Marcksl1 modulates endothelial cell mechanoresponse to haemodynamic forces to control blood vessel shape and size.
Igor KondrychynDouglas J KellyNúria Taberner CarreteroAkane NomoriKagayaki KatoJeronica ChongHiroyuki NakajimaSatoru OkudaNaoki MochizukiLi-Kun PhngPublished in: Nature communications (2020)
The formation of vascular tubes is driven by extensive changes in endothelial cell (EC) shape. Here, we have identified a role of the actin-binding protein, Marcksl1, in modulating the mechanical properties of EC cortex to regulate cell shape and vessel structure during angiogenesis. Increasing and depleting Marcksl1 expression level in vivo results in an increase and decrease, respectively, in EC size and the diameter of microvessels. Furthermore, endothelial overexpression of Marcksl1 induces ectopic blebbing on both apical and basal membranes, during and after lumen formation, that is suppressed by reduced blood flow. High resolution imaging reveals that Marcksl1 promotes the formation of linear actin bundles and decreases actin density at the EC cortex. Our findings demonstrate that a balanced network of linear and branched actin at the EC cortex is essential in conferring cortical integrity to resist the deforming forces of blood flow to regulate vessel structure.
Keyphrases
- blood flow
- endothelial cells
- high resolution
- binding protein
- functional connectivity
- cell migration
- high glucose
- poor prognosis
- signaling pathway
- cell proliferation
- mass spectrometry
- single cell
- vascular endothelial growth factor
- cell therapy
- photodynamic therapy
- mesenchymal stem cells
- optic nerve
- fluorescence imaging
- ultrasound guided
- tandem mass spectrometry