Increased secretion of adipocyte-derived extracellular vesicles is associated with adipose tissue inflammation and the mobilization of excess lipid in human obesity
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Published:2024-07-04
Issue:1
Volume:22
Page:
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ISSN:1479-5876
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Container-title:Journal of Translational Medicine
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language:en
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Short-container-title:J Transl Med
Author:
Matilainen JohannaORCID, Berg Viivi, Vaittinen Maija, Impola Ulla, Mustonen Anne-Mari, Männistö Ville, Malinen Marjo, Luukkonen Veera, Rosso NataliaORCID, Turunen Tanja, Käkelä Pirjo, Palmisano Silvia, Arasu Uma Thanigai, Sihvo Sanna P., Aaltonen Niina, Härkönen Kai, Caddeo Andrea, Kaminska DorotaORCID, Pajukanta Päivi, Kaikkonen Minna U., Tiribelli ClaudioORCID, Käkelä Reijo, Laitinen Saara, Pihlajamäki JussiORCID, Nieminen Petteri, Rilla Kirsi
Abstract
Abstract
Background
Obesity is a worldwide epidemic characterized by adipose tissue (AT) inflammation. AT is also a source of extracellular vesicles (EVs) that have recently been implicated in disorders related to metabolic syndrome. However, our understanding of mechanistic aspect of obesity’s impact on EV secretion from human AT remains limited.
Methods
We investigated EVs from human Simpson Golabi Behmel Syndrome (SGBS) adipocytes, and from AT as well as plasma of subjects undergoing bariatric surgery. SGBS cells were treated with TNFα, palmitic acid, and eicosapentaenoic acid. Various analyses, including nanoparticle tracking analysis, electron microscopy, high-resolution confocal microscopy, and gas chromatography–mass spectrometry, were utilized to study EVs. Plasma EVs were analyzed with imaging flow cytometry.
Results
EVs from mature SGBS cells differed significantly in size and quantity compared to preadipocytes, disagreeing with previous findings in mouse adipocytes and indicating that adipogenesis promotes EV secretion in human adipocytes. Inflammatory stimuli also induced EV secretion, and altered EV fatty acid (FA) profiles more than those of cells, suggesting the role of EVs as rapid responders to metabolic shifts. Visceral AT (VAT) exhibited higher EV secretion compared to subcutaneous AT (SAT), with VAT EV counts positively correlating with plasma triacylglycerol (TAG) levels. Notably, the plasma EVs of subjects with obesity contained a higher number of adiponectin-positive EVs than those of lean subjects, further demonstrating higher AT EV secretion in obesity. Moreover, plasma EV counts of people with obesity positively correlated with body mass index and TNF expression in SAT, connecting increased EV secretion with AT expansion and inflammation. Finally, EVs from SGBS adipocytes and AT contained TAGs, and EV secretion increased despite signs of less active lipolytic pathways, indicating that AT EVs could be involved in the mobilization of excess lipids into circulation.
Conclusions
We are the first to provide detailed FA profiles of human AT EVs. We report that AT EV secretion increases in human obesity, implicating their role in TAG transport and association with adverse metabolic parameters, thereby emphasizing their role in metabolic disorders. These findings promote our understanding of the roles that EVs play in human AT biology and metabolic disorders.
Funder
Academy of Finland Saastamoisen säätiö Helena Vuorenmiehen säätiö Magnus Ehrnroothin Säätiö Instrumentariumin Tiedesäätiö Itä-Suomen Yliopisto Suomen Kulttuurirahasto
Publisher
Springer Science and Business Media LLC
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