Altering metabolism programs cell identity via NAD+-dependent deacetylation

Robert A. Bone; Molly P. Lowndes; Silvia Raineri; Alba R Riveiro; Sarah L. Lundregan; Morten Dall; Karolina Sulek; Jose A.H. Romero; Luna Malzard; Sandra Koigi; Indra J. Heckenbach; Victor Solis-Mezarino; Moritz Völker-Albert; Catherine G. Vasilopoulou; Florian Meier; Ala Trusina; Matthias Mann; Michael L Nielsen; Jonas T. Treebak; Joshua M. Brickman

doi:10.1038/s44318-025-00417-0

Altering metabolism programs cell identity via NAD⁺-dependent deacetylation

Robert A. Bone, Molly P. Lowndes, Silvia Raineri, Alba R Riveiro, Sarah L. Lundregan, Morten Dall, Karolina Sulek, Jose A.H. Romero, Luna Malzard, Sandra Koigi, Indra J. Heckenbach, Victor Solis-Mezarino, Moritz Völker-Albert, Catherine G. Vasilopoulou, Florian Meier, Ala Trusina, Matthias Mann, Michael L Nielsen, Jonas T. Treebak, Joshua M. Brickman^*

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

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Abstract

Cells change their metabolic profiles in response to underlying gene regulatory networks, but how can alterations in metabolism encode specific transcriptional instructions? Here, we show that forcing a metabolic change in embryonic stem cells (ESCs) promotes a developmental identity that better approximates the inner cell mass (ICM) of the early mammalian blastocyst in cultures. This shift in cellular identity depends on the inhibition of glycolysis and stimulation of oxidative phosphorylation (OXPHOS) triggered by the replacement of d-glucose by d-galactose in ESC media. Enhanced OXPHOS in turn activates NAD + -dependent deacetylases of the Sirtuin family, resulting in the deacetylation of histones and key transcription factors to focus enhancer activity while reducing transcriptional noise, which results in a robustly enhanced ESC phenotype. This exploitation of a NAD + /NADH coenzyme coupled to OXPHOS as a means of programming lineage-specific transcription suggests new paradigms for how cells respond to alterations in their environment, and implies cellular rejuvenation exploits enzymatic activities for simultaneous activation of a discrete enhancer set alongside silencing genome-wide transcriptional noise.

Originalsprog	Engelsk
Tidsskrift	EMBO Journal
Vol/bind	44
Udgave nummer	11
Sider (fra-til)	3056-3084
ISSN	0261-4189
DOI	https://doi.org/10.1038/s44318-025-00417-0
Status	Udgivet - 2025

Bibliografisk note

Publisher Copyright:
© The Author(s) 2025.

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10.1038/s44318-025-00417-0Licens: CC BY

FulltextForlagets udgivne version, 8,81 MBLicens: CC BY

Citationsformater

Bone, R. A., Lowndes, M. P., Raineri, S., R Riveiro, A., Lundregan, S. L., Dall, M., Sulek, K., Romero, J. A. H., Malzard, L., Koigi, S., Heckenbach, I. J., Solis-Mezarino, V., Völker-Albert, M., Vasilopoulou, C. G., Meier, F., Trusina, A., Mann, M., L Nielsen, M., Treebak, J. T., & Brickman, J. M. (2025). Altering metabolism programs cell identity via NAD⁺-dependent deacetylation. EMBO Journal, 44(11), 3056-3084. https://doi.org/10.1038/s44318-025-00417-0

Bone, RA , Lowndes, MP , Raineri, S, R Riveiro, A, Lundregan, SL, Dall, M, Sulek, K, Romero, JAH, Malzard, L, Koigi, S, Heckenbach, IJ, Solis-Mezarino, V, Völker-Albert, M, Vasilopoulou, CG, Meier, F, Trusina, A , Mann, M , L Nielsen, M , Treebak, JT & Brickman, JM 2025, 'Altering metabolism programs cell identity via NAD⁺-dependent deacetylation', EMBO Journal, bind 44, nr. 11, s. 3056-3084. https://doi.org/10.1038/s44318-025-00417-0

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title = "Altering metabolism programs cell identity via NAD+-dependent deacetylation",

abstract = "Cells change their metabolic profiles in response to underlying gene regulatory networks, but how can alterations in metabolism encode specific transcriptional instructions? Here, we show that forcing a metabolic change in embryonic stem cells (ESCs) promotes a developmental identity that better approximates the inner cell mass (ICM) of the early mammalian blastocyst in cultures. This shift in cellular identity depends on the inhibition of glycolysis and stimulation of oxidative phosphorylation (OXPHOS) triggered by the replacement of d-glucose by d-galactose in ESC media. Enhanced OXPHOS in turn activates NAD + -dependent deacetylases of the Sirtuin family, resulting in the deacetylation of histones and key transcription factors to focus enhancer activity while reducing transcriptional noise, which results in a robustly enhanced ESC phenotype. This exploitation of a NAD + /NADH coenzyme coupled to OXPHOS as a means of programming lineage-specific transcription suggests new paradigms for how cells respond to alterations in their environment, and implies cellular rejuvenation exploits enzymatic activities for simultaneous activation of a discrete enhancer set alongside silencing genome-wide transcriptional noise.",

