Journal
INTERNATIONAL JOURNAL OF MOLECULAR SCIENCES
Volume 22, Issue 22, Pages -Publisher
MDPI
DOI: 10.3390/ijms222212417
Keywords
Src; Cbl; Crk; Rac1; Cdc42; RhoA
Funding
- MIUR [L.232,11-12-16]
- Tuscany Region (Bando Regionale Ricerca Salute 2018-MAGIC) [D78D20000910002]
- Swedish Cancer Society [CAN 2017/502, 20 1008 PjF]
- Swedish Research Council [2016-02495, 2020-02563]
- Swedish Research Council [2016-02495, 2020-02563] Funding Source: Swedish Research Council
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The study reveals a signaling pathway triggered by CD93 that regulates actin cytoskeletal dynamics responsible for endothelial cell adhesion.
During angiogenesis, cell adhesion molecules expressed on the endothelial cell surface promote the growth and survival of newly forming vessels. Hence, elucidation of the signaling pathways activated by cell-to-matrix adhesion may assist in the discovery of new targets to be used in antiangiogenic therapy. In proliferating endothelial cells, the single-pass transmembrane glycoprotein CD93 has recently emerged as an important endothelial cell adhesion molecule regulating vascular maturation. In this study, we unveil a signaling pathway triggered by CD93 that regulates actin cytoskeletal dynamics responsible of endothelial cell adhesion. We show that the Src-dependent phosphorylation of CD93 and the adaptor protein Cbl leads to the recruitment of Crk, which works as a downstream integrator in the CD93-mediated signaling. Moreover, confocal microscopy analysis of FRET-based biosensors shows that CD93 drives the coordinated activation of Rac1 and RhoA at the cell edge of spreading cells, thus promoting the establishment of cell polarity and adhesion required for cell motility.
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