Deletion of intestinal Hdac3 remodels the lipidome of enterocytes and protects mice from diet-induced obesity
Version 2 2024-06-06, 00:10Version 2 2024-06-06, 00:10
Version 1 2020-05-27, 15:57Version 1 2020-05-27, 15:57
journal contribution
posted on 2024-06-06, 00:10 authored by M Dávalos-Salas, MK Montgomery, CM Reehorst, R Nightingale, I Ng, H Anderton, S Al-Obaidi, A Lesmana, CM Scott, P Ioannidis, H Kalra, S Keerthikumar, L Tögel, A Rigopoulos, SJ Gong, DS Williams, P Yoganantharaja, K Bell-Anderson, S Mathivanan, Y Gibert, S Hiebert, AM Scott, MJ Watt, JM Mariadason© 2019, The Author(s). Histone deacetylase 3 (Hdac3) regulates the expression of lipid metabolism genes in multiple tissues, however its role in regulating lipid metabolism in the intestinal epithelium is unknown. Here we demonstrate that intestine-specific deletion of Hdac3 (Hdac3IKO) protects mice from diet induced obesity. Intestinal epithelial cells (IECs) from Hdac3IKO mice display co-ordinate induction of genes and proteins involved in mitochondrial and peroxisomal β-oxidation, have an increased rate of fatty acid oxidation, and undergo marked remodelling of their lipidome, particularly a reduction in long chain triglycerides. Many HDAC3-regulated fatty oxidation genes are transcriptional targets of the PPAR family of nuclear receptors, Hdac3 deletion enhances their induction by PPAR-agonists, and pharmacological HDAC3 inhibition induces their expression in enterocytes. These findings establish a central role for HDAC3 in co-ordinating PPAR-regulated lipid oxidation in the intestinal epithelium, and identify intestinal HDAC3 as a potential therapeutic target for preventing obesity and related diseases.
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Nature CommunicationsVolume
10Article number
5291Pagination
1-14Location
Berlin, GermanyPublisher DOI
Open access
- Yes
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2041-1723Language
engPublication classification
C1 Refereed article in a scholarly journalPublisher
Springer NatureUsage metrics
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