The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.

The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.

Nogo-B mediates vascular protection and facilitates monocyte- and macrophage-dependent vascular remodeling. PirB is an alternate receptor for Nogo-B, but a role for the Nogo-PirB axis within the vascular system has not been previously reported. We examined whether Nogo-B or PirB play a role in regul...

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Main Authors: Yuka Kondo, Caroline C Jadlowiec, Akihito Muto, Tai Yi, Clinton Protack, Michael J Collins, George Tellides, William C Sessa, Alan Dardik
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3835671?pdf=render
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spelling doaj-479819f1e87f46d3a56f03b6573d45722020-11-25T00:23:37ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-01811e8101910.1371/journal.pone.0081019The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.Yuka KondoCaroline C JadlowiecAkihito MutoTai YiClinton ProtackMichael J CollinsGeorge TellidesWilliam C SessaAlan DardikNogo-B mediates vascular protection and facilitates monocyte- and macrophage-dependent vascular remodeling. PirB is an alternate receptor for Nogo-B, but a role for the Nogo-PirB axis within the vascular system has not been previously reported. We examined whether Nogo-B or PirB play a role in regulating macrophage-mediated vascular remodeling and hypothesized that endothelial Nogo-B regulates vein graft macrophage infiltration via its alternate receptor PirB.Vein grafts were performed using Nogo and PirB wild type and knockout mice. Human vein grafts were similarly analyzed. The hindlimb ischemia model was performed in PirB wild type and knockout mice. Accompanying in vitro work included isolation of macrophages from PirB wild type and knockout mice.Increased Nogo-B and PirB mRNA transcripts and protein expression were observed within mouse and human vein grafts. Both Nogo knockout and PirB knockout vein grafts showed increased wall thickness and increased numbers of F4/80-positive macrophages. Macrophages derived from PirB knockout mice had increased adhesion to fibronectin, increased EC-specific binding, and increased numbers of mRNA transcripts of M2 markers as well as MMP3 and MMP9. PirB knockout vein grafts had increased active MMP9 compared to wild type vein grafts. PirB knockout mice had increased recovery from hindlimb ischemia and increased macrophage infiltration compared to wild type mice.Vein graft adaptation shows increased expression of both Nogo-B and PirB. Loss of PirB, or its endothelial ligand Nogo-B, results in increased inflammatory cell infiltration and vein graft wall thickening. These findings suggest that PirB regulates macrophage activity in vein grafts and that Nogo-B in the vein graft limits macrophage infiltration and vein graft thickening. PirB may play a more general role in regulating macrophage responses to vascular injury. Macrophage inhibition via Nogo-PirB interactions may be an important mechanism regulating vein graft adaptation to the arterial circulation.http://europepmc.org/articles/PMC3835671?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Yuka Kondo
Caroline C Jadlowiec
Akihito Muto
Tai Yi
Clinton Protack
Michael J Collins
George Tellides
William C Sessa
Alan Dardik
spellingShingle Yuka Kondo
Caroline C Jadlowiec
Akihito Muto
Tai Yi
Clinton Protack
Michael J Collins
George Tellides
William C Sessa
Alan Dardik
The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
PLoS ONE
author_facet Yuka Kondo
Caroline C Jadlowiec
Akihito Muto
Tai Yi
Clinton Protack
Michael J Collins
George Tellides
William C Sessa
Alan Dardik
author_sort Yuka Kondo
title The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
title_short The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
title_full The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
title_fullStr The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
title_full_unstemmed The Nogo-B-PirB axis controls macrophage-mediated vascular remodeling.
title_sort nogo-b-pirb axis controls macrophage-mediated vascular remodeling.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Nogo-B mediates vascular protection and facilitates monocyte- and macrophage-dependent vascular remodeling. PirB is an alternate receptor for Nogo-B, but a role for the Nogo-PirB axis within the vascular system has not been previously reported. We examined whether Nogo-B or PirB play a role in regulating macrophage-mediated vascular remodeling and hypothesized that endothelial Nogo-B regulates vein graft macrophage infiltration via its alternate receptor PirB.Vein grafts were performed using Nogo and PirB wild type and knockout mice. Human vein grafts were similarly analyzed. The hindlimb ischemia model was performed in PirB wild type and knockout mice. Accompanying in vitro work included isolation of macrophages from PirB wild type and knockout mice.Increased Nogo-B and PirB mRNA transcripts and protein expression were observed within mouse and human vein grafts. Both Nogo knockout and PirB knockout vein grafts showed increased wall thickness and increased numbers of F4/80-positive macrophages. Macrophages derived from PirB knockout mice had increased adhesion to fibronectin, increased EC-specific binding, and increased numbers of mRNA transcripts of M2 markers as well as MMP3 and MMP9. PirB knockout vein grafts had increased active MMP9 compared to wild type vein grafts. PirB knockout mice had increased recovery from hindlimb ischemia and increased macrophage infiltration compared to wild type mice.Vein graft adaptation shows increased expression of both Nogo-B and PirB. Loss of PirB, or its endothelial ligand Nogo-B, results in increased inflammatory cell infiltration and vein graft wall thickening. These findings suggest that PirB regulates macrophage activity in vein grafts and that Nogo-B in the vein graft limits macrophage infiltration and vein graft thickening. PirB may play a more general role in regulating macrophage responses to vascular injury. Macrophage inhibition via Nogo-PirB interactions may be an important mechanism regulating vein graft adaptation to the arterial circulation.
url http://europepmc.org/articles/PMC3835671?pdf=render
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