Programmed mitophagy is essential for the glycolytic switch during cell differentiation

Lorena Esteban-Martínez; Elena Sierra-Filardi; Rebecca S. McGreal; María Salazar-Roa; Guillermo Mariño; Esther Seco; Sylvère Durand; David Enot; Osvaldo Graña; Marcos Malumbres; Ales Cvekl; Ana María Cuervo; Guido Kroemer; Patricia Boya

doi:10.15252/embj.201695916

Programmed mitophagy is essential for the glycolytic switch during cell differentiation

Lorena Esteban-Martínez, Elena Sierra-Filardi, Rebecca S. McGreal, María Salazar-Roa, Guillermo Mariño, Esther Seco, Sylvère Durand, David Enot, Osvaldo Graña, Marcos Malumbres, Ales Cvekl, Ana María Cuervo, Guido Kroemer, Patricia Boya

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209 Scopus citations

Abstract

Retinal ganglion cells (RGCs) are the sole projecting neurons of the retina and their axons form the optic nerve. Here, we show that embryogenesis-associated mouse RGC differentiation depends on mitophagy, the programmed autophagic clearance of mitochondria. The elimination of mitochondria during RGC differentiation was coupled to a metabolic shift with increased lactate production and elevated expression of glycolytic enzymes at the mRNA level. Pharmacological and genetic inhibition of either mitophagy or glycolysis consistently inhibited RGC differentiation. Local hypoxia triggered expression of the mitophagy regulator BCL2/adenovirus E1B 19-kDa-interacting protein 3-like (BNIP3L, best known as NIX) at peak RGC differentiation. Retinas from NIX-deficient mice displayed increased mitochondrial mass, reduced expression of glycolytic enzymes and decreased neuronal differentiation. Similarly, we provide evidence that NIX-dependent mitophagy contributes to mitochondrial elimination during macrophage polarization towards the proinflammatory and more glycolytic M1 phenotype, but not to M2 macrophage differentiation, which primarily relies on oxidative phosphorylation. In summary, developmentally controlled mitophagy promotes a metabolic switch towards glycolysis, which in turn contributes to cellular differentiation in several distinct developmental contexts.

Original language	English (US)
Pages (from-to)	1688-1706
Number of pages	19
Journal	EMBO Journal
Volume	36
Issue number	12
DOIs	https://doi.org/10.15252/embj.201695916
State	Published - Jun 14 2017

Keywords

BNIP3L/NIX
hypoxia
macrophages
metabolic reprogramming
retinal ganglion cells

ASJC Scopus subject areas

Neuroscience(all)
Molecular Biology
Biochemistry, Genetics and Molecular Biology(all)
Immunology and Microbiology(all)

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10.15252/embj.201695916

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@article{c72f6c54fdde469385b6792111a68833,

title = "Programmed mitophagy is essential for the glycolytic switch during cell differentiation",

abstract = "Retinal ganglion cells (RGCs) are the sole projecting neurons of the retina and their axons form the optic nerve. Here, we show that embryogenesis-associated mouse RGC differentiation depends on mitophagy, the programmed autophagic clearance of mitochondria. The elimination of mitochondria during RGC differentiation was coupled to a metabolic shift with increased lactate production and elevated expression of glycolytic enzymes at the mRNA level. Pharmacological and genetic inhibition of either mitophagy or glycolysis consistently inhibited RGC differentiation. Local hypoxia triggered expression of the mitophagy regulator BCL2/adenovirus E1B 19-kDa-interacting protein 3-like (BNIP3L, best known as NIX) at peak RGC differentiation. Retinas from NIX-deficient mice displayed increased mitochondrial mass, reduced expression of glycolytic enzymes and decreased neuronal differentiation. Similarly, we provide evidence that NIX-dependent mitophagy contributes to mitochondrial elimination during macrophage polarization towards the proinflammatory and more glycolytic M1 phenotype, but not to M2 macrophage differentiation, which primarily relies on oxidative phosphorylation. In summary, developmentally controlled mitophagy promotes a metabolic switch towards glycolysis, which in turn contributes to cellular differentiation in several distinct developmental contexts.",

keywords = "BNIP3L/NIX, hypoxia, macrophages, metabolic reprogramming, retinal ganglion cells",

