Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis

BACKGROUND: Macrophages play a pivotal role in atherosclerotic plaque development. Recent evidence has suggested the glucagon-like peptide-1 receptor (GLP-1R) agonist, liraglutide, can attenuate pro-inflammatory responses in macrophages. We hypothesized that liraglutide could limit atherosclerosis p...

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Autores principales: Bruen, Robyn, Curley, Sean, Kajani, Sarina, Crean, Daniel, O’Reilly, Marcella E., Lucitt, Margaret B., Godson, Catherine G., McGillicuddy, Fiona C., Belton, Orina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2017
Materias:
Original Investigation
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5674826/
https://www.ncbi.nlm.nih.gov/pubmed/29110715
http://dx.doi.org/10.1186/s12933-017-0626-3
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author Bruen, Robyn
Curley, Sean
Kajani, Sarina
Crean, Daniel
O’Reilly, Marcella E.
Lucitt, Margaret B.
Godson, Catherine G.
McGillicuddy, Fiona C.
Belton, Orina
author_facet Bruen, Robyn
Curley, Sean
Kajani, Sarina
Crean, Daniel
O’Reilly, Marcella E.
Lucitt, Margaret B.
Godson, Catherine G.
McGillicuddy, Fiona C.
Belton, Orina
author_sort Bruen, Robyn
collection PubMed
description BACKGROUND: Macrophages play a pivotal role in atherosclerotic plaque development. Recent evidence has suggested the glucagon-like peptide-1 receptor (GLP-1R) agonist, liraglutide, can attenuate pro-inflammatory responses in macrophages. We hypothesized that liraglutide could limit atherosclerosis progression in vivo via modulation of the inflammatory response. METHODS: Human THP-1 macrophages and bone marrow-derived macrophages, from both wild-type C57BL/6 (WT) and apolipoprotein E null mice (ApoE(−/−)) were used to investigate the effect of liraglutide on the inflammatory response in vitro. In parallel, ApoE(−/−) mice were fed a high-fat (60% calories from fat) high-cholesterol (1%) diet for 8 weeks to induce atherosclerotic disease progression with/without daily 300 μg/kg liraglutide administration for the final 6 weeks. Macrophages were analysed for MΦ1 and MΦ2 macrophage markers by Western blotting, RT-qPCR, ELISA and flow cytometry. Atherosclerotic lesions in aortae from ApoE(−/−) mice were analysed by en face staining and monocyte and macrophage populations from bone marrow derived cells analysed by flow cytometry. RESULTS: Liraglutide decreased atherosclerotic lesion formation in ApoE(−/−) mice coincident with a reduction in pro-inflammatory and increased anti-inflammatory monocyte/macrophage populations in vivo. Liraglutide decreased IL-1beta in MΦ0 THP-1 macrophages and bone marrow-derived macrophages from WT mice and induced a significant increase in the MΦ2 surface marker mannose receptor in both MΦ0 and MΦ2 macrophages. Significant reduction in total lesion development was found with once daily 300 μg/kg liraglutide treatment in ApoE(−/−) mice. Interestingly, liraglutide inhibited disease progression at the iliac bifurcation suggesting that it retards the initiation and development of disease. These results corresponded to attenuated MΦ1 markers (CCR7, IL-6 and TNF-alpha), augmented MΦ2 cell markers (Arg-1, IL-10 and CD163) and finally decreased MΦ1-like monocytes and macrophages from bone marrow-derived cells. CONCLUSIONS: This data supports a therapeutic role for liraglutide as an atheroprotective agent via modulating macrophage cell fate towards MΦ2 pro-resolving macrophages. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12933-017-0626-3) contains supplementary material, which is available to authorized users.
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spelling pubmed-56748262017-11-15 Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis Bruen, Robyn Curley, Sean Kajani, Sarina Crean, Daniel O’Reilly, Marcella E. Lucitt, Margaret B. Godson, Catherine G. McGillicuddy, Fiona C. Belton, Orina Cardiovasc Diabetol Original Investigation BACKGROUND: Macrophages play a pivotal role in atherosclerotic plaque development. Recent evidence has suggested the glucagon-like peptide-1 receptor (GLP-1R) agonist, liraglutide, can attenuate pro-inflammatory responses in macrophages. We hypothesized that liraglutide could limit atherosclerosis progression in vivo via modulation of the inflammatory response. METHODS: Human THP-1 macrophages and bone marrow-derived macrophages, from both wild-type C57BL/6 (WT) and apolipoprotein E null mice (ApoE(−/−)) were used to investigate the effect of liraglutide on the inflammatory response in vitro. In parallel, ApoE(−/−) mice were fed a high-fat (60% calories from fat) high-cholesterol (1%) diet for 8 weeks to induce atherosclerotic disease progression with/without daily 300 μg/kg liraglutide administration for the final 6 weeks. Macrophages were analysed for MΦ1 and MΦ2 macrophage markers by Western blotting, RT-qPCR, ELISA and flow cytometry. Atherosclerotic lesions in aortae from ApoE(−/−) mice were analysed by en face staining and monocyte and macrophage populations from bone marrow derived cells analysed by flow cytometry. RESULTS: Liraglutide decreased atherosclerotic lesion formation in ApoE(−/−) mice coincident with a reduction in pro-inflammatory and increased anti-inflammatory monocyte/macrophage populations in vivo. Liraglutide decreased IL-1beta in MΦ0 THP-1 macrophages and bone marrow-derived macrophages from WT mice and induced a significant increase in the MΦ2 surface marker mannose receptor in both MΦ0 and MΦ2 macrophages. Significant reduction in total lesion development was found with once daily 300 μg/kg liraglutide treatment in ApoE(−/−) mice. Interestingly, liraglutide inhibited disease progression at the iliac bifurcation suggesting that it retards the initiation and development of disease. These results corresponded to attenuated MΦ1 markers (CCR7, IL-6 and TNF-alpha), augmented MΦ2 cell markers (Arg-1, IL-10 and CD163) and finally decreased MΦ1-like monocytes and macrophages from bone marrow-derived cells. CONCLUSIONS: This data supports a therapeutic role for liraglutide as an atheroprotective agent via modulating macrophage cell fate towards MΦ2 pro-resolving macrophages. ELECTRONIC SUPPLEMENTARY MATERIAL: The online version of this article (10.1186/s12933-017-0626-3) contains supplementary material, which is available to authorized users. BioMed Central 2017-11-06 /pmc/articles/PMC5674826/ /pubmed/29110715 http://dx.doi.org/10.1186/s12933-017-0626-3 Text en © The Author(s) 2017 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Original Investigation
Bruen, Robyn
Curley, Sean
Kajani, Sarina
Crean, Daniel
O’Reilly, Marcella E.
Lucitt, Margaret B.
Godson, Catherine G.
McGillicuddy, Fiona C.
Belton, Orina
Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title_full Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title_fullStr Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title_full_unstemmed Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title_short Liraglutide dictates macrophage phenotype in apolipoprotein E null mice during early atherosclerosis
title_sort liraglutide dictates macrophage phenotype in apolipoprotein e null mice during early atherosclerosis
topic Original Investigation
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5674826/
https://www.ncbi.nlm.nih.gov/pubmed/29110715
http://dx.doi.org/10.1186/s12933-017-0626-3
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