| Literature DB >> 24049740 |
Elodie Luche1, Béatrice Cousin, Lucile Garidou, Matteo Serino, Aurélie Waget, Corinne Barreau, Mireille André, Philippe Valet, Michael Courtney, Louis Casteilla, Rémy Burcelin.
Abstract
Metabolic endotoxemia triggers inflammation, targets cells from the stroma-vascular fraction of adipose depots, and metabolic disease. To identify these cells we here infused mice with lipopolysaccharides and showed by FACS analyses and BrdU staining that the number of small subcutaneous adipocytes, preadipocytes and macrophages increased in wild type but not in CD14-knockout (KO) mice. This mechanism was direct since in CD14KO mice grafted subcutaneously and simultaneously with fat pads from CD14KO and wild-type mice the concentration of cytokine mRNA was increased in the wild-type fat pad only. Conversely, the mRNA concentration of genes involved in glucose and lipid metabolism and the number of large adipocytes was reduced. Eventually, a pretreatment with LPS enhanced HFD-induced metabolic diseases. Altogether, these results show that metabolic endotoxemia increases the proliferation of preadipocytes through a CD14-dependent mechanism directly, without recruiting CD14-positive cells from non-adipose depot origin. This mechanism could precede the onset of metabolic diseases.Entities:
Keywords: Adipose tissue; Gut microbiota; Inflammation; LPS; Metabolic endotoxemia
Year: 2013 PMID: 24049740 PMCID: PMC3773833 DOI: 10.1016/j.molmet.2013.06.005
Source DB: PubMed Journal: Mol Metab ISSN: 2212-8778 Impact factor: 7.422