Characterization of cardiac metabolism in iPSC-derived cardiomyocytes: lessons from maturation and disease modeling

S. Vuckovic; R. Dinani; E.E. Nollet; D.W.D. Kuster; J.W. Buikema; R.H. Houtkooper; M. Nabben; J. van der Velden; B. Goversen

doi:10.1186/s13287-022-03021-9

Characterization of cardiac metabolism in iPSC-derived cardiomyocytes: lessons from maturation and disease modeling

S. Vuckovic, R. Dinani, E.E. Nollet, D.W.D. Kuster, J.W. Buikema, R.H. Houtkooper, M. Nabben, J. van der Velden, B. Goversen^*

^*Corresponding author for this work

Carim - Cardiomyopathy

Research output: Contribution to journal › (Systematic) Review article › peer-review

Abstract

Background Induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) have emerged as a powerful tool for disease modeling, though their immature nature currently limits translation into clinical practice. Maturation strategies increasingly pay attention to cardiac metabolism because of its pivotal role in cardiomyocyte development and function. Moreover, aberrances in cardiac metabolism are central to the pathogenesis of cardiac disease. Thus, proper modeling of human cardiac disease warrants careful characterization of the metabolic properties of iPSC-CMs. Methods Here, we examined the effect of maturation protocols on healthy iPSC-CMs applied in 23 studies and compared fold changes in functional metabolic characteristics to assess the level of maturation. In addition, pathological metabolic remodeling was assessed in 13 iPSC-CM studies that focus on hypertrophic cardiomyopathy (HCM), which is characterized by abnormalities in metabolism. Results Matured iPSC-CMs were characterized by mitochondrial maturation, increased oxidative capacity and enhanced fatty acid use for energy production. HCM iPSC-CMs presented varying degrees of metabolic remodeling ranging from compensatory to energy depletion stages, likely due to the different types of mutations and clinical phenotypes modeled. HCM further displayed early onset hypertrophy, independent of the type of mutation or disease stage. Conclusions Maturation strategies improve the metabolic characteristics of iPSC-CMs, but not to the level of the adult heart. Therefore, a combination of maturation strategies might prove to be more effective. Due to early onset hypertrophy, HCM iPSC-CMs may be less suitable to detect early disease modifiers in HCM and might prove more useful to examine the effects of gene editing and new drugs in advanced disease stages. With this review, we provide an overview of the assays used for characterization of cardiac metabolism in iPSC-CMs and advise on which metabolic assays to include in future maturation and disease modeling studies.

Original language	English
Article number	332
Number of pages	19
Journal	Stem Cell Research & Therapy
Volume	13
Issue number	1
DOIs	https://doi.org/10.1186/s13287-022-03021-9
Publication status	Published - 23 Jul 2022

Keywords

iPSC
Stem cells
Cardiomyocyte
Metabolism
Maturation
HCM
Disease modeling
PLURIPOTENT STEM-CELL
HYPERTROPHIC CARDIOMYOPATHY
ENERGY-METABOLISM
MITOCHONDRIAL
MECHANISM
CONTRACTION
SURVIVAL
STATE
AMPK

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@article{c35e1dd75cb443d99c57fad9fcb10ffa,

title = "Characterization of cardiac metabolism in iPSC-derived cardiomyocytes: lessons from maturation and disease modeling",

abstract = "Background Induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) have emerged as a powerful tool for disease modeling, though their immature nature currently limits translation into clinical practice. Maturation strategies increasingly pay attention to cardiac metabolism because of its pivotal role in cardiomyocyte development and function. Moreover, aberrances in cardiac metabolism are central to the pathogenesis of cardiac disease. Thus, proper modeling of human cardiac disease warrants careful characterization of the metabolic properties of iPSC-CMs. Methods Here, we examined the effect of maturation protocols on healthy iPSC-CMs applied in 23 studies and compared fold changes in functional metabolic characteristics to assess the level of maturation. In addition, pathological metabolic remodeling was assessed in 13 iPSC-CM studies that focus on hypertrophic cardiomyopathy (HCM), which is characterized by abnormalities in metabolism. Results Matured iPSC-CMs were characterized by mitochondrial maturation, increased oxidative capacity and enhanced fatty acid use for energy production. HCM iPSC-CMs presented varying degrees of metabolic remodeling ranging from compensatory to energy depletion stages, likely due to the different types of mutations and clinical phenotypes modeled. HCM further displayed early onset hypertrophy, independent of the type of mutation or disease stage. Conclusions Maturation strategies improve the metabolic characteristics of iPSC-CMs, but not to the level of the adult heart. Therefore, a combination of maturation strategies might prove to be more effective. Due to early onset hypertrophy, HCM iPSC-CMs may be less suitable to detect early disease modifiers in HCM and might prove more useful to examine the effects of gene editing and new drugs in advanced disease stages. With this review, we provide an overview of the assays used for characterization of cardiac metabolism in iPSC-CMs and advise on which metabolic assays to include in future maturation and disease modeling studies.",

keywords = "iPSC, Stem cells, Cardiomyocyte, Metabolism, Maturation, HCM, Disease modeling, PLURIPOTENT STEM-CELL, HYPERTROPHIC CARDIOMYOPATHY, ENERGY-METABOLISM, MITOCHONDRIAL, MECHANISM, CONTRACTION, SURVIVAL, STATE, AMPK",

author = "S. Vuckovic and R. Dinani and E.E. Nollet and D.W.D. Kuster and J.W. Buikema and R.H. Houtkooper and M. Nabben and {van der Velden}, J. and B. Goversen",

note = "Funding Information: This work is supported by funding from the Dutch Heart Foundation and Stichting Hartedroom CVON DOUBLE DOSE 2020B005 to D.W.D.K., M.N. and J.v.d.V, NWO VICI (NWO-ZonMW; 91818602 VICI) to J.v.d.V. and an Amsterdam UMC Innovation Impulse grant (2020) to R.H.H. and J.v.d.V. Publisher Copyright: {\textcopyright} 2022, The Author(s).",

year = "2022",

month = jul,

day = "23",

doi = "10.1186/s13287-022-03021-9",

language = "English",

volume = "13",

journal = "Stem Cell Research & Therapy",

issn = "1757-6512",

publisher = "BioMed Central",

number = "1",

}

TY - JOUR

T1 - Characterization of cardiac metabolism in iPSC-derived cardiomyocytes: lessons from maturation and disease modeling

AU - Vuckovic, S.

