3.9 Article

BMP-SMAD signalling output is highly regionalized in cardiovascular and lymphatic endothelial networks

期刊

BMC DEVELOPMENTAL BIOLOGY
卷 16, 期 -, 页码 -

出版社

BMC
DOI: 10.1186/s12861-016-0133-x

关键词

BMP-SMAD signalling; Sprouting angiogenesis; Valve development; Lymphangiogenesis; Endocardium; Phenotype switching; Heterogeneity; Retina; Stochastic expression; Morphogen

资金

  1. VIB
  2. KU Leuven
  3. Interuniversity Attraction Poles Program [IUAP VII/07]
  4. Research Council of the KU Leuven [GOA11/012]
  5. FWO [G0542N13]
  6. Hercules Foundation (InfraMouse) [ZW09-03, AKUL/09/037]

向作者/读者索取更多资源

Background: Bone morphogenetic protein (BMP) signalling has emerged as a fundamental pathway in endothelial cell biology and deregulation of this pathway is implicated in several vascular disorders. BMP signalling output in endothelial cells is highly context-and dose-dependent. Phosphorylation of the BMP intracellular effectors, SMAD1/5/9, is routinely used to monitor BMP signalling activity. To better understand the in vivo context-dependency of BMP-SMAD signalling, we investigated differences in BMP-SMAD transcriptional activity in different vascular beds during mouse embryonic and postnatal stages. For this, we used the BRE::gfp BMP signalling reporter mouse in which the BMP response element (BRE) from the ID1-promotor, a SMAD1/5/9 target gene, drives the expression of GFP. Results: A mosaic pattern of GFP was present in various angiogenic sprouting plexuses and in endocardium of cardiac cushions and trabeculae in the heart. High calibre veins seemed to be more BRE:: gfp transcriptionally active than arteries, and ubiquitous activity was present in embryonic lymphatic vasculature. Postnatal lymphatic vessels showed however only discrete micro-domains of transcriptional activity. Dynamic shifts in transcriptional activity were also observed in the endocardium of the developing heart, with a general decrease in activity over time. Surprisingly, proliferative endothelial cells were almost never GFP-positive. Patches of transcriptional activity seemed to correlate with vasculature undergoing hemodynamic alterations. Conclusion: The BRE:: gfp mouse allows to investigate selective context-dependent aspects of BMP-SMAD signalling. Our data reveals the highly dynamic nature of BMP-SMAD mediated transcriptional regulation in time and space throughout the vascular tree, supporting that BMP-SMAD signalling can be a source of phenotypic diversity in some, but not all, healthy endothelium. This knowledge can provide insight in vascular bed or organ-specific diseases and phenotypic heterogeneity within an endothelial cell population.

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