| Literature DB >> 31851905 |
Mario A Lauterbach1, Jasmin E Hanke2, Magdalini Serefidou3, Matthew S J Mangan4, Carl-Christian Kolbe1, Timo Hess5, Maximilian Rothe1, Romina Kaiser4, Florian Hoss1, Jan Gehlen5, Gudrun Engels1, Maike Kreutzenbeck1, Susanne V Schmidt1, Anette Christ6, Axel Imhof7, Karsten Hiller8, Eicke Latz9.
Abstract
Toll-like receptor (TLR) activation induces inflammatory responses in macrophages by activating temporally defined transcriptional cascades. Whether concurrent changes in the cellular metabolism that occur upon TLR activation influence the quality of the transcriptional responses remains unknown. Here, we investigated how macrophages adopt their metabolism early after activation to regulate TLR-inducible gene induction. Shortly after TLR4 activation, macrophages increased glycolysis and tricarboxylic acid (TCA) cycle volume. Metabolic tracing studies revealed that TLR signaling redirected metabolic fluxes to generate acetyl-Coenzyme A (CoA) from glucose resulting in augmented histone acetylation. Signaling through the adaptor proteins MyD88 and TRIF resulted in activation of ATP-citrate lyase, which in turn facilitated the induction of distinct LPS-inducible gene sets. We postulate that metabolic licensing of histone acetylation provides another layer of control that serves to fine-tune transcriptional responses downstream of TLR activation. Our work highlights the potential of targeting the metabolic-epigenetic axis in inflammatory settings.Entities:
Keywords: ATP-citrate lyase; TLR signaling; histone acetylation; inflammation; macrophage metabolism
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Year: 2019 PMID: 31851905 DOI: 10.1016/j.immuni.2019.11.009
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 31.745