author = "Lorena Esteban-Mart{\'i}nez and Elena Sierra-Filardi and McGreal, {Rebecca S.} and Mar{\'i}a Salazar-Roa and Guillermo Mari{\~n}o and Esther Seco and Sylv{\`e}re Durand and David Enot and Osvaldo Gra{\~n}a and Marcos Malumbres and Ales Cvekl and Cuervo, {Ana Mar{\'i}a} and Guido Kroemer and Patricia Boya",

note = "Funding Information: Research in P.B. laboratory is supported by grants BFU2015-65623, BFU2015-71869-REDT from Spain's Ministerio de Econom{\'i}a y Competitividad and I-link 0701 (to P.B. and A.M.C.) from CSIC. L.E.M. was recipient of a JAE-Pre grant from CSIC. G.M. is funded by the Ram{\'o}n y Cajal Program (RYC-2013-12751), supported by Spain's Ministerio de Econom{\'i}a y Competitividad (BFU2015-68539) and the BBVA Foundation (BBM_BIO_3105). GK is supported by the Ligue Contre le Cancer ({\'e}quipe labelis{\'e}e); Agence National de la Recherche (ANR)—Projets blancs; ANR under the framework of E-Rare-2, the ERA-Net for Research on Rare Diseases; Association Pour la Recherche sur le Cancer (ARC); Canc{\'e}rop{\^o}le Ile-de-France; Institut National du Cancer (INCa); Institut Universitaire de France; Fondation pour la Recherche M{\'e}dicale (FRM); the European Commission (ArtForce); the European Research Council (ERC); the LeDucq Foundation; the LabEx Immuno-Oncology; the SIRIC Stratified Oncology Cell DNA Repair and Tumor Immune Elimination (SOCRATE); the SIRIC Cancer Research and Personalized Medicine (CARPEM); and the Paris Alliance of Cancer Research Institutes (PACRI). A.C. research is supported by NIH grants EY012200 and EY014237. M.S.R. was supported by the Asociaci{\'o}n Espa{\~n}ola contra el C{\'a}ncer (AECC, AIOA120833SALA). Work in the M.M. laboratory was supported by grants from the MINECO: (SAF2015-69920-R), Consolider-Ingenio 2010 Programme (SAF2014-57791-REDC), Excellence Network CellSYS (BFU2014-52125-REDT) and the OncoCycle Programme (S2010/BMD-2470) from the Comunidad de Madrid. We thank N. Marsh-Armstrong and S. Martin-Puig for reagents; O. Howard for English-language editing; M. Casas for graphical abstract artwork; E. Rial for reagents and Seahorse analysis; and A. Corbi, T. Su{\'a}rez, H.L. Vieira, A. Zorzano, J.M. Sanchez-Puelles, M. Mor{\'a}n, I. Lopez-Sanchez and I. Trounce for discussion. Publisher Copyright: {\textcopyright} 2017 The Authors",

year = "2017",

month = jun,

day = "14",

doi = "10.15252/embj.201695916",

language = "English (US)",

volume = "36",

pages = "1688--1706",

journal = "EMBO Journal",

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T1 - Programmed mitophagy is essential for the glycolytic switch during cell differentiation

AU - Esteban-Martínez, Lorena

AU - Sierra-Filardi, Elena

AU - McGreal, Rebecca S.

