Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.

Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.

Red wine polyphenol compounds (RWPC) exert paradoxical effects depending on the dose on post-ischemic neovascularisation. Low dose RWPC (0.2 mg/kg/day) is pro-angiogenic, whereas high dose (20 mg/kg/day) is anti-angiogenic. We recently reported that the endothelial effect of RWPC is mediated through...

Full description

Bibliographic Details
Main Authors: Matthieu Chalopin, Raffaella Soleti, Tarek Benameur, Angela Tesse, Sébastien Faure, Maria Carmen Martínez, Ramaroson Andriantsitohaina
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2014-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC4192547?pdf=render
id doaj-b9570b4805c94123acad596066f659f3
record_format Article
spelling doaj-b9570b4805c94123acad596066f659f32020-11-25T01:36:38ZengPublic Library of Science (PLoS)PLoS ONE1932-62032014-01-01910e11008010.1371/journal.pone.0110080Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.Matthieu ChalopinRaffaella SoletiTarek BenameurAngela TesseSébastien FaureMaria Carmen MartínezRamaroson AndriantsitohainaRed wine polyphenol compounds (RWPC) exert paradoxical effects depending on the dose on post-ischemic neovascularisation. Low dose RWPC (0.2 mg/kg/day) is pro-angiogenic, whereas high dose (20 mg/kg/day) is anti-angiogenic. We recently reported that the endothelial effect of RWPC is mediated through the activation of a redox-sensitive pathway, mitochondrial biogenesis and the activation of α isoform of the estrogen receptor (ERα). Here, we investigated the implication of ERα on angiogenic properties of RWPC. Using ovariectomized mice lacking ERα treated with high dose of RWPC after hindlimb ischemia, we examined blood flow reperfusion, vascular density, nitric oxide (NO) production, expression and activation of proteins involved in angiogenic process and muscle energy sensing network. As expected, high dose of RWPC treatment reduced both blood flow and vascular density in muscles of mice expressing ERα. These effects were associated with reduced NO production resulting from diminished activity of eNOS. In the absence of RWPC, ERα deficient mice showed a reduced neo-vascularisation associated with a decreased NO production. Surprisingly in mice lacking ERα, high dose of RWPC increased blood flow and capillary density in conjunction with increased NO pathway and production as well as VEGF expression. Of particular interest is the activation of Sirt-1, AMPKα and PGC-1α/β axis in ischemic hindlimb from both strains. Altogether, the results highlight a pro-angiogenic property of RWPC via an ERα-independent mechanism that is associated with an up-regulation of energy sensing network. This study brings a corner stone of a novel pathway for RWPC to correct cardiovascular diseases associated with failed neovascularisation.http://europepmc.org/articles/PMC4192547?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Matthieu Chalopin
Raffaella Soleti
Tarek Benameur
Angela Tesse
Sébastien Faure
Maria Carmen Martínez
Ramaroson Andriantsitohaina
spellingShingle Matthieu Chalopin
Raffaella Soleti
Tarek Benameur
Angela Tesse
Sébastien Faure
Maria Carmen Martínez
Ramaroson Andriantsitohaina
Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
PLoS ONE
author_facet Matthieu Chalopin
Raffaella Soleti
Tarek Benameur
Angela Tesse
Sébastien Faure
Maria Carmen Martínez
Ramaroson Andriantsitohaina
author_sort Matthieu Chalopin
title Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
title_short Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
title_full Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
title_fullStr Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
title_full_unstemmed Red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
title_sort red wine polyphenol compounds favor neovascularisation through estrogen receptor α-independent mechanism in mice.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2014-01-01
description Red wine polyphenol compounds (RWPC) exert paradoxical effects depending on the dose on post-ischemic neovascularisation. Low dose RWPC (0.2 mg/kg/day) is pro-angiogenic, whereas high dose (20 mg/kg/day) is anti-angiogenic. We recently reported that the endothelial effect of RWPC is mediated through the activation of a redox-sensitive pathway, mitochondrial biogenesis and the activation of α isoform of the estrogen receptor (ERα). Here, we investigated the implication of ERα on angiogenic properties of RWPC. Using ovariectomized mice lacking ERα treated with high dose of RWPC after hindlimb ischemia, we examined blood flow reperfusion, vascular density, nitric oxide (NO) production, expression and activation of proteins involved in angiogenic process and muscle energy sensing network. As expected, high dose of RWPC treatment reduced both blood flow and vascular density in muscles of mice expressing ERα. These effects were associated with reduced NO production resulting from diminished activity of eNOS. In the absence of RWPC, ERα deficient mice showed a reduced neo-vascularisation associated with a decreased NO production. Surprisingly in mice lacking ERα, high dose of RWPC increased blood flow and capillary density in conjunction with increased NO pathway and production as well as VEGF expression. Of particular interest is the activation of Sirt-1, AMPKα and PGC-1α/β axis in ischemic hindlimb from both strains. Altogether, the results highlight a pro-angiogenic property of RWPC via an ERα-independent mechanism that is associated with an up-regulation of energy sensing network. This study brings a corner stone of a novel pathway for RWPC to correct cardiovascular diseases associated with failed neovascularisation.
url http://europepmc.org/articles/PMC4192547?pdf=render
work_keys_str_mv AT matthieuchalopin redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT raffaellasoleti redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT tarekbenameur redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT angelatesse redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT sebastienfaure redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT mariacarmenmartinez redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
AT ramarosonandriantsitohaina redwinepolyphenolcompoundsfavorneovascularisationthroughestrogenreceptoraindependentmechanisminmice
_version_ 1725061851082915840

Similar Items