An inverted Caveolin-1 topology defines a novel exosome secreted from prostate cancer cells

Author:

Ariotti Nicholas,Wu Yeping,Okano Satomi,Gambin Yann,Follett Jordan,Rae James,Ferguson Charles,Teasdale Rohan D.,Alexandrov Kirill,Meunier Frederic A.,Hill Michelle M.,Parton Robert G.

Abstract

ABSTRACTCaveolin-1 (Cav1) expression and secretion is associated with prostate cancer (PCa) disease progression but the mechanisms underpinning Cav1 release remain poorly understood. Numerous studies have shown Cav1 can be secreted within exosome-like vesicles, but antibody-mediated neutralization can mitigate PCa progression; this is suggestive of an inverted (non-exosomal) Cav1 topology. Here we show that Cav1 can be secreted from specific PCa types in an inverted vesicle-associated form consistent with the features of bioactive Cav1 secretion. Characterization of the isolated vesicles by electron microscopy, single molecule fluorescent microscopy and proteomics reveals they represent a novel class of exosomes ∼40 nm in diameter containing ∼50-60 copies of Cav1 and strikingly, are released via a non-canonical secretory autophagy pathway. This study provides novel insights into a mechanism whereby Cav1 translocates from a normal plasma membrane distribution to an inverted secreted form implicated in PCa disease progression.

Publisher

Cold Spring Harbor Laboratory

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