S-nitrosylation of VASP at cysteine 64 mediates the inflammation-stimulated increase in microvascular permeability

Patricia Zamorano,Natalie Marín,Francisco Córdova,Alejandra Aguilar,Cynthia J. Meininger,Mauricio P. Boric,Nikola Golenhofen,Jorge E. Contreras,Jose Sarmiento,Walter N. Durán,Fabiola A. Sánchez

S-nitrosylation of VASP at cysteine 64 mediates the inflammation-stimulated increase in microvascular permeability

2017

Patricia Zamorano
Natalie Marín
Francisco Córdova
Alejandra Aguilar
Cynthia J. Meininger
Mauricio P. Boric
Nikola Golenhofen
Jorge E. Contreras
Jose Sarmiento
Walter N. Durán
Fabiola A. Sánchez

Here, we demonstrate that S-nitrosylation of vasodilator-stimulated phosphoprotein (VASP) on C64 is a mechanism for the onset of platelet-activating factor-induced hyperpermeability. Our results reveal a dual role of VASP in endothelial permeability. In addition to its well-documented function in barrier integrity, we show that S-nitrosylation of VASP contributes to the onset of endothelial permeability.

Keywords:

Phosphoprotein
Inflammation
Permeability (electromagnetism)
Biochemistry
Vascular permeability
S-Nitrosylation
Nitric oxide
Tyrosine phosphorylation
Barrier function
Cell biology
Biology
Enos
Cysteine

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