Inhibition of Endothelial Notch Signaling Impairs Fatty Acid Transport and Leads to Metabolic and Vascular Remodeling of the Adult Heart-Reference-Cited by-同舟云学术

Inhibition of Endothelial Notch Signaling Impairs Fatty Acid Transport and Leads to Metabolic and Vascular Remodeling of the Adult Heart

Published:2018-06-12 Issue:24 Volume:137 Page:2592-2608
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Jabs Markus¹,Rose Adam J.²³,Lehmann Lorenz H.⁴⁵⁶,Taylor Jacqueline¹,Moll Iris¹,Sijmonsma Tjeerd P.²,Herberich Stefanie E.¹,Sauer Sven W.⁷,Poschet Gernot⁸,Federico Giuseppina⁹,Mogler Carolin¹⁰,Weis Eva-Maria¹,Augustin Hellmut G.¹¹¹²,Yan Minhong¹³,Gretz Norbert¹⁴,Schmid Roland M.¹⁵,Adams Ralf H.¹⁶,Gröne Hermann-Joseph⁹,Hell Rüdiger⁸,Okun Jürgen G.⁷,Backs Johannes⁴⁶,Nawroth Peter P.¹⁷,Herzig Stephan¹⁸,Fischer Andreas¹¹⁷¹²

Affiliation:

1. Division Vascular Signaling and Cancer (M.J., J.T., I.M., S.E.H., E.-M.W., A.F.)

2. Joint Division Molecular Metabolic Control, German Cancer Research Center, Heidelberg, Center for Molecular Biology, and University Hospital Heidelberg, Germany (A.J.R., T.P.S.).

3. Nutrient Metabolism and Signaling Lab, Department of Biochemistry and Molecular Biology, Monash Biomedicine Discovery Institute, Monash University, Clayton, Australia (A.J.R.).

4. Department of Molecular Cardiology and Epigenetics (L.H.L., J.B.)

5. Department of Cardiology (L.H.L.)

6. Center for Cardiovascular Research, Partner Site Heidelberg/Mannheim (L.H.L., J.B.).

7. Department of General Pediatrics, Division of Inherited Metabolic Diseases, University Children’s Hospital Heidelberg, Germany (S.W.S., J.G.O.).

8. Center for Organismal Studies (G.P., R.H.)

9. Division Cellular and Molecular Pathology (G.F., H.-J.G), German Cancer Research Center, Heidelberg.

10. Institute for Pathology (C.M.)

11. Division Vascular Oncology and Metastasis (H.G.A.)

12. European Center for Angioscience (H.G.A., A.F.)

13. Technical University of Munich, Germany. Department of Molecular Oncology, Genentech, South San Francisco, CA (M.Y.).

14. Medical Research Center Mannheim (N.G.), University of Heidelberg, Germany.

15. Department of Medicine II, Klinikum rechts der Isar (R.M.S.)

16. Department of Tissue Morphogenesis, Max Planck Institute for Molecular Biomedicine, Faculty of Medicine, University of Münster, Germany (R.H.A.).

17. Department of Endocrinology and Clinical Chemistry (P.P.N., A.F.), University Hospital Heidelberg, Germany.

18. Institute for Diabetes and Cancer (IDC), Joint Heidelberg-IDC Translational Diabetes Program, Helmholtz Center Munich, Neuherberg, Germany (S.H.).

Abstract

Background: Nutrients are transported through endothelial cells before being metabolized in muscle cells. However, little is known about the regulation of endothelial transport processes. Notch signaling is a critical regulator of metabolism and angiogenesis during development. Here, we studied how genetic and pharmacological manipulation of endothelial Notch signaling in adult mice affects endothelial fatty acid transport, cardiac angiogenesis, and heart function. Methods: Endothelial-specific Notch inhibition was achieved by conditional genetic inactivation of Rbp-jκ in adult mice to analyze fatty acid metabolism and heart function. Wild-type mice were treated with neutralizing antibodies against the Notch ligand Delta-like 4. Fatty acid transport was studied in cultured endothelial cells and transgenic mice. Results: Treatment of wild-type mice with Delta-like 4 neutralizing antibodies for 8 weeks impaired fractional shortening and ejection fraction in the majority of mice. Inhibition of Notch signaling specifically in the endothelium of adult mice by genetic ablation of Rbp-jκ caused heart hypertrophy and failure. Impaired heart function was preceded by alterations in fatty acid metabolism and an increase in cardiac blood vessel density. Endothelial Notch signaling controlled the expression of endothelial lipase, Angptl4, CD36, and Fabp4, which are all needed for fatty acid transport across the vessel wall. In endothelial-specific Rbp-jκ–mutant mice, lipase activity and transendothelial transport of long-chain fatty acids to muscle cells were impaired. In turn, lipids accumulated in the plasma and liver. The attenuated supply of cardiomyocytes with long-chain fatty acids was accompanied by higher glucose uptake, increased concentration of glycolysis intermediates, and mTOR-S6K signaling. Treatment with the mTOR inhibitor rapamycin or displacing glucose as cardiac substrate by feeding a ketogenic diet prolonged the survival of endothelial-specific Rbp-jκ–deficient mice. Conclusions: This study identifies Notch signaling as a novel regulator of fatty acid transport across the endothelium and as an essential repressor of angiogenesis in the adult heart. The data imply that the endothelium controls cardiomyocyte metabolism and function.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

Link

https://www.ahajournals.org/doi/pdf/10.1161/CIRCULATIONAHA.117.029733

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