| Literature DB >> 28132834 |
Carmen Lorenz1, Pierre Lesimple2, Raul Bukowiecki3, Annika Zink4, Gizem Inak3, Barbara Mlody3, Manvendra Singh3, Marcus Semtner3, Nancy Mah5, Karine Auré2, Megan Leong3, Oleksandr Zabiegalov3, Ekaterini-Maria Lyras5, Vanessa Pfiffer3, Beatrix Fauler6, Jenny Eichhorst7, Burkhard Wiesner7, Norbert Huebner3, Josef Priller8, Thorsten Mielke6, David Meierhofer6, Zsuzsanna Izsvák3, Jochen C Meier9, Frédéric Bouillaud2, James Adjaye10, Markus Schuelke5, Erich E Wanker3, Anne Lombès11, Alessandro Prigione12.
Abstract
Mitochondrial DNA (mtDNA) mutations frequently cause neurological diseases. Modeling of these defects has been difficult because of the challenges associated with engineering mtDNA. We show here that neural progenitor cells (NPCs) derived from human induced pluripotent stem cells (iPSCs) retain the parental mtDNA profile and exhibit a metabolic switch toward oxidative phosphorylation. NPCs derived in this way from patients carrying a deleterious homoplasmic mutation in the mitochondrial gene MT-ATP6 (m.9185T>C) showed defective ATP production and abnormally high mitochondrial membrane potential (MMP), plus altered calcium homeostasis, which represents a potential cause of neural impairment. High-content screening of FDA-approved drugs using the MMP phenotype highlighted avanafil, which we found was able to partially rescue the calcium defect in patient NPCs and differentiated neurons. Overall, our results show that iPSC-derived NPCs provide an effective model for drug screening to target mtDNA disorders that affect the nervous system.Entities:
Keywords: NPCs; calcium; drug discovery; iPSCs; induced pluripotent stem cells; metabolism; mitochondria; mitochondrial disorders; mtDNA mutations; neural progenitors
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Year: 2017 PMID: 28132834 DOI: 10.1016/j.stem.2016.12.013
Source DB: PubMed Journal: Cell Stem Cell ISSN: 1875-9777 Impact factor: 24.633