Netrin-1 promotes naive pluripotency through Neo1 and Unc5b co-regulation of Wnt and MAPK signalling

被引:0
|
作者
Aurélia Huyghe
Giacomo Furlan
Duygu Ozmadenci
Christina Galonska
Jocelyn Charlton
Xavier Gaume
Noémie Combémorel
Christina Riemenschneider
Nicolas Allègre
Jenny Zhang
Pauline Wajda
Nicolas Rama
Pauline Vieugué
Isabelle Durand
Marie Brevet
Nicolas Gadot
Thomas Imhof
Bradley J. Merrill
Manuel Koch
Patrick Mehlen
Claire Chazaud
Alexander Meissner
Fabrice Lavial
机构
[1] Labex DEVweCAN,Cellular Reprogramming and Oncogenesis Laboratory, Equipe labellisée la Ligue contre le cancer
[2] Université de Lyon,Department of Genome Regulation
[3] Université Claude Bernard Lyon 1,Department of Stem Cell and Regenerative Biology
[4] INSERM 1052,GReD
[5] CNRS 5286,Department of Biochemistry and Molecular Genetics
[6] Centre Léon Bérard,Apoptosis, Cancer and Development Laboratory
[7] Centre de recherche en cancérologie de Lyon,Cytometry Facility
[8] Max Planck Institute for Molecular Genetics,Research Pathology platform, Department of translational research and innovation
[9] Broad Institute of MIT and Harvard,Institute for Dental Research and Oral Musculoskeletal Research, Center for Biochemistry
[10] Harvard Stem Cell Institute,Department of Translational Research and Innovation
[11] Harvard University,undefined
[12] Université Clermont Auvergne,undefined
[13] CNRS,undefined
[14] INSERM,undefined
[15] BP38,undefined
[16] University of Illinois at Chicago,undefined
[17] Université de Lyon,undefined
[18] Université Claude Bernard Lyon 1,undefined
[19] INSERM 1052,undefined
[20] CNRS 5286,undefined
[21] Centre Léon Bérard,undefined
[22] Centre de recherche en cancérologie de Lyon,undefined
[23] Université de Lyon,undefined
[24] Université Claude Bernard Lyon 1,undefined
[25] Centre Léon Bérard,undefined
[26] Centre de recherche en cancérologie de Lyon,undefined
[27] INSERM 1052,undefined
[28] CNRS 5286,undefined
[29] Centre Léon Bérard,undefined
[30] University of Cologne,undefined
[31] Centre Léon Bérard,undefined
来源
Nature Cell Biology | 2020年 / 22卷
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摘要
In mouse embryonic stem cells (mESCs), chemical blockade of Gsk3α/β and Mek1/2 (2i) instructs a self-renewing ground state whose endogenous inducers are unknown. Here we show that the axon guidance cue Netrin-1 promotes naive pluripotency by triggering profound signalling, transcriptomic and epigenetic changes in mESCs. Furthermore, we demonstrate that Netrin-1 can substitute for blockade of Gsk3α/β and Mek1/2 to sustain self-renewal of mESCs in combination with leukaemia inhibitory factor and regulates the formation of the mouse pluripotent blastocyst. Mechanistically, we reveal how Netrin-1 and the balance of its receptors Neo1 and Unc5B co-regulate Wnt and MAPK pathways in both mouse and human ESCs. Netrin-1 induces Fak kinase to inactivate Gsk3α/β and stabilize β-catenin while increasing the phosphatase activity of a Ppp2r2c-containing Pp2a complex to reduce Erk1/2 activity. Collectively, this work identifies Netrin-1 as a regulator of pluripotency and reveals that it mediates different effects in mESCs depending on its receptor dosage, opening perspectives for balancing self-renewal and lineage commitment.
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页码:389 / 400
页数:11
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