Resveratrol promotes white adipocytes browning and improves metabolic disorders in Sirt1‐dependent manner in mice

Li, Zilun; Zhang, Zili; Ke, Liangru; Sun, Yu; Li, Wenxue; Feng, Xiaodong; Zhu, Wei; Chen, Sifan

doi:10.1096/fj.201902222r

Cited by 32 publications

(28 citation statements)

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“…[48] It has been reported that CR and SIRT1 activation promote the recruitment of brown adipocytes within WAT, an effect that has been associated with improved glucose homeostasis. [49,50] Consistent with these reports, we found a remarkable induction of brown adipocyte-specific genes (i.e., Ucp1, Adrb3, or Cidea) in subcutaneous WAT of CR mice, whereas the effects of SIRT1 overexpression on the expression of these genes was very marginal or inexistent. Importantly, regardless of the effects on the mRNA levels of brown adipocyte-specific genes, we did not find any detectable UCP1 protein in WAT of CR and Sirt1-Tg mice, suggesting that browning of WAT was negligible.…”

Section: Discussionsupporting

confidence: 89%

Calorie Restriction and SIRT1 Overexpression Induce Different Gene Expression Profiles in White Adipose Tissue in Association with Metabolic Improvement

Pardo

Velilla

Herrero

et al. 2021

Molecular Nutrition Food Res

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Introduction Calorie restriction (CR) exerts multiple effects on health, including the amelioration of systemic insulin resistance. Although the precise mechanisms by which CR improves glucose homeostasis remain poorly defined, SIRT1 has been suggested to act as a central mediator of the cellular responses to CR. Here, we aim at identifying the mechanisms by which CR and SIRT1 modulate white adipose tissue (WAT) function, a key tissue in the control of glucose homeostasis. Material and Methods A gene expression profiling study using DNA microarrays is conducted in WAT of control and SIRT1 transgenic mice fed ad libitum (AL) and mice subjected to 40% CR. Results Gene expression profiling reveals a relatively low degree of overlap between the transcriptional programs regulated by SIRT1 and CR. Gene networks related to extracellular matrix appear commonly downregulated by SIRT1/CR, whereas mitochondrial biogenesis is enhanced exclusively by CR. Moreover, WAT inflammation is reduced by CR and SIRT1, although their anti‐inflammatory effects appeared to be achieved by regulating different gene networks related to the immune system. Concluding Remarks In WAT, SIRT1 does not mediate most of the effects of CR on gene expression. Still, gene networks differentially regulated by SIRT1 and CR converge to reduce WAT inflammation.

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Section: Discussionsupporting

confidence: 89%

Calorie Restriction and SIRT1 Overexpression Induce Different Gene Expression Profiles in White Adipose Tissue in Association with Metabolic Improvement

Pardo

Velilla

Herrero

et al. 2021

Molecular Nutrition Food Res

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“…Transmission electron microscopy showed that 3T3-L1 cells treated with BBR exhibited the characteristics of brown-like adipocytes with increased mitochondrial density and smaller lipid droplets (Figure 4 B). Previous studies have demonstrated that SIRT1 played an important role in energy metabolism and remodeling of adipose tissue 21 , 44 , 45 . We next elucidated whether SIRT1 is necessary for BBR to regulate the remodeling of adipose tissue.…”

Section: Resultsmentioning

confidence: 99%

Berberine modulates deacetylation of PPARγ to promote adipose tissue remodeling and thermogenesis via AMPK/SIRT1 pathway

et al. 2021

Int. J. Biol. Sci.

