4.7 Article

Ketogenic Diet Increases Serum and White Adipose Tissue SIRT1 Expression in Mice

期刊

出版社

MDPI
DOI: 10.3390/ijms232415860

关键词

SIRT1; ketogenic diet; ketone bodies; obesity; epigenetic regulators; adipose tissue

资金

  1. Sapienza Progetti di Ateneo [RP11916B8955250D]
  2. PRIN [2017RS5M44_002]
  3. Italian Ministry of Education, Universities and Research

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The effect of a ketogenic diet on SIRT1 levels in different tissues was examined in mice. The results showed increased SIRT1 expression in adipose tissue and serum, but not in brown adipose tissue and the liver. The findings suggest that the potential metabolic health benefits of a ketogenic diet may involve a synergistic interaction with SIRT1.
Overnutrition and its sequelae have become a global concern due to the increasing incidence of obesity and insulin resistance. A ketogenic diet (KD) is widely used as a dietary treatment for metabolic disorders. Sirtuin1 (SIRT1), a metabolic sensor which regulates fat homeostasis, is modulated by dietary interventions. However, the influence of nutritional ketosis on SIRT1 is still debated. We examined the effect of KD on adipose tissue, liver, and serum levels of SIRT1 in mice. Adult C57BL/6J male mice were randomly assigned to two isocaloric dietary groups and fed with either high-fat KD or normal chow (NC) for 4 weeks. Serum SIRT1, beta-hydroxybutyrate (beta HB), glucose, and triglyceride levels, as well as SIRT1 expression in visceral (VAT), subcutaneous (SAT), and brown (BAT) adipose tissues, and in the liver, were measured. KD-fed mice showed an increase in serum beta HB in parallel with serum SIRT1 (r = 0.732, p = 0.0156), and increased SIRT1 protein expression in SAT and VAT. SIRT1 levels remained unchanged in BAT and in the liver, which developed steatosis. Normal glycemia and triglycerides were observed. Under a KD, serum and white fat phenotypes show higher SIRT1, suggesting that one of the molecular mechanisms underlying a KD's potential benefits on metabolic health involves a synergistic interaction with SIRT1.

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