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Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36

Regulation of circulating free fatty acid (FFA) levels and delivery is crucial to maintain tissue homeostasis. Exosomes are nanomembranous vesicles that are released from diverse cell types and mediate intercellular communication by delivering bioactive molecules. Here, we sought to investigate the...

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Autores principales: Garcia, N. A., González-King, H., Grueso, E., Sánchez, R., Martinez-Romero, A., Jávega, B., O’Connor, J. E., Simons, P. J., Handberg, A., Sepúlveda, P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6541372/
https://www.ncbi.nlm.nih.gov/pubmed/31141569
http://dx.doi.org/10.1371/journal.pone.0217546
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author Garcia, N. A.
González-King, H.
Grueso, E.
Sánchez, R.
Martinez-Romero, A.
Jávega, B.
O’Connor, J. E.
Simons, P. J.
Handberg, A.
Sepúlveda, P.
author_facet Garcia, N. A.
González-King, H.
Grueso, E.
Sánchez, R.
Martinez-Romero, A.
Jávega, B.
O’Connor, J. E.
Simons, P. J.
Handberg, A.
Sepúlveda, P.
author_sort Garcia, N. A.
collection PubMed
description Regulation of circulating free fatty acid (FFA) levels and delivery is crucial to maintain tissue homeostasis. Exosomes are nanomembranous vesicles that are released from diverse cell types and mediate intercellular communication by delivering bioactive molecules. Here, we sought to investigate the uptake of FFAs by circulating exosomes, the delivery of FFA-loaded exosomes to cardiac cells and the possible role of the FFA transporter CD36 in these processes. Circulating exosomes were purified from the serum of healthy donors after an overnight fast (F) or 20 minutes after a high caloric breakfast (postprandial, PP). Western blotting, Immunogold Electron Microscopy and FACS analysis of circulating exosomes showed that CD36 was expressed under both states, but was higher in postprandial-derived exosomes. Flow cytometry analysis showed that circulating exosomes were able to take-up FFA directly from serum. Importantly, preincubation of exosomes with a blocking CD36 antibody significantly impeded uptake of the FFA analogue BODIPY, pointing to the role of CD36 in FFA exosomal uptake. Finally, we found that circulating exosomes could delivery FFA analogue BODIPY into cardiac cells ex vivo and in vivo in a mice model. Overall, our results suggest a novel mechanism in which circulating exosomes can delivery FFAs from the bloodstream to cardiac tissue. Further studies will be necessary to understand this mechanism and, in particular, its potential involvement in metabolic pathologies such as obesity, diabetes and atherosclerosis.
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spelling pubmed-65413722019-06-05 Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36 Garcia, N. A. González-King, H. Grueso, E. Sánchez, R. Martinez-Romero, A. Jávega, B. O’Connor, J. E. Simons, P. J. Handberg, A. Sepúlveda, P. PLoS One Research Article Regulation of circulating free fatty acid (FFA) levels and delivery is crucial to maintain tissue homeostasis. Exosomes are nanomembranous vesicles that are released from diverse cell types and mediate intercellular communication by delivering bioactive molecules. Here, we sought to investigate the uptake of FFAs by circulating exosomes, the delivery of FFA-loaded exosomes to cardiac cells and the possible role of the FFA transporter CD36 in these processes. Circulating exosomes were purified from the serum of healthy donors after an overnight fast (F) or 20 minutes after a high caloric breakfast (postprandial, PP). Western blotting, Immunogold Electron Microscopy and FACS analysis of circulating exosomes showed that CD36 was expressed under both states, but was higher in postprandial-derived exosomes. Flow cytometry analysis showed that circulating exosomes were able to take-up FFA directly from serum. Importantly, preincubation of exosomes with a blocking CD36 antibody significantly impeded uptake of the FFA analogue BODIPY, pointing to the role of CD36 in FFA exosomal uptake. Finally, we found that circulating exosomes could delivery FFA analogue BODIPY into cardiac cells ex vivo and in vivo in a mice model. Overall, our results suggest a novel mechanism in which circulating exosomes can delivery FFAs from the bloodstream to cardiac tissue. Further studies will be necessary to understand this mechanism and, in particular, its potential involvement in metabolic pathologies such as obesity, diabetes and atherosclerosis. Public Library of Science 2019-05-29 /pmc/articles/PMC6541372/ /pubmed/31141569 http://dx.doi.org/10.1371/journal.pone.0217546 Text en © 2019 Garcia et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Garcia, N. A.
González-King, H.
Grueso, E.
Sánchez, R.
Martinez-Romero, A.
Jávega, B.
O’Connor, J. E.
Simons, P. J.
Handberg, A.
Sepúlveda, P.
Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title_full Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title_fullStr Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title_full_unstemmed Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title_short Circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: Possible role of CD36
title_sort circulating exosomes deliver free fatty acids from the bloodstream to cardiac cells: possible role of cd36
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6541372/
https://www.ncbi.nlm.nih.gov/pubmed/31141569
http://dx.doi.org/10.1371/journal.pone.0217546
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