Endothelial Bmp4 Is Induced During Arterial Remodeling: Effects on Smooth Muscle Cell Migration and Proliferation

Matthew A. Corriere; Chris M. Rogers; Jonathan L. Eliason; JimBob Faulk; Tsutomu Kume; Brigid L M Hogan; Raul J. Guzman

doi:10.1016/j.jss.2007.03.077

Endothelial Bmp4 Is Induced During Arterial Remodeling: Effects on Smooth Muscle Cell Migration and Proliferation

Matthew A. Corriere, Chris M. Rogers, Jonathan L. Eliason, JimBob Faulk, Tsutomu Kume, Brigid L M Hogan, Raul J. Guzman^*

^*Corresponding author for this work

Medicine, Cardiology Division

Research output: Contribution to journal › Article › peer-review

22 Scopus citations

Abstract

Background: Bone morphogenetic proteins (BMPs) are members of the transforming growth factor-beta superfamily of proteins that have multiple functional roles in mammalian development. A role for BMP4 in adult vascular remodeling has recently been suggested. We evaluated the expression of Bmp4 during neointimal lesion development in vivo. Materials and methods: Heterozygous Bmp4^lacZ/+ mice were used to evaluate in vivo Bmp4 expression after carotid ligation. β-galactosidase (β-gal) activity was evaluated in histological sections 1 to 14 d after carotid ligation and this was compared with control carotid arteries. The effects of recombinant human (rh) BMP4 on smooth muscle cell (SMC) migration and proliferation were evaluated using a rat aortic SMC line. We next assessed the effects of BMP4 signaling by over-expressing a constitutively active BMP receptor (BMPR-IA/Alk-3) using adenovirus-mediated gene transfer. SMC proliferation, migration, and apoptosis were evaluated in adenovirus transfected cells. Results: Ligated carotid arteries expressed endothelium-specific β-gal staining after 1 d. Staining intensity increased at both 3 d and 1 wk after ligation and remained stable at 2 weeks while no β-gal staining was observed in control vessels. Endothelial-specific expression of β-galactosidase was confirmed through positive staining for PECAM-1. When human recombinant BMP4 was added to cultured SMCs, it inhibited migration but did not affect cultured SMC proliferation. SMCs infected with adenovirus encoding for the active BMP receptor Alk-3 demonstrated dose-dependent receptor expression. Alk-3 over-expressing cells showed a dose-dependent decrease in proliferation and migration but no effect on apoptosis. Conclusions: These results demonstrate that endothelial Bmp4 expression is upregulated after carotid ligation in vivo, and furthermore, that activating the BMP signaling cascade results in decreased SMC proliferation and migration. This suggests that BMPs may counterbalance the effect of mitogen up-regulation observed during the development of neointimal hyperplasia.

Original language	English (US)
Pages (from-to)	142-149
Number of pages	8
Journal	Journal of Surgical Research
Volume	145
Issue number	1
DOIs	https://doi.org/10.1016/j.jss.2007.03.077
State	Published - Mar 2008

Keywords

BMPs
arterial remodeling
bone morphogenetic proteins
endothelial cell
migration
mouse
proliferation
shear stress
smooth muscle cell

ASJC Scopus subject areas

Surgery

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10.1016/j.jss.2007.03.077

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@article{81cb5e954197427fa39b3f7083acb50a,

title = "Endothelial Bmp4 Is Induced During Arterial Remodeling: Effects on Smooth Muscle Cell Migration and Proliferation",

abstract = "Background: Bone morphogenetic proteins (BMPs) are members of the transforming growth factor-beta superfamily of proteins that have multiple functional roles in mammalian development. A role for BMP4 in adult vascular remodeling has recently been suggested. We evaluated the expression of Bmp4 during neointimal lesion development in vivo. Materials and methods: Heterozygous Bmp4lacZ/+ mice were used to evaluate in vivo Bmp4 expression after carotid ligation. β-galactosidase (β-gal) activity was evaluated in histological sections 1 to 14 d after carotid ligation and this was compared with control carotid arteries. The effects of recombinant human (rh) BMP4 on smooth muscle cell (SMC) migration and proliferation were evaluated using a rat aortic SMC line. We next assessed the effects of BMP4 signaling by over-expressing a constitutively active BMP receptor (BMPR-IA/Alk-3) using adenovirus-mediated gene transfer. SMC proliferation, migration, and apoptosis were evaluated in adenovirus transfected cells. Results: Ligated carotid arteries expressed endothelium-specific β-gal staining after 1 d. Staining intensity increased at both 3 d and 1 wk after ligation and remained stable at 2 weeks while no β-gal staining was observed in control vessels. Endothelial-specific expression of β-galactosidase was confirmed through positive staining for PECAM-1. When human recombinant BMP4 was added to cultured SMCs, it inhibited migration but did not affect cultured SMC proliferation. SMCs infected with adenovirus encoding for the active BMP receptor Alk-3 demonstrated dose-dependent receptor expression. Alk-3 over-expressing cells showed a dose-dependent decrease in proliferation and migration but no effect on apoptosis. Conclusions: These results demonstrate that endothelial Bmp4 expression is upregulated after carotid ligation in vivo, and furthermore, that activating the BMP signaling cascade results in decreased SMC proliferation and migration. This suggests that BMPs may counterbalance the effect of mitogen up-regulation observed during the development of neointimal hyperplasia.",

keywords = "BMPs, arterial remodeling, bone morphogenetic proteins, endothelial cell, migration, mouse, proliferation, shear stress, smooth muscle cell",

author = "Corriere, {Matthew A.} and Rogers, {Chris M.} and Eliason, {Jonathan L.} and JimBob Faulk and Tsutomu Kume and Hogan, {Brigid L M} and Guzman, {Raul J.}",

note = "Funding Information: This research was supported by a Mentored Clinical Scientist Development Award HL069926 from the National Heart, Lung, and Blood Institute (RJG), and grants from the Lifeline Foundation and the William J. von Liebig Foundation.",

year = "2008",

month = mar,

doi = "10.1016/j.jss.2007.03.077",

language = "English (US)",

volume = "145",

pages = "142--149",

journal = "Journal of Surgical Research",

issn = "0022-4804",

publisher = "Academic Press Inc.",

number = "1",

}

TY - JOUR

T1 - Endothelial Bmp4 Is Induced During Arterial Remodeling

T2 - Effects on Smooth Muscle Cell Migration and Proliferation

AU - Corriere, Matthew A.

