Adiponectin is a cytokine produced predominantly by adipose tissue and correlates with glucose and lipid homeostasis. However, the effects of adiponectin on endoplasmic reticulum (ER) stress and apoptosis of adipose tissue remain elusive. In this study, we found that tunicamycin-induced ER stress increased serum free fatty acid (FFA) and impaired glucose tolerance, elevated the mRNA levels of GRP78, Chop, ATF2 and caspase 3, but reduced adiponectin mRNA level in white adipose tissue. Moreover, ER stress-triggered adipocyte apoptosis by increasing cellular FFA level and Ca2+ level. Further analysis revealed that adiponectin alleviated ER stress-induced adipocyte apoptosis by elevating peroxisome proliferator-activated receptor alpha (PPARα) mRNA level. Our data also confirmed that adiponectin reduced early apoptotic cells and blocked the mitochondrial apoptosis pathway by activating the AdipoR1/AMP-activated protein kinase (AMPK) signal pathway. In addition, PPARα bound to ATF2 promoter region and inhibited transcription of ATF2. The inhibition of adipocyte apoptosis by adiponectin was correlated with transcriptional suppression of ATF2. Furthermore, adiponectin inhibited ER stress-induced apoptosis by activating the AMPK/PKC pathway. In summary, our data demonstrate adiponectin inhibited ER stress and apoptosis of adipocyte in vivo and in vitro by activating the AMPK/PPARα/ATF2 pathway. Our study establishes that adiponectin is an important adipocytokine for preventing and treating obesity.
Our results indicated that Foxc2 inhibited inflammation and promoted browning of WAT through positive regulation of leptin signal and the STAT3-PRDM16 complex. These findings identify a new potential means to prevent and treat obese caused metabolic syndrome of mammals.
shown that Sirt1 is involved in regulation of inflammation response and inhibits inflammatory pathways in macrophages and dendritic cells (6, 7). In 3T3-L1 adipocytes, Sirt1 can attenuate TNF--induced insulin resistance and inflammation (3,8). Resveratrol (RES) is a natural polyphenolic compound known for its beneficial effects on energy homeostasis (9, 10). Studies have shown that RES attenuates inflammation of adipocytes and vascular endothelial cells by activating Sirt1 and inducing autophagy (11-13). However, the regulatory mechanism of RES on Sirt1 and adipose inflammation remains unclear.The Akt/mammalian target of rapamycin (mTOR) pathway plays an important role in the regulation of cellular gluconeogenesis and metabolism (14,15). mTOR is highly conserved serine/threonine kinase that is expressed in cancer cells, adipocytes, and hepatocytes, and can be directly phosphorylated by activated . During development of obesity, adipose pro-inflammatory responses are closely associated with the development of insulin resistance in adipose tissue (19,20). A recent study showed that phosphorylation of Akt in macrophages could activate mTOR signal and then led to inflammation and insulin resistance in high-fat diet (HFD)-induced obesity (21). Moreover, Pang et al. (22) reported that Sirt1 directly bound protein kinase B (Akt2) and then inhibited adipogenesis in porcine adipocytes. Busch et al. (23) also suggested that Akt was one of the main upstream stimulatory kinases that modulated by Sirt1. However, whether the interaction between Sirt1 and Akt2 can regulate adipose inflammation has not been studied.We suggested that RES would attenuate HFD-induced obesity and adipose inflammation by activating Sirt1. We found that RES promoted the interaction of Sirt1 and Akt2, and then inhibited adipose inflammation by activating the mTOR/S6K1 pathway. These findings identify a novel function of Sirt1 in the regulation of adipose inflammation Sirtuin type 1 (Sirt1) is a member of the silencing information regulator 2 (Sir2) family called sirtuins, and is wellknown for its deacetylation in regulation of gene silencing, energy homeostasis, and apoptosis (1-3). The overloaded calorie intake leads to dysfunction of adipocytes and causes obesity (4). Obesity is closely associated with chronic inflammation and characterized by abnormal cytokine production, increased acute-phase reactants, and an activated network of inflammatory signal pathways (5 Abbreviations: Akt2, protein kinase B; HFD, high-fat diet; IL-6, interleukin-6; iNOS, inducible nitric oxide synthase; mTOR, mammalian target of rapamycin; NAM, nicotinamide; RES, resveratrol; Sirt1, sirtuin type 1.
Alpha-melanocyte stimulating hormone (αMSH) is an important adenohypophysis polypeptide hormone that regulates body metabolic status. To date, it is well known that the disorder of hypothalamic αMSH secretion is related to many metabolic diseases, such as obesity and type II diabetes. However, the underlying mechanisms are poorly understood. In our study, we focused on the reactive oxygen species (ROS)-induced adipocyte apoptosis and tried to unveil the role of αMSH in this process and the signal pathway which αMSH acts through. Kunming white mice were used and induced to oxidative stress status by hydrogen peroxide (H2O2) injection and a significant reduction of αMSH were found in mice serum, while elevated ROS level and mRNA level of pro-apoptotic genes were observed in mice adipose tissue. What is more, when detect the function of αMSH in ROS-induced apoptosis, similar inhibitory trend was found with the oxidative stress inhibitor N-acetyl-L-cysteine (NAC) in ROS-induced adipocyte apoptosis and this trend is αMSH receptor melanocortin 5 receptor (MC5R) depended, while an opposite trend was found between αMSH and Foxo1, which is a known positive regulator of adipocyte apoptosis. Further, we found that the repress effect of αMSH in adipocytes apoptosis is acting through Foxo1/mTORC2 pathway. These findings indicate that, αMSH has a strong inhibitory effect on ROS-induced adipocyte apoptosis and underlying mechanism is interacting with key factors in mTOR signal pathway. Our study demonstrated a great role of αMSH in adipocyte apoptosis and brings a new therapeutic mean to the treatment of obesity and diabetes.
Alpha-melanocyte stimulating hormone (αMSH) has an important role in the regulation of body weight and energy expenditure. Nevertheless, the molecular mechanisms of circulating αMSH on preadipocyte proliferation remain elusive. We found αMSH was reduced by high fat diet (HFD) while leptin was elevated in adipose tissue. Leptin resistance and endoplasmic reticulum (ER) stress of adipose tissue were increased in obese mice. αMSH increased leptin sensitivity and alleviated ER stress along with increased p-STAT3 level and reduced SOCS3, GRP78, CHOP, ATF4, p27 and p53 levels. αMSH and leptin co-treatment alleviated ER stress through decreasing the levels of GRP78 and CHOP. Tunicamycin (TM) or thapsigargin (Tg) induced ER stress blunted leptin sensitivity and inhibited preadipocyte proliferation. αMSH and leptin co-treatment increased the cell number, augmented G1-S transition, elevated leptin sensitivity, and reduced ER stress; it also activated Notch1 signal and stimulated preadipocyte proliferation, whereas ER stress marker genes were decreased during this process. However, the effects of αMSH and leptin were blocked by the specific inhibitor of Notch1 signal. In summary, our data revealed αMSH enhanced leptin sensitivity and preadipocyte proliferation, meanwhile inhibited ER stress of preadipocytes by activating Notch1 signal.
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