| Literature DB >> 29320704 |
Martin Whitham1, Benjamin L Parker2, Martin Friedrichsen3, Janne R Hingst3, Marit Hjorth4, William E Hughes4, Casey L Egan5, Lena Cron5, Kevin I Watt6, Rhiannon P Kuchel7, Navind Jayasooriah8, Emma Estevez5, Tim Petzold5, Catherine M Suter9, Paul Gregorevic10, Bente Kiens3, Erik A Richter3, David E James2, Jørgen F P Wojtaszewski3, Mark A Febbraio11.
Abstract
Exercise stimulates the release of molecules into the circulation, supporting the concept that inter-tissue signaling proteins are important mediators of adaptations to exercise. Recognizing that many circulating proteins are packaged in extracellular vesicles (EVs), we employed quantitative proteomic techniques to characterize the exercise-induced secretion of EV-contained proteins. Following a 1-hr bout of cycling exercise in healthy humans, we observed an increase in the circulation of over 300 proteins, with a notable enrichment of several classes of proteins that compose exosomes and small vesicles. Pulse-chase and intravital imaging experiments suggested EVs liberated by exercise have a propensity to localize in the liver and can transfer their protein cargo. Moreover, by employing arteriovenous balance studies across the contracting human limb, we identified several novel candidate myokines, released into circulation independently of classical secretion. These data identify a new paradigm by which tissue crosstalk during exercise can exert systemic biological effects.Entities:
Keywords: arteriovenous; exercise; exosome; extracellular vesicle; integrin; muscle; myokine; proteomics
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Year: 2018 PMID: 29320704 DOI: 10.1016/j.cmet.2017.12.001
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287