AU - Rogers, Chris M.

AU - Eliason, Jonathan L.

AU - Faulk, JimBob

AU - Kume, Tsutomu

AU - Hogan, Brigid L M

AU - Guzman, Raul J.

N1 - Funding Information: This research was supported by a Mentored Clinical Scientist Development Award HL069926 from the National Heart, Lung, and Blood Institute (RJG), and grants from the Lifeline Foundation and the William J. von Liebig Foundation.

PY - 2008/3

Y1 - 2008/3

N2 - Background: Bone morphogenetic proteins (BMPs) are members of the transforming growth factor-beta superfamily of proteins that have multiple functional roles in mammalian development. A role for BMP4 in adult vascular remodeling has recently been suggested. We evaluated the expression of Bmp4 during neointimal lesion development in vivo. Materials and methods: Heterozygous Bmp4lacZ/+ mice were used to evaluate in vivo Bmp4 expression after carotid ligation. β-galactosidase (β-gal) activity was evaluated in histological sections 1 to 14 d after carotid ligation and this was compared with control carotid arteries. The effects of recombinant human (rh) BMP4 on smooth muscle cell (SMC) migration and proliferation were evaluated using a rat aortic SMC line. We next assessed the effects of BMP4 signaling by over-expressing a constitutively active BMP receptor (BMPR-IA/Alk-3) using adenovirus-mediated gene transfer. SMC proliferation, migration, and apoptosis were evaluated in adenovirus transfected cells. Results: Ligated carotid arteries expressed endothelium-specific β-gal staining after 1 d. Staining intensity increased at both 3 d and 1 wk after ligation and remained stable at 2 weeks while no β-gal staining was observed in control vessels. Endothelial-specific expression of β-galactosidase was confirmed through positive staining for PECAM-1. When human recombinant BMP4 was added to cultured SMCs, it inhibited migration but did not affect cultured SMC proliferation. SMCs infected with adenovirus encoding for the active BMP receptor Alk-3 demonstrated dose-dependent receptor expression. Alk-3 over-expressing cells showed a dose-dependent decrease in proliferation and migration but no effect on apoptosis. Conclusions: These results demonstrate that endothelial Bmp4 expression is upregulated after carotid ligation in vivo, and furthermore, that activating the BMP signaling cascade results in decreased SMC proliferation and migration. This suggests that BMPs may counterbalance the effect of mitogen up-regulation observed during the development of neointimal hyperplasia.

AB - Background: Bone morphogenetic proteins (BMPs) are members of the transforming growth factor-beta superfamily of proteins that have multiple functional roles in mammalian development. A role for BMP4 in adult vascular remodeling has recently been suggested. We evaluated the expression of Bmp4 during neointimal lesion development in vivo. Materials and methods: Heterozygous Bmp4lacZ/+ mice were used to evaluate in vivo Bmp4 expression after carotid ligation. β-galactosidase (β-gal) activity was evaluated in histological sections 1 to 14 d after carotid ligation and this was compared with control carotid arteries. The effects of recombinant human (rh) BMP4 on smooth muscle cell (SMC) migration and proliferation were evaluated using a rat aortic SMC line. We next assessed the effects of BMP4 signaling by over-expressing a constitutively active BMP receptor (BMPR-IA/Alk-3) using adenovirus-mediated gene transfer. SMC proliferation, migration, and apoptosis were evaluated in adenovirus transfected cells. Results: Ligated carotid arteries expressed endothelium-specific β-gal staining after 1 d. Staining intensity increased at both 3 d and 1 wk after ligation and remained stable at 2 weeks while no β-gal staining was observed in control vessels. Endothelial-specific expression of β-galactosidase was confirmed through positive staining for PECAM-1. When human recombinant BMP4 was added to cultured SMCs, it inhibited migration but did not affect cultured SMC proliferation. SMCs infected with adenovirus encoding for the active BMP receptor Alk-3 demonstrated dose-dependent receptor expression. Alk-3 over-expressing cells showed a dose-dependent decrease in proliferation and migration but no effect on apoptosis. Conclusions: These results demonstrate that endothelial Bmp4 expression is upregulated after carotid ligation in vivo, and furthermore, that activating the BMP signaling cascade results in decreased SMC proliferation and migration. This suggests that BMPs may counterbalance the effect of mitogen up-regulation observed during the development of neointimal hyperplasia.

KW - BMPs

KW - arterial remodeling

KW - bone morphogenetic proteins

KW - endothelial cell

KW - migration

KW - mouse

KW - proliferation

KW - shear stress

KW - smooth muscle cell

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DO - 10.1016/j.jss.2007.03.077

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C2 - 17706674

AN - SCOPUS:38949213376

SN - 0022-4804

VL - 145

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JO - Journal of Surgical Research

JF - Journal of Surgical Research

IS - 1

ER -

Endothelial Bmp4 Is Induced During Arterial Remodeling: Effects on Smooth Muscle Cell Migration and Proliferation

Abstract

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