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author = "Bone, {Robert A.} and Lowndes, {Molly P.} and Silvia Raineri and {R Riveiro}, Alba and Lundregan, {Sarah L.} and Morten Dall and Karolina Sulek and Romero, {Jose A.H.} and Luna Malzard and Sandra Koigi and Heckenbach, {Indra J.} and Victor Solis-Mezarino and Moritz V{\"o}lker-Albert and Vasilopoulou, {Catherine G.} and Florian Meier and Ala Trusina and Matthias Mann and {L Nielsen}, Michael and Treebak, {Jonas T.} and Brickman, {Joshua M.}",

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doi = "10.1038/s44318-025-00417-0",

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T1 - Altering metabolism programs cell identity via NAD+-dependent deacetylation

AU - Bone, Robert A.

AU - Lowndes, Molly P.

AU - Raineri, Silvia

AU - R Riveiro, Alba

AU - Lundregan, Sarah L.

AU - Dall, Morten

AU - Sulek, Karolina

AU - Romero, Jose A.H.

AU - Malzard, Luna

AU - Koigi, Sandra

AU - Heckenbach, Indra J.

AU - Solis-Mezarino, Victor

AU - Völker-Albert, Moritz

AU - Vasilopoulou, Catherine G.

AU - Meier, Florian

AU - Trusina, Ala

AU - Mann, Matthias

AU - L Nielsen, Michael

AU - Treebak, Jonas T.

AU - Brickman, Joshua M.

PY - 2025

Y1 - 2025

N2 - Cells change their metabolic profiles in response to underlying gene regulatory networks, but how can alterations in metabolism encode specific transcriptional instructions? Here, we show that forcing a metabolic change in embryonic stem cells (ESCs) promotes a developmental identity that better approximates the inner cell mass (ICM) of the early mammalian blastocyst in cultures. This shift in cellular identity depends on the inhibition of glycolysis and stimulation of oxidative phosphorylation (OXPHOS) triggered by the replacement of d-glucose by d-galactose in ESC media. Enhanced OXPHOS in turn activates NAD + -dependent deacetylases of the Sirtuin family, resulting in the deacetylation of histones and key transcription factors to focus enhancer activity while reducing transcriptional noise, which results in a robustly enhanced ESC phenotype. This exploitation of a NAD + /NADH coenzyme coupled to OXPHOS as a means of programming lineage-specific transcription suggests new paradigms for how cells respond to alterations in their environment, and implies cellular rejuvenation exploits enzymatic activities for simultaneous activation of a discrete enhancer set alongside silencing genome-wide transcriptional noise.

AB - Cells change their metabolic profiles in response to underlying gene regulatory networks, but how can alterations in metabolism encode specific transcriptional instructions? Here, we show that forcing a metabolic change in embryonic stem cells (ESCs) promotes a developmental identity that better approximates the inner cell mass (ICM) of the early mammalian blastocyst in cultures. This shift in cellular identity depends on the inhibition of glycolysis and stimulation of oxidative phosphorylation (OXPHOS) triggered by the replacement of d-glucose by d-galactose in ESC media. Enhanced OXPHOS in turn activates NAD + -dependent deacetylases of the Sirtuin family, resulting in the deacetylation of histones and key transcription factors to focus enhancer activity while reducing transcriptional noise, which results in a robustly enhanced ESC phenotype. This exploitation of a NAD + /NADH coenzyme coupled to OXPHOS as a means of programming lineage-specific transcription suggests new paradigms for how cells respond to alterations in their environment, and implies cellular rejuvenation exploits enzymatic activities for simultaneous activation of a discrete enhancer set alongside silencing genome-wide transcriptional noise.

KW - Aging

KW - Enhancers

KW - Metabolism

KW - Pluripotency

KW - Sirtuins

U2 - 10.1038/s44318-025-00417-0

DO - 10.1038/s44318-025-00417-0

M3 - Journal article

C2 - 40281356

AN - SCOPUS:105003470286

SN - 0261-4189

VL - 44

SP - 3056

EP - 3084

JO - EMBO Journal

JF - EMBO Journal

IS - 11

ER -