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Transcriptional regulation of endothelial blood brain barrier differentiation by Wnt signaling

Project

The brain vasculature has evolved to protect the central nervous system from the constantly changing milieu in the blood stream. Endothelial cells of brain capillaries form the so called blood brain barrier (BBB), an active permeability barrier and transport system which allows a selective passage of nutrients from blood to the nervous tissue. The continuous cross talk of endothelial cells, pericytes and nervous cells influences many vascular functions and determines and maintains the BBB characteristics after birth. Our limited knowledge of the nature of these signals prevents effective therapy of several diseases such as hemorrhagic stroke or brain edema. Furthermore, the development of tools to reversibly ?open? the barrier would strongly improve drug delivery to the brain. In the present project we propose to tackle the problem by studying the transcriptional mechanisms which direct BBB differentiation. This strategy is based on preliminary work which shows that the cross talk between nervous cells and the endothelium is mediated by Wnt factors and downstream beta-catenin transcriptional activity. The understanding of the mechanism of action of Wnt signalling on brain endothelium may yield novel strategies and tools for modulating BBB permeability. The project is divided in three related objectives: 1) to define the mechanism of action and downstream partners of Wnt in brain angiogenesis and BBB differentiation; 2) to use this knowledge to develop an optimized BBB model in vitro and in vivo; 3) to test whether modulation of Wnt signalling may have a therapeutic impact in the regulation of BBB in pathological conditions.

  • Overview
  • Research Areas
  • Publications

Overview

Contributors

LA PORTA CATERINA ANNA MARIA   Scientific Manager  

Type

7PQ_ERC - 7 Programma Quadro_European Research Coucil

Funder

EUROPEAN COMMISSION
External Organization Funding Organization

Date/time interval

August 1, 2011 - July 31, 2016

Project duration

60 months

Research Areas

Concepts (2)


LS3_7 - Cell signalling and cellular interactions - (2013)

LS3_9 - Development, developmental genetics, pattern formation and embryology in animals - (2013)

Keywords (2)

ANGIOGENESIS
SIGNAL TRANSDUCTION PATHWAYS
No Results Found

Publications

Outputs

Sulindac metabolites decrease cerebrovascular malformations in CCM3-knockout mice 
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
2015
Academic Article
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