| Literature DB >> 32720716 |
Shih-Jung Fan1, Benjamin Kroeger1, Pauline P Marie1, Esther M Bridges2, John D Mason1, Kristie McCormick1, Christos E Zois2, Helen Sheldon2, Nasullah Khalid Alham3,4, Errin Johnson5, Matthew Ellis1, Maria Irina Stefana1, Cláudia C Mendes1, Stephen Mark Wainwright1, Christopher Cunningham6, Freddie C Hamdy6, John F Morris1, Adrian L Harris2, Clive Wilson1, Deborah Ci Goberdhan1.
Abstract
Exosomes are secreted extracellular vesicles carrying diverse molecular cargos, which can modulate recipient cell behaviour. They are thought to derive from intraluminal vesicles formed in late endosomal multivesicular bodies (MVBs). An alternate exosome formation mechanism, which is conserved from fly to human, is described here, with exosomes carrying unique cargos, including the GTPase Rab11, generated in Rab11-positive recycling endosomal MVBs. Release of Rab11-positive exosomes from cancer cells is increased relative to late endosomal exosomes by reducing growth regulatory Akt/mechanistic Target of Rapamycin Complex 1 (mTORC1) signalling or depleting the key metabolic substrate glutamine, which diverts membrane flux through recycling endosomes. Vesicles produced under these conditions promote tumour cell proliferation and turnover and modulate blood vessel networks in xenograft mouse models in vivo. Their growth-promoting activity, which is also observed in vitro, is Rab11a-dependent, involves ERK-MAPK-signalling and is inhibited by antibodies against amphiregulin, an EGFR ligand concentrated on these vesicles. Therefore, glutamine depletion or mTORC1 inhibition stimulates release from Rab11a compartments of exosomes with pro-tumorigenic functions, which we propose promote stress-induced tumour adaptation.Entities:
Keywords: Rab11(a); exosome; extracellular vesicle; mechanistic Target of Rapamycin; multivesicular body
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Year: 2020 PMID: 32720716 PMCID: PMC7429491 DOI: 10.15252/embj.2019103009
Source DB: PubMed Journal: EMBO J ISSN: 0261-4189 Impact factor: 14.012