Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress

Nicole C.A. van Engeland; Freddy Suarez Rodriguez; Adolfo Rivero-Müller; Tommaso Ristori; Camille L. Duran; Oscar M.J.A. Stassen; Daniel Antfolk; Rob C.H. Driessen; Saku Ruohonen; Suvi T. Ruohonen; Salla Nuutinen; Eriika Savontaus; Sandra Loerakker; Kayla J. Bayless; Marika Sjöqvist; Carlijn V.C. Bouten; John E. Eriksson; Cecilia M. Sahlgren

doi:10.1038/s41598-019-48218-w

Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress

Nicole C.A. van Engeland, Freddy Suarez Rodriguez, Adolfo Rivero-Müller, Tommaso Ristori, Camille L. Duran, Oscar M.J.A. Stassen, Daniel Antfolk, Rob C.H. Driessen, Saku Ruohonen, Suvi T. Ruohonen, Salla Nuutinen, Eriika Savontaus, Sandra Loerakker, Kayla J. Bayless, Marika Sjöqvist, Carlijn V.C. Bouten, John E. Eriksson, Cecilia M. Sahlgren

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Abstract

The intermediate filament (IF) cytoskeleton has been proposed to regulate morphogenic processes by integrating the cell fate signaling machinery with mechanical cues. Signaling between endothelial cells (ECs) and vascular smooth muscle cells (VSMCs) through the Notch pathway regulates arterial remodeling in response to changes in blood flow. Here we show that the IF-protein vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic forces. Vimentin is important for Notch transactivation by ECs and vimentin knockout mice (VimKO) display disrupted VSMC differentiation and adverse remodeling in aortic explants and in vivo. Shear stress increases Jagged1 levels and Notch activation in a vimentin-dependent manner. Shear stress induces phosphorylation of vimentin at serine 38 and phosphorylated vimentin interacts with Jagged1 and increases Notch activation potential. Reduced Jagged1-Notch transactivation strength disrupts lateral signal induction through the arterial wall leading to adverse remodeling. Taken together we demonstrate that vimentin forms a central part of a mechanochemical transduction pathway that regulates multilayer communication and structural homeostasis of the arterial wall.

Original language	English (US)
Article number	12415
Journal	Scientific reports
Volume	9
Issue number	1
DOIs	https://doi.org/10.1038/s41598-019-48218-w
State	Published - Dec 1 2019
Externally published	Yes

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van Engeland, N. C. A., Suarez Rodriguez, F., Rivero-Müller, A., Ristori, T., Duran, C. L., Stassen, O. M. J. A., Antfolk, D., Driessen, R. C. H., Ruohonen, S., Ruohonen, S. T., Nuutinen, S., Savontaus, E., Loerakker, S., Bayless, K. J., Sjöqvist, M., Bouten, C. V. C., Eriksson, J. E., & Sahlgren, C. M. (2019). Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress. Scientific reports, 9(1), Article 12415. https://doi.org/10.1038/s41598-019-48218-w

van Engeland, NCA, Suarez Rodriguez, F, Rivero-Müller, A, Ristori, T, Duran, CL, Stassen, OMJA, Antfolk, D, Driessen, RCH, Ruohonen, S, Ruohonen, ST, Nuutinen, S, Savontaus, E, Loerakker, S, Bayless, KJ, Sjöqvist, M, Bouten, CVC, Eriksson, JE & Sahlgren, CM 2019, 'Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress', Scientific reports, vol. 9, no. 1, 12415. https://doi.org/10.1038/s41598-019-48218-w

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title = "Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress",

abstract = "The intermediate filament (IF) cytoskeleton has been proposed to regulate morphogenic processes by integrating the cell fate signaling machinery with mechanical cues. Signaling between endothelial cells (ECs) and vascular smooth muscle cells (VSMCs) through the Notch pathway regulates arterial remodeling in response to changes in blood flow. Here we show that the IF-protein vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic forces. Vimentin is important for Notch transactivation by ECs and vimentin knockout mice (VimKO) display disrupted VSMC differentiation and adverse remodeling in aortic explants and in vivo. Shear stress increases Jagged1 levels and Notch activation in a vimentin-dependent manner. Shear stress induces phosphorylation of vimentin at serine 38 and phosphorylated vimentin interacts with Jagged1 and increases Notch activation potential. Reduced Jagged1-Notch transactivation strength disrupts lateral signal induction through the arterial wall leading to adverse remodeling. Taken together we demonstrate that vimentin forms a central part of a mechanochemical transduction pathway that regulates multilayer communication and structural homeostasis of the arterial wall.",

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AU - van Engeland, Nicole C.A.

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AU - Ristori, Tommaso

AU - Duran, Camille L.

AU - Stassen, Oscar M.J.A.

AU - Antfolk, Daniel

AU - Driessen, Rob C.H.

AU - Ruohonen, Saku

AU - Ruohonen, Suvi T.

AU - Nuutinen, Salla

AU - Savontaus, Eriika

AU - Loerakker, Sandra

AU - Bayless, Kayla J.

AU - Sjöqvist, Marika

AU - Bouten, Carlijn V.C.

AU - Eriksson, John E.

AU - Sahlgren, Cecilia M.

PY - 2019/12/1

Y1 - 2019/12/1

N2 - The intermediate filament (IF) cytoskeleton has been proposed to regulate morphogenic processes by integrating the cell fate signaling machinery with mechanical cues. Signaling between endothelial cells (ECs) and vascular smooth muscle cells (VSMCs) through the Notch pathway regulates arterial remodeling in response to changes in blood flow. Here we show that the IF-protein vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic forces. Vimentin is important for Notch transactivation by ECs and vimentin knockout mice (VimKO) display disrupted VSMC differentiation and adverse remodeling in aortic explants and in vivo. Shear stress increases Jagged1 levels and Notch activation in a vimentin-dependent manner. Shear stress induces phosphorylation of vimentin at serine 38 and phosphorylated vimentin interacts with Jagged1 and increases Notch activation potential. Reduced Jagged1-Notch transactivation strength disrupts lateral signal induction through the arterial wall leading to adverse remodeling. Taken together we demonstrate that vimentin forms a central part of a mechanochemical transduction pathway that regulates multilayer communication and structural homeostasis of the arterial wall.

AB - The intermediate filament (IF) cytoskeleton has been proposed to regulate morphogenic processes by integrating the cell fate signaling machinery with mechanical cues. Signaling between endothelial cells (ECs) and vascular smooth muscle cells (VSMCs) through the Notch pathway regulates arterial remodeling in response to changes in blood flow. Here we show that the IF-protein vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic forces. Vimentin is important for Notch transactivation by ECs and vimentin knockout mice (VimKO) display disrupted VSMC differentiation and adverse remodeling in aortic explants and in vivo. Shear stress increases Jagged1 levels and Notch activation in a vimentin-dependent manner. Shear stress induces phosphorylation of vimentin at serine 38 and phosphorylated vimentin interacts with Jagged1 and increases Notch activation potential. Reduced Jagged1-Notch transactivation strength disrupts lateral signal induction through the arterial wall leading to adverse remodeling. Taken together we demonstrate that vimentin forms a central part of a mechanochemical transduction pathway that regulates multilayer communication and structural homeostasis of the arterial wall.

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Vimentin regulates Notch signaling strength and arterial remodeling in response to hemodynamic stress

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