro optical recordings. Our simulations showed that physiologically accurate population of models can be obtained by integrating AP and CaTr control records. Thus, constructed population of models correctly predicted the drug effects and occurrence of adverse episodes, even though the population was optimized only based on control data and in vitro drug testing data were not deployed during its calibration. Furthermore, the in silico investigation yielded mechanistic insights: e.g., through simulations, bepridil's more proarrhythmic action in adult cardiomyocytes compared to hiPSC-CMs could be traced to the different expression of ion currents in the two. Therefore, our work 1) supports the utility of all-optical electrophysiology in providing high-content data to refine experimentally calibrated populations of in silico hiPSC-CMs, 2) offers insights into certain limitations when translating results obtained in hiPSC-CMs to humans, and 3) shows the strength of combining high-throughput in vitro and population in silico approaches.

Alkuperäiskieli	Englanti
Sivut	2596-2611
Sivumäärä	16
Julkaisu	Biophysical Journal
Vuosikerta	118
Numero	10
DOI - pysyväislinkit	https://doi.org/10.1016/j.bpj.2020.03.018
Tila	Julkaistu - 2020
OKM-julkaisutyyppi	A1 Alkuperäisartikkeli tieteellisessä aikakauslehdessä

Rahoitus

M.P. was supported by the Academy of Finland (decision number 307967 ). E.P. and B.R. were supported by an NC3Rs Infrastructure for Impact Award ( NC/P001076/1 ), a Wellcome Trust Senior Research Fellowship in Basic Biomedical Sciences ( 100246/Z/12/Z , 214290/Z/18/Z ), EPSRC Impact Acceleration Awards ( EP/K503769/1 ), the CompBioMed project (European Commission grant agreement No. 675451 and 823712 ), the Oxford BHF Centre of Research Excellence ( RE/08/004/23915 , RE/13/1/30181 ), and the TransQST project (Innovative Medicines Initiative 2 Joint Undertaking under grant agreement No. 116030 , receiving support from the European Union’s Horizon 2020 research and innovation programme and EFPIA). E.E. was supported by the National Institutes of Health ( R01HL144157 ) and the National Science Foundation ( 1827535 and 1830941 ).

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10.1016/j.bpj.2020.03.018

1-s2.0-S000634952030268X-mainFinal published version, 3,11 MBLisenssi: CC BY

http://urn.fi/urn:nbn:fi:tuni-202006236200

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abstract = "High-throughput in vitro drug assays have been impacted by recent advances in human induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) technology and by contact-free all-optical systems simultaneously measuring action potentials (APs) and Ca2+ transients (CaTrs). Parallel computational advances have shown that in silico simulations can predict drug effects with high accuracy. We combine these in vitro and in silico technologies and demonstrate the utility of high-throughput experimental data to refine in silico hiPSC-CM populations and to predict and explain drug action mechanisms. Optically obtained hiPSC-CM APs and CaTrs were used from spontaneous activity and under optical pacing in control and drug conditions at multiple doses. An updated version of the Paci2018 model was developed to refine the description of hiPSC-CM spontaneous electrical activity: a population of in silico hiPSC-CMs was constructed and calibrated using simultaneously recorded APs and CaTrs. We tested in silico five drugs (astemizole, dofetilide, ibutilide, bepridil, and diltiazem) and compared the outcomes to in vitro optical recordings. Our simulations showed that physiologically accurate population of models can be obtained by integrating AP and CaTr control records. Thus, constructed population of models correctly predicted the drug effects and occurrence of adverse episodes, even though the population was optimized only based on control data and in vitro drug testing data were not deployed during its calibration. Furthermore, the in silico investigation yielded mechanistic insights: e.g., through simulations, bepridil's more proarrhythmic action in adult cardiomyocytes compared to hiPSC-CMs could be traced to the different expression of ion currents in the two. Therefore, our work 1) supports the utility of all-optical electrophysiology in providing high-content data to refine experimentally calibrated populations of in silico hiPSC-CMs, 2) offers insights into certain limitations when translating results obtained in hiPSC-CMs to humans, and 3) shows the strength of combining high-throughput in vitro and population in silico approaches.",

author = "Michelangelo Paci and Elisa Passini and Aleksandra Klimas and Stefano Severi and Jari Hyttinen and Blanca Rodriguez and Emilia Entcheva",

year = "2020",

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T1 - All-Optical Electrophysiology Refines Populations of In Silico Human iPSC-CMs for Drug Evaluation

