| Literature DB >> 33972798 |
Kai-Chun Li1, Enrico Girardi1, Felix Kartnig1, Sarah Grosche1, Tea Pemovska1, Johannes W Bigenzahn1,2, Ulrich Goldmann1, Vitaly Sedlyarov1, Ariel Bensimon1, Sandra Schick1, Jung-Ming G Lin1, Bettina Gürtl1, Daniela Reil1, Kristaps Klavins1, Stefan Kubicek1,3, Sara Sdelci1,4, Giulio Superti-Furga5,6.
Abstract
Metabolism negotiates cell-endogenous requirements of energy, nutrients and building blocks with the immediate environment to enable various processes, including growth and differentiation. While there is an increasing number of examples of crosstalk between metabolism and chromatin, few involve uptake of exogenous metabolites. Solute carriers (SLCs) represent the largest group of transporters in the human genome and are responsible for the transport of a wide variety of substrates, including nutrients and metabolites. We aimed to investigate the possible involvement of SLC-mediated solutes uptake and cellular metabolism in regulating cellular epigenetic states. Here, we perform a CRISPR-Cas9 transporter-focused genetic screen and a metabolic compound library screen for the regulation of BRD4-dependent chromatin states in human myeloid leukaemia cells. Intersection of the two orthogonal approaches reveal that loss of transporters involved with purine transport or inhibition of de novo purine synthesis lead to dysfunction of BRD4-dependent transcriptional regulation. Through mechanistic characterization of the metabolic circuitry, we elucidate the convergence of SLC-mediated purine uptake and de novo purine synthesis on BRD4-chromatin occupancy. Moreover, adenine-related metabolite supplementation effectively restores BRD4 functionality on purine impairment. Our study highlights the specific role of purine/adenine metabolism in modulating BRD4-dependent epigenetic states.Entities:
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Year: 2021 PMID: 33972798 PMCID: PMC7612075 DOI: 10.1038/s42255-021-00386-8
Source DB: PubMed Journal: Nat Metab ISSN: 2522-5812