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Respiratory Research
Published in: Respiratory Research 1/2011

Open Access 01-12-2011 | Research

Physiologic and molecular consequences of endothelial Bmpr2 mutation

Authors: Susan Majka, Moira Hagen, Thomas Blackwell, Julie Harral, Jennifer A Johnson, Robert Gendron, Helene Paradis, Daniel Crona, James E Loyd, Eva Nozik-Grayck, Kurt R Stenmark, James West

Published in: Respiratory Research | Issue 1/2011

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Abstract

Background

Pulmonary arterial hypertension (PAH) is thought to be driven by dysfunction of pulmonary vascular microendothelial cells (PMVEC). Most hereditary PAH is associated with BMPR2 mutations. However, the physiologic and molecular consequences of expression of BMPR2 mutations in PMVEC are unknown.

Methods

In vivo experiments were performed on adult mice with conditional endothelial-specific expression of the truncation mutation Bmpr2delx4+, with age-matched transactivator-only mice as controls. Phenotype was assessed by RVSP, counts of muscularized vessels and proliferating cells, and staining for thromboses, inflammatory cells, and apoptotic cells. The effects of BMPR2 knockdown in PMVEC by siRNA on rates of apoptosis were assessed. Affymetrix expression arrays were performed on PMVEC isolated and cultured from triple transgenic mice carrying the immortomouse gene, a transactivator, and either control, Bmpr2delx4+ or Bmpr2R899X mutation.

Results

Transgenic mice showed increased RVSP and corresponding muscularization of small vessels, with histologic alterations including thrombosis, increased inflammatory cells, increased proliferating cells, and a moderate increase in apoptotic cells. Expression arrays showed alterations in specific pathways consistent with the histologic changes. Bmpr2delx4+ and Bmpr2R899X mutations resulted in very similar alterations in proliferation, apoptosis, metabolism, and adhesion; Bmpr2delx4+ cells showed upregulation of platelet adhesion genes and cytokines not seen in Bmpr2R899X PMVEC. Bmpr2 mutation in PMVEC does not cause a loss of differentiation markers as was seen with Bmpr2 mutation in smooth muscle cells.

Conclusions

Bmpr2 mutation in PMVEC in vivo may drive PAH through multiple, potentially independent, downstream mechanisms, including proliferation, apoptosis, inflammation, and thrombosis.
Appendix
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Metadata
Title
Physiologic and molecular consequences of endothelial Bmpr2 mutation
Authors
Susan Majka
Moira Hagen
Thomas Blackwell
Julie Harral
Jennifer A Johnson
Robert Gendron
Helene Paradis
Daniel Crona
James E Loyd
Eva Nozik-Grayck
Kurt R Stenmark
James West
Publication date
01-12-2011
Publisher
BioMed Central
Published in
Respiratory Research / Issue 1/2011
Electronic ISSN: 1465-993X
DOI
https://doi.org/10.1186/1465-9921-12-84

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