@article{699e1bf9736748fa8f26fb917dd98ee3,
title = "MAP4K4 Inhibition Promotes Survival of Human Stem Cell-Derived Cardiomyocytes and Reduces Infarct Size In Vivo",
abstract = "Heart disease is a paramount cause of global death and disability. Although cardiomyocyte death plays a causal role and its suppression would be logical, no clinical counter-measures target the responsible intracellular pathways. Therapeutic progress has been hampered by lack of preclinical human validation. Mitogen-activated protein kinase kinase kinase kinase-4 (MAP4K4) is activated in failing human hearts and relevant rodent models. Using human induced-pluripotent-stem-cell-derived cardiomyocytes (hiPSC-CMs) and MAP4K4 gene silencing, we demonstrate that death induced by oxidative stress requires MAP4K4. Consequently, we devised a small-molecule inhibitor, DMX-5804, that rescues cell survival, mitochondrial function, and calcium cycling in hiPSC-CMs. As proof of principle that drug discovery in hiPSC-CMs may predict efficacy in vivo, DMX-5804 reduces ischemia-reperfusion injury in mice by more than 50%. We implicate MAP4K4 as a well-posed target toward suppressing human cardiac cell death and highlight the utility of hiPSC-CMs in drug discovery to enhance cardiomyocyte survival. Using human iPSC-derived cardiomyocytes to enhance cardiac drug discovery, Fiedler et al. performed MAP4K4 target validation by gene silencing in this human model. MAP4K4 inhibitors augment human cardiomyocyte viability and function in 2D culture and 3D engineered heart tissue. An exemplar successfully reduces infarct size in proof-of-principle studies in mice.",
keywords = "apoptosis, cardiac muscle, drug discovery, heart, signal transduction",
author = "Fiedler, {Lorna R.} and Kathryn Chapman and Min Xie and Evie Maifoshie and Micaela Jenkins and Golforoush, {Pelin Arabacilar} and Mohamed Bellahcene and Michela Noseda and D{\"o}rte Faust and Ashley Jarvis and Gary Newton and Paiva, {Marta Abreu} and Mutsuo Harada and Stuckey, {Daniel J.} and Weihua Song and Josef Habib and Priyanka Narasimham and Rehan Aqil and Devika Sanmugalingam and Robert Yan and Lorenzo Pavanello and Motoaki Sano and Wang, {Sam C.} and Sampson, {Robert D.} and Sunthar Kanayaganam and Taffet, {George E.} and Michael, {Lloyd H.} and Entman, {Mark L.} and Tan, {Tse Hua} and Harding, {Sian E.} and Low, {Caroline M.R.} and Catherine Tralau-Stewart and Trevor Perrior and Schneider, {Michael D.}",
note = "Funding Information: We are grateful to the investigators cited for key reagents; F. al-Beidh, D. Zhang, X. Wang, W. Boerwinkle, L. Shirley, Q. Xiang, T. Pham, and J. Pocius for assistance; F. de Mayo and the Baylor College of Medicine Transgenic Mouse Core; S. Rothery and the Imperial Facility for Imaging by Light Microscopy; D. Alessi and staff of the Medical Research Council (MRC) Protein Phosphorylation and Ubiquitination Unit; and members of the British Heart Foundation (BHF) Centre for Research Excellence for discussions. This work was supported in part by the BHF (CH/08/002/29257, RE/08/002, RG/08/007, and SI/11/2/28875), European Commission (223372), European Research Council (233158), MRC-BHF Cardiovascular Stem Cell Research Strategic Development Grant (G0901467), MRC-Imperial Confidence in Concept Fund (MC PC 12015), NIH (R01 HL52555), and Wellcome Trust (WT10638 and WT205256). Conceptualization, M.D.S.; Methodology, R.A. K.C. D.F. L.R.F. S.E.H. A.J. M.J. C.M.R.L. E.M. G.N. D.S. M.S. M.D.S. C.T.-S. D.J.S. and M.X.; Formal Analysis, K.C. A.J. C.M.R.L. G.N. T.P. and C.T.-S.; Investigation, M.B. K.C. M.L.E. D.F. L.R.F. P.A.G. M.H. S.E.H. M.J. S.K. E.M. L.H.M. M.N. P.N. M.A.P. L.P. R.D.S. D.S. M.D.S. W.S. D.J.S. G.E.T. S.C.W. M.X. and R.Y.; Resources, T.-H.T. and M.D.S.; Writing – Original Draft, K.C. L.R.F. A.J. M.J. T.P. M.D.S. and M.X.; Writing – Review & Editing, K.C. L.R.F. M.J. G.N. T.P. M.D.S. and M.X.; Supervision, T.P. and M.D.S.; Project Administration, T.P. and M.D.S.; Funding Acquisition, M.D.S. M.D.S. declares patent applications related to this work (UK patent applications nos. 1716867.5 and 1819839.0; international patent application no. PCT/GB2018/052936). Funding Information: We are grateful to the investigators cited for key reagents; F. al-Beidh, D. Zhang, X. Wang, W. Boerwinkle, L. Shirley, Q. Xiang, T. Pham, and J. Pocius for assistance; F. de Mayo and the Baylor College of Medicine Transgenic Mouse Core; S. Rothery and the Imperial Facility for Imaging by Light Microscopy; D. Alessi and staff of the Medical Research Council (MRC) Protein Phosphorylation and Ubiquitination Unit; and members of the British Heart Foundation (BHF) Centre for Research Excellence for discussions. This work was supported in part by the BHF ( CH/08/002/29257 , RE/08/002 , RG/08/007 , and SI/11/2/28875 ), European Commission ( 223372 ), European Research Council ( 233158 ), MRC-BHF Cardiovascular Stem Cell Research Strategic Development Grant ( G0901467 ), MRC-Imperial Confidence in Concept Fund ( MC PC 12015 ), NIH ( R01 HL52555 ), and Wellcome Trust ( WT10638 and WT205256 ). Publisher Copyright: {\textcopyright} 2019 The Authors",
year = "2019",
month = apr,
day = "4",
doi = "10.1016/j.stem.2019.01.013",
language = "English (US)",
volume = "24",
pages = "579--591.e12",
journal = "Cell Stem Cell",
issn = "1934-5909",
publisher = "Cell Press",
number = "4",
}