| Literature DB >> 28223285 |
Maria Pina Mollica1, Giuseppina Mattace Raso2, Gina Cavaliere1, Giovanna Trinchese1, Chiara De Filippo1, Serena Aceto1, Marina Prisco1, Claudio Pirozzi2, Francesca Di Guida2, Adriano Lama2, Marianna Crispino1, Diana Tronino2, Paola Di Vaio2, Roberto Berni Canani3,4,5, Antonio Calignano2, Rosaria Meli6.
Abstract
Fatty liver, oxidative stress, and mitochondrial dysfunction are key pathophysiological features of insulin resistance and obesity. Butyrate, produced by fermentation in the large intestine by gut microbiota, and its synthetic derivative, the N-(1-carbamoyl-2-phenyl-ethyl) butyramide, FBA, have been demonstrated to be protective against insulin resistance and fatty liver. Here, hepatic mitochondria were identified as the main target of the beneficial effect of both butyrate-based compounds in reverting insulin resistance and fat accumulation in diet-induced obese mice. In particular, butyrate and FBA improved respiratory capacity and fatty acid oxidation, activated the AMPK-acetyl-CoA carboxylase pathway, and promoted inefficient metabolism, as shown by the increase in proton leak. Both treatments consistently increased utilization of substrates, especially fatty acids, leading to the reduction of intracellular lipid accumulation and oxidative stress. Finally, the shift of the mitochondrial dynamic toward fusion by butyrate and FBA resulted in the improvement not only of mitochondrial cell energy metabolism but also of glucose homeostasis. In conclusion, butyrate and its more palatable synthetic derivative, FBA, modulating mitochondrial function, efficiency, and dynamics, can be considered a new therapeutic strategy to counteract obesity and insulin resistance.Entities:
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Year: 2017 PMID: 28223285 DOI: 10.2337/db16-0924
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461