AU - Paci, Michelangelo

AU - Passini, Elisa

AU - Klimas, Aleksandra

AU - Severi, Stefano

AU - Hyttinen, Jari

AU - Rodriguez, Blanca

AU - Entcheva, Emilia

PY - 2020

Y1 - 2020

N2 - High-throughput in vitro drug assays have been impacted by recent advances in human induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) technology and by contact-free all-optical systems simultaneously measuring action potentials (APs) and Ca2+ transients (CaTrs). Parallel computational advances have shown that in silico simulations can predict drug effects with high accuracy. We combine these in vitro and in silico technologies and demonstrate the utility of high-throughput experimental data to refine in silico hiPSC-CM populations and to predict and explain drug action mechanisms. Optically obtained hiPSC-CM APs and CaTrs were used from spontaneous activity and under optical pacing in control and drug conditions at multiple doses. An updated version of the Paci2018 model was developed to refine the description of hiPSC-CM spontaneous electrical activity: a population of in silico hiPSC-CMs was constructed and calibrated using simultaneously recorded APs and CaTrs. We tested in silico five drugs (astemizole, dofetilide, ibutilide, bepridil, and diltiazem) and compared the outcomes to in vitro optical recordings. Our simulations showed that physiologically accurate population of models can be obtained by integrating AP and CaTr control records. Thus, constructed population of models correctly predicted the drug effects and occurrence of adverse episodes, even though the population was optimized only based on control data and in vitro drug testing data were not deployed during its calibration. Furthermore, the in silico investigation yielded mechanistic insights: e.g., through simulations, bepridil's more proarrhythmic action in adult cardiomyocytes compared to hiPSC-CMs could be traced to the different expression of ion currents in the two. Therefore, our work 1) supports the utility of all-optical electrophysiology in providing high-content data to refine experimentally calibrated populations of in silico hiPSC-CMs, 2) offers insights into certain limitations when translating results obtained in hiPSC-CMs to humans, and 3) shows the strength of combining high-throughput in vitro and population in silico approaches.

AB - High-throughput in vitro drug assays have been impacted by recent advances in human induced pluripotent stem cell-derived cardiomyocyte (hiPSC-CM) technology and by contact-free all-optical systems simultaneously measuring action potentials (APs) and Ca2+ transients (CaTrs). Parallel computational advances have shown that in silico simulations can predict drug effects with high accuracy. We combine these in vitro and in silico technologies and demonstrate the utility of high-throughput experimental data to refine in silico hiPSC-CM populations and to predict and explain drug action mechanisms. Optically obtained hiPSC-CM APs and CaTrs were used from spontaneous activity and under optical pacing in control and drug conditions at multiple doses. An updated version of the Paci2018 model was developed to refine the description of hiPSC-CM spontaneous electrical activity: a population of in silico hiPSC-CMs was constructed and calibrated using simultaneously recorded APs and CaTrs. We tested in silico five drugs (astemizole, dofetilide, ibutilide, bepridil, and diltiazem) and compared the outcomes to in vitro optical recordings. Our simulations showed that physiologically accurate population of models can be obtained by integrating AP and CaTr control records. Thus, constructed population of models correctly predicted the drug effects and occurrence of adverse episodes, even though the population was optimized only based on control data and in vitro drug testing data were not deployed during its calibration. Furthermore, the in silico investigation yielded mechanistic insights: e.g., through simulations, bepridil's more proarrhythmic action in adult cardiomyocytes compared to hiPSC-CMs could be traced to the different expression of ion currents in the two. Therefore, our work 1) supports the utility of all-optical electrophysiology in providing high-content data to refine experimentally calibrated populations of in silico hiPSC-CMs, 2) offers insights into certain limitations when translating results obtained in hiPSC-CMs to humans, and 3) shows the strength of combining high-throughput in vitro and population in silico approaches.

U2 - 10.1016/j.bpj.2020.03.018

DO - 10.1016/j.bpj.2020.03.018

M3 - Article

AN - SCOPUS:85083303522

SN - 0006-3495

VL - 118

SP - 2596

EP - 2611

JO - Biophysical Journal

JF - Biophysical Journal

IS - 10

ER -

All-Optical Electrophysiology Refines Populations of In Silico Human iPSC-CMs for Drug Evaluation

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