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Heterogeneity in VEGF Receptor-2 mobility and organization on the endothelial cell surface leads to diverse activation models by VEGF

biorxiv. 2020; 
Bruno da Rocha-Azevedo,  Sungsoo Lee,  Aparajita Dasgupta,  Anthony R. Vega,  Luciana R. de Oliveira,  Tae Kim,  Mark Kittisopikul,  Khuloud Jaqaman
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Recombinant Proteins For stimulation, cells were treated with 2 nM VEGF-A165 (Genscript, Piscataway, NJ) at time points indicated in time-course analysis or Western Blots. Get A Quote

摘要

The nanoscale organization of cell surface receptors plays an important role in signaling. We determined this organization and its relation to receptor activation for VEGF Receptor-2 (VEGFR-2), a critical receptor tyrosine kinase in endothelial cells (ECs), by combining live-cell single-molecule imaging of endogenous VEGFR-2 with rigorous computational analysis. We found that surface VEGFR-2 can be mobile or immobile/confined, and monomeric or non-monomeric, with a complex interplay between the two. The mobility and interaction heterogeneity of VEGFR-2 in the basal state led to heterogeneity in the sequence of steps leading to VEGFR-2 activation by VEGF. Specifically, we found that VEGF can bind to both monomer... More

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