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Pharmacological stimulation of adipose tissue remodeling and thermogenesis to increase energy expenditure is expected to be a viable therapeutic strategy for obesity. Berberine has been reported to have pharmacological activity in adipose tissue to anti-obesity, while the mechanism remains unclear. Here, we observed that berberine significantly reduced the body weight and insulin resistance of high-fat diet mice by promoting the distribution of brown adipose tissue and thermogenesis. We have further demonstrated that berberine activated energy metabolic sensing pathway AMPK/SIRT1 axis to increase the level of PPARγ deacetylation, which leads to promoting adipose tissue remodeling and increasing the expression of the thermogenic protein UCP-1. These findings suggest that berberine that enhances the AMPK/SIRT1 pathway can act as a selective PPARγ activator to promote adipose tissue remodeling and thermogenesis. This study proposes a new mechanism for the regulation of berberine in adipose tissue and offers a great prospect for berberine in obesity treatment

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“…Bars represent the mean ± SD. *P < 0.05 of cellular biochemical processes (Li et al, 2020;Liu et al, 2020;Wu et al, 2018;Zhang, Bi, et al, 2019). Mounting evidence indicated that SIRT1 could enhance the expression and transcriptional activity of Nrf2 to exert potent anti-oxidant effects (Huang et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

“…SIRT1 might be involved in the mechanisms by which astaxanthin modulates Nrf2/Prx2/ASK1/p38 signalling after traumatic brain injury. SIRT1 is a type of histone deacetylase that regulates a variety of cellular biochemical processes (Li et al, 2020; Liu et al, 2020; Wu et al, 2018; Zhang, Bi, et al, 2019). Mounting evidence indicated that SIRT1 could enhance the expression and transcriptional activity of Nrf2 to exert potent anti‐oxidant effects (Huang et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

Astaxanthin ameliorates oxidative stress and neuronal apoptosis via SIRT1/NRF2/Prx2/ASK1/p38 after traumatic brain injury in mice

Zhang

et al. 2021

British J Pharmacology

114

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Background and Purpose Oxidative stress and neuronal apoptosis play key roles in traumatic brain injury. We investigated the protective effects of astaxanthin against traumatic brain injury and its underlying mechanisms of action. Experimental Approach A weight‐drop model of traumatic brain injury in vivo and hydrogen peroxide exposure in vitro model were established. Brain oedema, behaviour tests, western blot, biochemical analysis, lesion volume, histopathological study and cell viability were performed. Key Results Astaxanthin significantly reduced oxidative insults on Days 1, 3 and 7 after traumatic brain injury. Neuronal apoptosis was also ameliorated on Day 3. Additionally, astaxanthin improved neurological functions up to 3 weeks after traumatic brain injury. Astaxanthin treatment dramatically enhanced the expression of peroxiredoxin 2 (Prx2), nuclear factor‐erythroid 2‐related factor 2 (NRF2/Nrf2) and sirtuin 1 (SIRT1), while it down‐regulated the phosphorylation of apoptosis signal‐regulating kinase 1 (ASK1) and p38. Inhibition of Prx2 by siRNA injection reversed the beneficial effects of astaxanthin against traumatic brain injury. Additionally, Nrf2 knockout prevented the neuroprotective effects of astaxanthin in traumatic brain injury. In contrast, overexpression of Prx2 in Nrf2 knockout mice attenuated the secondary brain injury after traumatic brain injury. Moreover, inhibiting SIRT1 by EX527 dramatically inhibited the neuroprotective effects of astaxanthin and suppressed SIRT1/Nrf2/Prx2/ASK1/p38 pathway both in vivo and in vitro. Conclusion and Implications Astaxanthin improved the neurological functions and protected the brain from injury after traumatic brain injury, primarily by reducing oxidative stress and neuronal death via SIRT1/Nrf2/Prx2/ASK1/p38 signalling pathway and might be a new candidate to ameliorate traumatic brain injury.

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Resveratrol promotes white adipocytes browning and improves metabolic disorders in Sirt1‐dependent manner in mice

Cited by 32 publications

References 50 publications

Calorie Restriction and SIRT1 Overexpression Induce Different Gene Expression Profiles in White Adipose Tissue in Association with Metabolic Improvement

Calorie Restriction and SIRT1 Overexpression Induce Different Gene Expression Profiles in White Adipose Tissue in Association with Metabolic Improvement

Berberine modulates deacetylation of PPARγ to promote adipose tissue remodeling and thermogenesis via AMPK/SIRT1 pathway

Astaxanthin ameliorates oxidative stress and neuronal apoptosis via SIRT1/NRF2/Prx2/ASK1/p38 after traumatic brain injury in mice

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