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Force-induced changes of α-catenin conformation stabilize vascular junctions independently of vinculin

Authors :
Marika Meyer zu Brickwedde
Dietmar Vestweber
Giuseppe Trapani
Ute Ipe
Hans R. Schöler
Laura J Braun
Hermann vom Bruch
Britta Trappmann
Martina Schmitt
Stephan Huveneers
Mirsana P. Ebrahimkutty
Noboru Ishiyama
Cao Nguyen Duong
Johan de Rooij
Astrid F. Nottebaum
Mitsuhiko Ikura
Randy Brückner
Medical Biochemistry
ACS - Atherosclerosis & ischemic syndromes
ACS - Microcirculation
Source :
Journal of Cell Science, article-version (VoR) Version of Record, Journal of cell science, 134(24). Company of Biologists Ltd
Publication Year :
2021

Abstract

Cadherin-mediated cell adhesion requires anchoring via the β-catenin–α-catenin complex to the actin cytoskeleton, yet, α-catenin only binds F-actin weakly. A covalent fusion of VE-cadherin to α-catenin enhances actin anchorage in endothelial cells and strongly stabilizes endothelial junctions in vivo, blocking inflammatory responses. Here, we have analyzed the underlying mechanism. We found that VE-cadherin–α-catenin constitutively recruits the actin adaptor vinculin. However, removal of the vinculin-binding region of α-catenin did not impair the ability of VE-cadherin–α-catenin to enhance junction integrity. Searching for an alternative explanation for the junction-stabilizing mechanism, we found that an antibody-defined epitope, normally buried in a short α1-helix of the actin-binding domain (ABD) of α-catenin, is openly displayed in junctional VE-cadherin–α-catenin chimera. We found that this epitope became exposed in normal α-catenin upon triggering thrombin-induced tension across the VE-cadherin complex. These results suggest that the VE-cadherin–α-catenin chimera stabilizes endothelial junctions due to conformational changes in the ABD of α-catenin that support constitutive strong binding to actin.<br />Summary: There are novel antibody epitopes at the actin-binding domain of α-catenin that correlate with high affinity binding and are exposed in junction-stabilizing VE-cadherin–α-catenin fusion proteins.

Details

Language :
English
ISSN :
00219533
Volume :
134
Issue :
24
Database :
OpenAIRE
Journal :
Journal of cell science
Accession number :
edsair.doi.dedup.....47461191fa45546406534ba75f0e1b68
Full Text :
https://doi.org/10.1242/jcs.259012