2019
DOI: 10.1016/j.stem.2019.01.013
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MAP4K4 Inhibition Promotes Survival of Human Stem Cell-Derived Cardiomyocytes and Reduces Infarct Size In Vivo

Abstract: Highlights d Human iPSC-cardiomyocytes were used for MAP4K4 target validation and drug discovery d MAP4K4 shRNA protects hiPSC-cardiomyocytes from lethal oxidative stress d MAP4K4 inhibitors promote hiPSC-cardiomyocyte survival and function d MAP4K4 inhibition markedly reduces cardiac ischemiareperfusion injury in mice

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Cited by 68 publications
(72 citation statements)
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“…Although hPSC-CMs represent a scalable human platform for cardiac drug discovery reproducing many relevant features of cardiomyocytes' function, a few cautionary notes need to be highlighted. Cells used here include vCor4U that enrich for ventricular cardiomyocytes 23 , the relevant cells in a model of ischemic injury. Our RNA-seq data indicate that IMR-90 express cardiomyocytes' structural and functional genes in the absence of reprogramming genes, a proliferation signature or fibroblast markers.…”
Section: Discussionmentioning
confidence: 99%
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“…Although hPSC-CMs represent a scalable human platform for cardiac drug discovery reproducing many relevant features of cardiomyocytes' function, a few cautionary notes need to be highlighted. Cells used here include vCor4U that enrich for ventricular cardiomyocytes 23 , the relevant cells in a model of ischemic injury. Our RNA-seq data indicate that IMR-90 express cardiomyocytes' structural and functional genes in the absence of reprogramming genes, a proliferation signature or fibroblast markers.…”
Section: Discussionmentioning
confidence: 99%
“…Co-cultures were exposed to menadione, a naphthoquinone that induces endogenous reactive oxygen species (ROS) 32 , instrumental mediators of ischemia-reperfusion injury as in myocardial infarction ( Supplementary Fig. S1) 23,33,34 . As shown by the 56.5% inhibition of DRAQ7 uptake, co-culture with cMSCs protected the human cardiomyocytes from cell death after oxidative stress (p = 0.0007; Fig.…”
Section: Suppression Of Cell Death By Mouse Cmsc In Human Cardiomyocymentioning
confidence: 99%
“…Priming hPSC-CMs through simple maturation steps generates cells responsive to I/R with mortality rates unseen in their unprimed counterparts, ultimately providing the biological model needed to test clinically effective small molecules (Hidalgo et al, 2018) or investigate the cardioprotective mechanism of cardiac progenitors (Sebastiao et al, 2019). The most intriguing example of in vitro I/R modeling to date fully embraces hPSC-CMs as platform for both drug screening and development (Fiedler et al, 2019). The researchers identify MAP4K4 as a druggable target, activity of which is altered across several clinically relevant heart failure models, and employ an I/R setup with primed hPSC-CMs to screen for suitable small-molecule inhibitors.…”
Section: Ischemia/reperfusion Injury Modelingmentioning
confidence: 99%
“…Currently, advanced modeling of the adult myocardium requires hEHTs. These multiparametric setups integrating stimulation and data acquisition systems, act as human preclinical models refining the predictive efficacy of less throughput-limited 2D hPSC-CM models (Fiedler et al, 2019). Nevertheless, while closely resembling adult tissue transcriptomic and functional features, hEHTs fall short of gaining the status of full-fledged organoids, not fully mimicking adult myocardial macroscopic ultrastructure (Tiburcy et al, 2017;Ronaldson-Bouchard et al, 2018), thus requiring additional bioengineering efforts to scale up the systems from tissue-to organ-models, as the recently proposed atrioventricular composite (Zhao et al, 2019).…”
Section: Conclusion and Future Perspectivesmentioning
confidence: 99%
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