AU - Salazar-Roa, María

AU - Mariño, Guillermo

AU - Seco, Esther

AU - Durand, Sylvère

AU - Enot, David

AU - Graña, Osvaldo

AU - Malumbres, Marcos

AU - Cvekl, Ales

AU - Cuervo, Ana María

AU - Kroemer, Guido

AU - Boya, Patricia

N1 - Funding Information: Research in P.B. laboratory is supported by grants BFU2015-65623, BFU2015-71869-REDT from Spain's Ministerio de Economía y Competitividad and I-link 0701 (to P.B. and A.M.C.) from CSIC. L.E.M. was recipient of a JAE-Pre grant from CSIC. G.M. is funded by the Ramón y Cajal Program (RYC-2013-12751), supported by Spain's Ministerio de Economía y Competitividad (BFU2015-68539) and the BBVA Foundation (BBM_BIO_3105). GK is supported by the Ligue Contre le Cancer (équipe labelisée); Agence National de la Recherche (ANR)—Projets blancs; ANR under the framework of E-Rare-2, the ERA-Net for Research on Rare Diseases; Association Pour la Recherche sur le Cancer (ARC); Cancéropôle Ile-de-France; Institut National du Cancer (INCa); Institut Universitaire de France; Fondation pour la Recherche Médicale (FRM); the European Commission (ArtForce); the European Research Council (ERC); the LeDucq Foundation; the LabEx Immuno-Oncology; the SIRIC Stratified Oncology Cell DNA Repair and Tumor Immune Elimination (SOCRATE); the SIRIC Cancer Research and Personalized Medicine (CARPEM); and the Paris Alliance of Cancer Research Institutes (PACRI). A.C. research is supported by NIH grants EY012200 and EY014237. M.S.R. was supported by the Asociación Española contra el Cáncer (AECC, AIOA120833SALA). Work in the M.M. laboratory was supported by grants from the MINECO: (SAF2015-69920-R), Consolider-Ingenio 2010 Programme (SAF2014-57791-REDC), Excellence Network CellSYS (BFU2014-52125-REDT) and the OncoCycle Programme (S2010/BMD-2470) from the Comunidad de Madrid. We thank N. Marsh-Armstrong and S. Martin-Puig for reagents; O. Howard for English-language editing; M. Casas for graphical abstract artwork; E. Rial for reagents and Seahorse analysis; and A. Corbi, T. Suárez, H.L. Vieira, A. Zorzano, J.M. Sanchez-Puelles, M. Morán, I. Lopez-Sanchez and I. Trounce for discussion. Publisher Copyright: © 2017 The Authors

PY - 2017/6/14

Y1 - 2017/6/14

N2 - Retinal ganglion cells (RGCs) are the sole projecting neurons of the retina and their axons form the optic nerve. Here, we show that embryogenesis-associated mouse RGC differentiation depends on mitophagy, the programmed autophagic clearance of mitochondria. The elimination of mitochondria during RGC differentiation was coupled to a metabolic shift with increased lactate production and elevated expression of glycolytic enzymes at the mRNA level. Pharmacological and genetic inhibition of either mitophagy or glycolysis consistently inhibited RGC differentiation. Local hypoxia triggered expression of the mitophagy regulator BCL2/adenovirus E1B 19-kDa-interacting protein 3-like (BNIP3L, best known as NIX) at peak RGC differentiation. Retinas from NIX-deficient mice displayed increased mitochondrial mass, reduced expression of glycolytic enzymes and decreased neuronal differentiation. Similarly, we provide evidence that NIX-dependent mitophagy contributes to mitochondrial elimination during macrophage polarization towards the proinflammatory and more glycolytic M1 phenotype, but not to M2 macrophage differentiation, which primarily relies on oxidative phosphorylation. In summary, developmentally controlled mitophagy promotes a metabolic switch towards glycolysis, which in turn contributes to cellular differentiation in several distinct developmental contexts.

AB - Retinal ganglion cells (RGCs) are the sole projecting neurons of the retina and their axons form the optic nerve. Here, we show that embryogenesis-associated mouse RGC differentiation depends on mitophagy, the programmed autophagic clearance of mitochondria. The elimination of mitochondria during RGC differentiation was coupled to a metabolic shift with increased lactate production and elevated expression of glycolytic enzymes at the mRNA level. Pharmacological and genetic inhibition of either mitophagy or glycolysis consistently inhibited RGC differentiation. Local hypoxia triggered expression of the mitophagy regulator BCL2/adenovirus E1B 19-kDa-interacting protein 3-like (BNIP3L, best known as NIX) at peak RGC differentiation. Retinas from NIX-deficient mice displayed increased mitochondrial mass, reduced expression of glycolytic enzymes and decreased neuronal differentiation. Similarly, we provide evidence that NIX-dependent mitophagy contributes to mitochondrial elimination during macrophage polarization towards the proinflammatory and more glycolytic M1 phenotype, but not to M2 macrophage differentiation, which primarily relies on oxidative phosphorylation. In summary, developmentally controlled mitophagy promotes a metabolic switch towards glycolysis, which in turn contributes to cellular differentiation in several distinct developmental contexts.

KW - BNIP3L/NIX

KW - hypoxia

KW - macrophages

KW - metabolic reprogramming

KW - retinal ganglion cells

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U2 - 10.15252/embj.201695916

DO - 10.15252/embj.201695916

M3 - Article

C2 - 28465321

AN - SCOPUS:85018982980

SN - 0261-4189

VL - 36

SP - 1688

EP - 1706

JO - EMBO Journal

JF - EMBO Journal

IS - 12

ER -

Programmed mitophagy is essential for the glycolytic switch during cell differentiation

Abstract

Keywords

ASJC Scopus subject areas

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