Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.

Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.

Exosomes are of increasing interest as alternative mode of cell-to-cell communication. We previously reported that exosomes secreted by human SOJ-6 pancreatic tumor cells induce (glyco)protein ligand-independent cell death and inhibit Notch-1 pathway, this latter being particularly active during car...

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Main Authors: Sadia Beloribi, Elodie Ristorcelli, Gilles Breuzard, Françoise Silvy, Justine Bertrand-Michel, Evelyne Beraud, Alain Verine, Dominique Lombardo
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3477155?pdf=render
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spelling doaj-f637aa85c8e74d0c8b2112061861d25a2020-11-25T01:15:00ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-01710e4748010.1371/journal.pone.0047480Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.Sadia BeloribiElodie RistorcelliGilles BreuzardFrançoise SilvyJustine Bertrand-MichelEvelyne BeraudAlain VerineDominique LombardoExosomes are of increasing interest as alternative mode of cell-to-cell communication. We previously reported that exosomes secreted by human SOJ-6 pancreatic tumor cells induce (glyco)protein ligand-independent cell death and inhibit Notch-1 pathway, this latter being particularly active during carcinogenesis and in cancer stem cells. Therefore, we asked whether exosomal lipids were key-elements for cell death and hypothesized that cholesterol-rich membrane microdomains were privileged sites of exosome interactions with tumor cells. To address these questions and based on the lipid composition of exosomes from SOJ-6 cells (Ristorcelli et al. (2008) FASEB J. 22; 3358-3369) enriched in cholesterol and sphingomyelin (lipids forming liquid-ordered phase, Lo) and depleted in phospholipids (lipids forming liquid-disordered phase, Ld), we designed Synthetic Exosome-Like Nanoparticles (SELN) with ratios Lo/Ld from 3.0 to 6.0 framing that of SOJ-6 cell exosomes. SELN decreased tumor cell survival, the higher the Lo/Ld ratio, the lower the cell survival. This decreased survival was due to activation of cell death with inhibition of Notch pathway. FRET analyses indicated fusions/exchanges of SELN with cell membranes. Fluorescent SELN co-localized with the ganglioside GM1 then with Rab5A, markers of lipid microdomains and of early endosomes, respectively. These interactions occurred at lipid microdomains of plasma and/or endosome membranes where the Notch-1 pathway matures. We thus demonstrated a major role for lipids in interactions between SELN and tumor cells, and in the ensued cell death. To our knowledge this is the first report on such effects of lipidic nanoparticles on tumor cell behavior. This may have implications in tumor progression.http://europepmc.org/articles/PMC3477155?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Sadia Beloribi
Elodie Ristorcelli
Gilles Breuzard
Françoise Silvy
Justine Bertrand-Michel
Evelyne Beraud
Alain Verine
Dominique Lombardo
spellingShingle Sadia Beloribi
Elodie Ristorcelli
Gilles Breuzard
Françoise Silvy
Justine Bertrand-Michel
Evelyne Beraud
Alain Verine
Dominique Lombardo
Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
PLoS ONE
author_facet Sadia Beloribi
Elodie Ristorcelli
Gilles Breuzard
Françoise Silvy
Justine Bertrand-Michel
Evelyne Beraud
Alain Verine
Dominique Lombardo
author_sort Sadia Beloribi
title Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
title_short Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
title_full Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
title_fullStr Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
title_full_unstemmed Exosomal lipids impact notch signaling and induce death of human pancreatic tumoral SOJ-6 cells.
title_sort exosomal lipids impact notch signaling and induce death of human pancreatic tumoral soj-6 cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Exosomes are of increasing interest as alternative mode of cell-to-cell communication. We previously reported that exosomes secreted by human SOJ-6 pancreatic tumor cells induce (glyco)protein ligand-independent cell death and inhibit Notch-1 pathway, this latter being particularly active during carcinogenesis and in cancer stem cells. Therefore, we asked whether exosomal lipids were key-elements for cell death and hypothesized that cholesterol-rich membrane microdomains were privileged sites of exosome interactions with tumor cells. To address these questions and based on the lipid composition of exosomes from SOJ-6 cells (Ristorcelli et al. (2008) FASEB J. 22; 3358-3369) enriched in cholesterol and sphingomyelin (lipids forming liquid-ordered phase, Lo) and depleted in phospholipids (lipids forming liquid-disordered phase, Ld), we designed Synthetic Exosome-Like Nanoparticles (SELN) with ratios Lo/Ld from 3.0 to 6.0 framing that of SOJ-6 cell exosomes. SELN decreased tumor cell survival, the higher the Lo/Ld ratio, the lower the cell survival. This decreased survival was due to activation of cell death with inhibition of Notch pathway. FRET analyses indicated fusions/exchanges of SELN with cell membranes. Fluorescent SELN co-localized with the ganglioside GM1 then with Rab5A, markers of lipid microdomains and of early endosomes, respectively. These interactions occurred at lipid microdomains of plasma and/or endosome membranes where the Notch-1 pathway matures. We thus demonstrated a major role for lipids in interactions between SELN and tumor cells, and in the ensued cell death. To our knowledge this is the first report on such effects of lipidic nanoparticles on tumor cell behavior. This may have implications in tumor progression.
url http://europepmc.org/articles/PMC3477155?pdf=render
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