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dc.contributor.author
Vandoorne, Tijs
dc.contributor.author
Veys, Koen
dc.contributor.author
Guo, Wenting
dc.contributor.author
Sicart, Adria
dc.contributor.author
Vints, Katlijn
dc.contributor.author
Swijsen, Ann
dc.contributor.author
Moisse, Matthieu
dc.contributor.author
Eelen, Guy
dc.contributor.author
Gounko, Natalia V.
dc.contributor.author
Fumagalli, Laura
dc.contributor.author
Fazal, Raheem
dc.contributor.author
Germeys, Christine
dc.contributor.author
Quaegebeur, Annelies
dc.contributor.author
Fendt, Sarah-Maria
dc.contributor.author
Carmeliet, Peter
dc.contributor.author
Verfaillie, Catherine
dc.contributor.author
Van Damme, Philip
dc.contributor.author
Ghesquière, Bart
dc.contributor.author
De Bock, Katrien
dc.contributor.author
Van Den Bosch, Ludo
dc.date.accessioned
2020-01-09T09:42:54Z
dc.date.available
2020-01-09T09:42:54Z
dc.date.issued
2019-09-12
dc.identifier.issn
2041-1723
dc.identifier.other
10.1038/s41467-019-12099-4
en_US
dc.identifier.uri
http://hdl.handle.net/20.500.11850/388812
dc.identifier.doi
10.3929/ethz-b-000365432
dc.description.abstract
Energy metabolism has been repeatedly linked to amyotrophic lateral sclerosis (ALS). Yet, motor neuron (MN) metabolism remains poorly studied and it is unknown if ALS MNs differ metabolically from healthy MNs. To address this question, we first performed a metabolic characterization of induced pluripotent stem cells (iPSCs) versus iPSC-derived MNs and subsequently compared MNs from ALS patients carrying FUS mutations to their CRISPR/Cas9-corrected counterparts. We discovered that human iPSCs undergo a lactate oxidation-fuelled prooxidative metabolic switch when they differentiate into functional MNs. Simultaneously, they rewire metabolic routes to import pyruvate into the TCA cycle in an energy substrate specific way. By comparing patient-derived MNs and their isogenic controls, we show that ALS-causing mutations in FUS did not affect glycolytic or mitochondrial energy metabolism of human MNs in vitro. These data show that metabolic dysfunction is not the underlying cause of the ALS-related phenotypes previously observed in these MNs.
en_US
dc.format
application/pdf
en_US
dc.language.iso
en
en_US
dc.publisher
Nature
dc.rights.uri
http://creativecommons.org/licenses/by/4.0/
dc.title
Differentiation but not ALS mutations in FUS rewires motor neuron metabolism
en_US
dc.type
Journal Article
dc.rights.license
Creative Commons Attribution 4.0 International
ethz.journal.title
Nature Communications
ethz.journal.volume
10
en_US
ethz.journal.issue
1
en_US
ethz.journal.abbreviated
Nat Commun
ethz.pages.start
4147
en_US
ethz.size
12 p.
en_US
ethz.version.deposit
publishedVersion
en_US
ethz.identifier.wos
ethz.identifier.scopus
ethz.publication.place
London
ethz.publication.status
published
en_US
ethz.leitzahl
ETH Zürich::00002 - ETH Zürich::00012 - Lehre und Forschung::00007 - Departemente::02070 - Dep. Gesundheitswiss. und Technologie / Dep. of Health Sciences and Technology::02535 - Institut für Bewegungswiss. und Sport / Institut of Human Movement Sc. and Sport::09560 - De Bock, Katrien / De Bock, Katrien
en_US
ethz.leitzahl.certified
ETH Zürich::00002 - ETH Zürich::00012 - Lehre und Forschung::00007 - Departemente::02070 - Dep. Gesundheitswiss. und Technologie / Dep. of Health Sciences and Technology::02535 - Institut für Bewegungswiss. und Sport / Institut of Human Movement Sc. and Sport::09560 - De Bock, Katrien / De Bock, Katrien
en_US
ethz.date.deposited
2019-09-20T03:11:06Z
ethz.source
SCOPUS
ethz.source
FORM
ethz.eth
yes
en_US
ethz.availability
Open access
en_US
ethz.rosetta.installDate
2020-01-09T09:43:07Z
ethz.rosetta.lastUpdated
2024-02-02T10:06:03Z
ethz.rosetta.versionExported
true
dc.identifier.olduri
http://hdl.handle.net/20.500.11850/365432
dc.identifier.olduri
http://hdl.handle.net/20.500.11850/388617
ethz.COinS
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