AI Article Synopsis

  • Type 2 diabetes and obesity are global issues, and dietary polyphenols like anthocyanins from berries can help alleviate symptoms of these diseases.
  • Research focused on two specific anthocyanins (DG and DS) to see if they could counteract the negative metabolic effects of the antipsychotic medication olanzapine, which can lead to metabolic syndrome.
  • Results indicated that while DG and DS effectively reduced fat accumulation in liver cells, they did not restore normal insulin signaling in muscle cells affected by olanzapine.

Article Abstract

Type 2 diabetes and obesity are major problems worldwide and dietary polyphenols have shown efficacy to ameliorate signs of these diseases. Anthocyanins from berries display potent antioxidants and protect against weight gain and insulin resistance in different models of diet-induced metabolic syndrome. Olanzapine is known to induce an accelerated form of metabolic syndrome. Due to the aforementioned, we evaluated whether delphinidin-3,5--diglucoside (DG) and delphinidin-3--sambubioside-5--glucoside (DS), two potent antidiabetic anthocyanins isolated from fruit, could prevent olanzapine-induced steatosis and insulin resistance in liver and skeletal muscle cells, respectively. HepG2 liver cells and L6 skeletal muscle cells were co-incubated with DG 50 μg/mL or DS 50 μg/mL plus olanzapine 50 μg/mL. Lipid accumulation was determined in HepG2 cells while the expression of p-Akt as a key regulator of the insulin-activated signaling pathways, mitochondrial function, and glucose uptake was assessed in L6 cells. DS and DG prevented olanzapine-induced lipid accumulation in liver cells. However, insulin signaling impairment induced by olanzapine in L6 cells was not rescued by DS and DG. Thus, anthocyanins modulate lipid metabolism, which is a relevant factor in hepatic tissue, but do not significantly influence skeletal muscle, where a potent antioxidant effect of olanzapine was found.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8537850PMC
http://dx.doi.org/10.3390/molecules26206149DOI Listing

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