Systemic VEGF inhibition accelerates experimental atherosclerosis and disrupts endothelial homeostasis--implications for cardiovascular safety

Stephan Winnik; Christine Lohmann; Giovanni Siciliani; Tobias von Lukowicz; Kira Kuschnerus; Nicolle Kraenkel; Chad E Brokopp; Frank Enseleit; Stephan Michels; Frank Ruschitzka; Thomas F Lüscher; Christian M Matter

doi:10.1016/j.ijcard.2013.03.010

Systemic VEGF inhibition accelerates experimental atherosclerosis and disrupts endothelial homeostasis--implications for cardiovascular safety

Int J Cardiol. 2013 Oct 3;168(3):2453-61. doi: 10.1016/j.ijcard.2013.03.010. Epub 2013 Apr 2.

Authors

Stephan Winnik¹, Christine Lohmann, Giovanni Siciliani, Tobias von Lukowicz, Kira Kuschnerus, Nicolle Kraenkel, Chad E Brokopp, Frank Enseleit, Stephan Michels, Frank Ruschitzka, Thomas F Lüscher, Christian M Matter

Affiliation

¹ Division of Cardiology, University Hospital Zurich, Zurich, Switzerland; Cardiovascular Research, Institute of Physiology, University of Zurich, Zurich, Switzerland.

PMID: 23561917
DOI: 10.1016/j.ijcard.2013.03.010

Abstract

Objectives: This study sought to examine the effects and underlying mechanisms of systemic VEGF inhibition in experimental atherosclerosis and aortic endothelial cells.

Background: Pharmacological inhibition of vascular endothelial growth factor (VEGF), a major mediator of angiogenesis, has become a widely applied treatment of certain cancers and multiple ocular diseases including age-related macular degeneration. However, recent clinical trials raise concern for systemic vascular adverse effects, prompting the Food and Drug Administration to revoke the approval of bevacizumab for metastatic breast cancer.

Methods: Eight-week old apolipoprotein E knockout mice received a high-cholesterol diet (1.25% cholesterol) for 24 weeks and were exposed to a systemic pan-VEGF receptor inhibitor (PTK787/ZK222584, 50mg/kg/d) or placebo (gavage) for the last 10 weeks. Atherosclerotic lesions were characterized in thoraco-abdominal aortae and aortic arches. Mechanistic analyses were performed in cultured human aortic endothelial cells.

Results: Systemic VEGF inhibition increased atherosclerotic lesions by 33% whereas features of plaque vulnerability (i.e. necrotic core size, fibrous cap thickness) remained unchanged compared with controls. Aortic eNOS expression was decreased (trend). In human endothelial cells VEGF inhibition induced a dose-dependent increase in mitochondrial superoxide generation with an uncoupling of eNOS, resulting in reduced NO availability and decreased proliferation.

Conclusion: Systemic VEGF inhibition disrupts endothelial homeostasis and accelerates atherogenesis, suggesting that these events contribute to the clinical cardiovascular adverse events of VEGF-inhibiting therapies. Cardiovascular safety profiles of currently applied anti-angiogenic regimens should be determined to improve patient selection for therapy and allow close monitoring of patients at increased cardiovascular risk.

Keywords: Adverse effects; Angiogenesis inhibitors; Cardiovascular diseases; Patient safety.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Angiogenesis Inhibitors / adverse effects*
Animals
Atherosclerosis / chemically induced*
Endothelium, Vascular / drug effects*
Endothelium, Vascular / physiopathology*
Homeostasis*
Male
Mice
Mice, Inbred C57BL
Phthalazines / adverse effects*
Pyridines / adverse effects*
Vascular Endothelial Growth Factor A / antagonists & inhibitors*

Substances

Angiogenesis Inhibitors
Phthalazines
Pyridines
VEGFA protein, human
Vascular Endothelial Growth Factor A
vatalanib