AU - Dinani, R.

AU - Nollet, E.E.

AU - Kuster, D.W.D.

AU - Buikema, J.W.

AU - Houtkooper, R.H.

AU - Nabben, M.

AU - van der Velden, J.

AU - Goversen, B.

N1 - Funding Information: This work is supported by funding from the Dutch Heart Foundation and Stichting Hartedroom CVON DOUBLE DOSE 2020B005 to D.W.D.K., M.N. and J.v.d.V, NWO VICI (NWO-ZonMW; 91818602 VICI) to J.v.d.V. and an Amsterdam UMC Innovation Impulse grant (2020) to R.H.H. and J.v.d.V. Publisher Copyright: © 2022, The Author(s).

PY - 2022/7/23

Y1 - 2022/7/23

N2 - Background Induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) have emerged as a powerful tool for disease modeling, though their immature nature currently limits translation into clinical practice. Maturation strategies increasingly pay attention to cardiac metabolism because of its pivotal role in cardiomyocyte development and function. Moreover, aberrances in cardiac metabolism are central to the pathogenesis of cardiac disease. Thus, proper modeling of human cardiac disease warrants careful characterization of the metabolic properties of iPSC-CMs. Methods Here, we examined the effect of maturation protocols on healthy iPSC-CMs applied in 23 studies and compared fold changes in functional metabolic characteristics to assess the level of maturation. In addition, pathological metabolic remodeling was assessed in 13 iPSC-CM studies that focus on hypertrophic cardiomyopathy (HCM), which is characterized by abnormalities in metabolism. Results Matured iPSC-CMs were characterized by mitochondrial maturation, increased oxidative capacity and enhanced fatty acid use for energy production. HCM iPSC-CMs presented varying degrees of metabolic remodeling ranging from compensatory to energy depletion stages, likely due to the different types of mutations and clinical phenotypes modeled. HCM further displayed early onset hypertrophy, independent of the type of mutation or disease stage. Conclusions Maturation strategies improve the metabolic characteristics of iPSC-CMs, but not to the level of the adult heart. Therefore, a combination of maturation strategies might prove to be more effective. Due to early onset hypertrophy, HCM iPSC-CMs may be less suitable to detect early disease modifiers in HCM and might prove more useful to examine the effects of gene editing and new drugs in advanced disease stages. With this review, we provide an overview of the assays used for characterization of cardiac metabolism in iPSC-CMs and advise on which metabolic assays to include in future maturation and disease modeling studies.

AB - Background Induced pluripotent stem cell-derived cardiomyocytes (iPSC-CMs) have emerged as a powerful tool for disease modeling, though their immature nature currently limits translation into clinical practice. Maturation strategies increasingly pay attention to cardiac metabolism because of its pivotal role in cardiomyocyte development and function. Moreover, aberrances in cardiac metabolism are central to the pathogenesis of cardiac disease. Thus, proper modeling of human cardiac disease warrants careful characterization of the metabolic properties of iPSC-CMs. Methods Here, we examined the effect of maturation protocols on healthy iPSC-CMs applied in 23 studies and compared fold changes in functional metabolic characteristics to assess the level of maturation. In addition, pathological metabolic remodeling was assessed in 13 iPSC-CM studies that focus on hypertrophic cardiomyopathy (HCM), which is characterized by abnormalities in metabolism. Results Matured iPSC-CMs were characterized by mitochondrial maturation, increased oxidative capacity and enhanced fatty acid use for energy production. HCM iPSC-CMs presented varying degrees of metabolic remodeling ranging from compensatory to energy depletion stages, likely due to the different types of mutations and clinical phenotypes modeled. HCM further displayed early onset hypertrophy, independent of the type of mutation or disease stage. Conclusions Maturation strategies improve the metabolic characteristics of iPSC-CMs, but not to the level of the adult heart. Therefore, a combination of maturation strategies might prove to be more effective. Due to early onset hypertrophy, HCM iPSC-CMs may be less suitable to detect early disease modifiers in HCM and might prove more useful to examine the effects of gene editing and new drugs in advanced disease stages. With this review, we provide an overview of the assays used for characterization of cardiac metabolism in iPSC-CMs and advise on which metabolic assays to include in future maturation and disease modeling studies.

KW - iPSC

KW - Stem cells

KW - Cardiomyocyte

KW - Metabolism

KW - Maturation

KW - HCM

KW - Disease modeling

KW - PLURIPOTENT STEM-CELL

KW - HYPERTROPHIC CARDIOMYOPATHY

KW - ENERGY-METABOLISM

KW - MITOCHONDRIAL

KW - MECHANISM

KW - CONTRACTION

KW - SURVIVAL

KW - STATE

KW - AMPK

U2 - 10.1186/s13287-022-03021-9

DO - 10.1186/s13287-022-03021-9

M3 - (Systematic) Review article

C2 - 35870954

SN - 1757-6512

VL - 13

JO - Stem Cell Research & Therapy

JF - Stem Cell Research & Therapy

IS - 1

M1 - 332

ER -