| Literature DB >> 34162963 |
Gautier Follain1,2,3,4,5, Naël Osmani1,2,3,4, Valentin Gensbittel1,2,3,4, Nandini Asokan1,2,3,4, Annabel Larnicol1,2,3,4, Luc Mercier1,2,3,4,6, Maria Jesus Garcia-Leon1,2,3,4, Ignacio Busnelli1,2,3,4, Angelique Pichot1,2,3, Nicodème Paul1,2,3, Raphaël Carapito1,2,3, Seiamak Bahram1,2,3, Olivier Lefebvre7,8,9,10, Jacky G Goetz11,12,13,14.
Abstract
Tumor progression and metastatic dissemination are driven by cell-intrinsic and biomechanical cues that favor the growth of life-threatening secondary tumors. We recently identified pro-metastatic vascular regions with blood flow profiles that are permissive for the arrest of circulating tumor cells. We have further established that such flow profiles also control endothelial remodeling, which favors extravasation of arrested CTCs. Yet, how shear forces control endothelial remodeling is unknown. In the present work, we aimed at dissecting the cellular and molecular mechanisms driving blood flow-dependent endothelial remodeling. Transcriptomic analysis of endothelial cells revealed that blood flow enhanced VEGFR signaling, among others. Using a combination of in vitro microfluidics and intravital imaging in zebrafish embryos, we now demonstrate that the early flow-driven endothelial response can be prevented upon specific inhibition of VEGFR tyrosine kinase and subsequent signaling. Inhibitory targeting of VEGFRs reduced endothelial remodeling and subsequent metastatic extravasation. These results confirm the importance of VEGFR-dependent endothelial remodeling as a driving force of CTC extravasation and metastatic dissemination. Furthermore, the present work suggests that therapies targeting endothelial remodeling might be a relevant clinical strategy in order to impede metastatic progression.Entities:
Year: 2021 PMID: 34162963 DOI: 10.1038/s41598-021-92515-2
Source DB: PubMed Journal: Sci Rep ISSN: 2045-2322 Impact factor: 4.379