Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice

Previous studies using B16BL6-derived exosomes labelled with gLuc–lactadherin (gLuc-LA), a fusion protein of Gaussia luciferase (a reporter protein) and lactadherin (an exosome-tropic protein), showed that the exosomes quickly disappeared from the systemic circulation after intravenous injection in...

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Autores principales: Imai, Takafumi, Takahashi, Yuki, Nishikawa, Makiya, Kato, Kana, Morishita, Masaki, Yamashita, Takuma, Matsumoto, Akihiro, Charoenviriyakul, Chonlada, Takakura, Yoshinobu
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Co-Action Publishing 2015
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Original Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4323410/
https://www.ncbi.nlm.nih.gov/pubmed/25669322
http://dx.doi.org/10.3402/jev.v4.26238
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author Imai, Takafumi
Takahashi, Yuki
Nishikawa, Makiya
Kato, Kana
Morishita, Masaki
Yamashita, Takuma
Matsumoto, Akihiro
Charoenviriyakul, Chonlada
Takakura, Yoshinobu
author_facet Imai, Takafumi
Takahashi, Yuki
Nishikawa, Makiya
Kato, Kana
Morishita, Masaki
Yamashita, Takuma
Matsumoto, Akihiro
Charoenviriyakul, Chonlada
Takakura, Yoshinobu
author_sort Imai, Takafumi
collection PubMed
description Previous studies using B16BL6-derived exosomes labelled with gLuc–lactadherin (gLuc-LA), a fusion protein of Gaussia luciferase (a reporter protein) and lactadherin (an exosome-tropic protein), showed that the exosomes quickly disappeared from the systemic circulation after intravenous injection in mice. In the present study, the mechanism of rapid clearance of intravenously injected B16BL6 exosomes was investigated. gLuc-LA-labelled exosomes were obtained from supernatant of B16BL6 cells after transfection with a plasmid DNA encoding gLuc-LA. Labelling was stable when the exosomes were incubated in serum. By using B16BL6 exosomes labelled with PKH26, a lipophilic fluorescent dye, it was demonstrated that PKH26-labelled B16BL6 exosomes were taken up by macrophages in the liver and spleen but not in the lung, while PKH26-labelled exosomes were taken up by the endothelial cells in the lung. Subsequently, gLuc-LA-labelled B16BL6 exosomes were injected into macrophage-depleted mice prepared by injection with clodronate-containing liposomes. The clearance of the intravenously injected B16BL6 exosomes from the blood circulation was much slower in macrophage-depleted mice than that in untreated mice. These results indicate that macrophages play important roles in the clearance of intravenously injected B16BL6 exosomes from the systemic circulation.
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spelling pubmed-43234102015-02-23 Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice Imai, Takafumi Takahashi, Yuki Nishikawa, Makiya Kato, Kana Morishita, Masaki Yamashita, Takuma Matsumoto, Akihiro Charoenviriyakul, Chonlada Takakura, Yoshinobu J Extracell Vesicles Original Research Article Previous studies using B16BL6-derived exosomes labelled with gLuc–lactadherin (gLuc-LA), a fusion protein of Gaussia luciferase (a reporter protein) and lactadherin (an exosome-tropic protein), showed that the exosomes quickly disappeared from the systemic circulation after intravenous injection in mice. In the present study, the mechanism of rapid clearance of intravenously injected B16BL6 exosomes was investigated. gLuc-LA-labelled exosomes were obtained from supernatant of B16BL6 cells after transfection with a plasmid DNA encoding gLuc-LA. Labelling was stable when the exosomes were incubated in serum. By using B16BL6 exosomes labelled with PKH26, a lipophilic fluorescent dye, it was demonstrated that PKH26-labelled B16BL6 exosomes were taken up by macrophages in the liver and spleen but not in the lung, while PKH26-labelled exosomes were taken up by the endothelial cells in the lung. Subsequently, gLuc-LA-labelled B16BL6 exosomes were injected into macrophage-depleted mice prepared by injection with clodronate-containing liposomes. The clearance of the intravenously injected B16BL6 exosomes from the blood circulation was much slower in macrophage-depleted mice than that in untreated mice. These results indicate that macrophages play important roles in the clearance of intravenously injected B16BL6 exosomes from the systemic circulation. Co-Action Publishing 2015-02-09 /pmc/articles/PMC4323410/ /pubmed/25669322 http://dx.doi.org/10.3402/jev.v4.26238 Text en © 2015 Takafumi Imai et al. http://creativecommons.org/licenses/by-nc-nd/3.0/ This is an Open Access article distributed under the terms of the Creative Commons Attribution-Noncommercial 3.0 Unported License, permitting all non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Research Article
Imai, Takafumi
Takahashi, Yuki
Nishikawa, Makiya
Kato, Kana
Morishita, Masaki
Yamashita, Takuma
Matsumoto, Akihiro
Charoenviriyakul, Chonlada
Takakura, Yoshinobu
Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title_full Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title_fullStr Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title_full_unstemmed Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title_short Macrophage-dependent clearance of systemically administered B16BL6-derived exosomes from the blood circulation in mice
title_sort macrophage-dependent clearance of systemically administered b16bl6-derived exosomes from the blood circulation in mice
topic Original Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4323410/
https://www.ncbi.nlm.nih.gov/pubmed/25669322
http://dx.doi.org/10.3402/jev.v4.26238
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