Litcius/Paper detail

BMAL1 coordinates energy metabolism and differentiation of pluripotent stem cells

Cristina Ameneiro, Tiago Moreira, Alejandro Fuentes-Iglesias, Alba Coego, Vera Garcia‐Outeiral, Adriana Escudero, Daniel Torrecilla, Sonia Mulero‐Navarro, José María Carvajal-González, Diana Guallar, Miguel Fidalgo

2020Life Science Alliance21 citationsDOIOpen Access PDF

Abstract

BMAL1 is essential for the regulation of circadian rhythms in differentiated cells and adult stem cells, but the molecular underpinnings of its function in pluripotent cells, which hold a great potential in regenerative medicine, remain to be addressed. Here, using transient and permanent loss-of-function approaches in mouse embryonic stem cells (ESCs), we reveal that although BMAL1 is dispensable for the maintenance of the pluripotent state, its depletion leads to deregulation of transcriptional programs linked to cell differentiation commitment. We further confirm that depletion of Bmal1 alters the differentiation potential of ESCs in vitro. Mechanistically, we demonstrate that BMAL1 participates in the regulation of energy metabolism maintaining a low mitochondrial function which is associated with pluripotency. Loss-of-function of Bmal1 leads to the deregulation of metabolic gene expression associated with a shift from glycolytic to oxidative metabolism. Our results highlight the important role that BMAL1 plays at the exit of pluripotency in vitro and provide evidence implicating a non-canonical circadian function of BMAL1 in the metabolic control for cell fate determination.

Topics & Concepts

Induced pluripotent stem cellCell biologyBiologyEmbryonic stem cellCellular differentiationStem cellRegenerative medicineCell fate determinationGeneticsGeneTranscription factorGenetics, Aging, and Longevity in Model OrganismsEpigenetics and DNA MethylationMitochondrial Function and Pathology