| Literature DB >> 27388216 |
Bastien Vergoni1, Pierre-Jean Cornejo1, Jérôme Gilleron1, Mansour Djedaini1, Franck Ceppo1, Arnaud Jacquel2, Gwennaelle Bouget1, Clémence Ginet1, Teresa Gonzalez3, Julie Maillet4, Véronique Dhennin4, Marie Verbanck4, Patrick Auberger2, Philippe Froguel5, Jean-François Tanti1, Mireille Cormont6.
Abstract
Activation of the p53 pathway in adipose tissue contributes to insulin resistance associated with obesity. However, the mechanisms of p53 activation and the effect on adipocyte functions are still elusive. Here we found a higher level of DNA oxidation and a reduction in telomere length in adipose tissue of mice fed a high-fat diet and an increase in DNA damage and activation of the p53 pathway in adipocytes. Interestingly, hallmarks of chronic DNA damage are visible at the onset of obesity. Furthermore, injection of lean mice with doxorubicin, a DNA damage-inducing drug, increased the expression of chemokines in adipose tissue and promoted its infiltration by proinflammatory macrophages and neutrophils together with adipocyte insulin resistance. In vitro, DNA damage in adipocytes increased the expression of chemokines and triggered the production of chemotactic factors for macrophages and neutrophils. Insulin signaling and effect on glucose uptake and Glut4 translocation were decreased, and lipolysis was increased. These events were prevented by p53 inhibition, whereas its activation by nutlin-3 reproduced the DNA damage-induced adverse effects. This study reveals that DNA damage in obese adipocytes could trigger p53-dependent signals involved in alteration of adipocyte metabolism and secretory function leading to adipose tissue inflammation, adipocyte dysfunction, and insulin resistance.Entities:
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Year: 2016 PMID: 27388216 DOI: 10.2337/db16-0014
Source DB: PubMed Journal: Diabetes ISSN: 0012-1797 Impact factor: 9.461