Vascular Permeability and Pathological Angiogenesis in Caveolin-1-Null Mice

Chang, Sung-Hee; Feng, Dian; Nagy, Janice A.; Sciuto, Tracey E.; Dvorak, Ann M.; Dvorak, Harold F.

doi:10.2353/ajpath.2009.090171

Cited by 87 publications

(73 citation statements)

References 59 publications

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“…By in vitro, ex vivo, and in vivo experiments, our results further confirm previous studies showing that the individual loss of eNOS 36 or caveolin-1 20,22 impairs the angiogenic response elicited by B16 melanoma cells inoculated in vivo. In addition, we show for the first time that reduced tumor angiogenesis in caveolin-1-null mice is due to unabated endothelial nitric oxide production, as genetic disruption of eNOS in the caveolin-1-null background partially or totally restores angiogenesis quantitatively.…”

Section: Discussionsupporting

confidence: 80%

“…21 Defective mobilization of endothelial progenitors in response to ischemia was further documented in caveolin-1-deficient mice. 38 However, using tumor angiogenesis assays, both an increase 18,19 and a decrease 20,22 in the number of angiogenic blood vessels have been reported. Studies reporting increased tumor angiogenesis also documented increased tumor growth in caveolin-1-null mice, 18,19 whereas studies reporting decreased angiogenesis showed decreased tumor growth.…”

Section: Discussionmentioning

confidence: 99%

“…Studies reporting increased tumor angiogenesis also documented increased tumor growth in caveolin-1-null mice, 18,19 whereas studies reporting decreased angiogenesis showed decreased tumor growth. 20,22 The method for numbering the tumor blood vessels has been suggested to explain the difference between these studies. 18 In our experiments, CD31 and ␣-smooth muscle cell actin staining of tumor sections confirmed the decreased number in vessels seen with the H&E staining in the caveolin-1 gene-deficient mice (not shown).…”

Section: Discussionmentioning

confidence: 99%

“…Decreased pathological neovascularization in caveolin-1-null mice has not been unanimously reported. Decreased angiogenesis was shown using bFGF-containing matrigel plugs, 20 VEGF-expressing adenoviral vector, 22 experimental colitis 23 or cerebral ischemia. 37 Reduced ischemic hindlimb reperfusion after femoral artery resection is also apparent in these mice.…”

Section: Discussionmentioning

confidence: 99%

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Altered Angiogenesis in Caveolin-1 Gene–Deficient Mice Is Restored by Ablation of Endothelial Nitric Oxide Synthase

Morais

Ebrahem

Anand‐Apte

et al. 2012

The American Journal of Pathology

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Caveolin-1 is an essential structural protein of caveolae, specialized plasma membrane organelles highly abundant in endothelial cells, where they regulate multiple functions including angiogenesis. Caveolin-1 exerts a tonic inhibition of endothelial nitric oxide synthase (eNOS) activity. Accordingly, caveolin-1 gene-disrupted mice have enhanced eNOS activity as well as increased systemic nitric oxide (NO) levels. We hypothesized that excess eNOS activity, secondary to caveolin deficiency, would mediate the decreased angiogenesis observed in caveolin-1 gene-disrupted mice. We tested tumor angiogenesis in mice lacking either one or both proteins, using in vitro, ex vivo, and in vivo assays. We show that endothelial cell migration, tube formation, cell sprouting from aortic rings, tumor growth, and angiogenesis are all significantly impaired in both caveolin-1-null and eNOSnull mice. We further show that these parameters were either partially or fully restored in double knockout mice that lack both caveolin-1 and eNOS. Furthermore, the effects of genetic ablation of eNOS are mimicked by the administration of the NOS inhibitor N-nitro-L-arginine methyl ester hydrochloride (L-NAME), including the reversal of the caveolin-1-null mouse angiogenic phenotype. This study is the first to demonstrate the detrimental effects of unregulated eNOS activity on angiogenesis, and shows that impaired tumor angiogenesis in caveolin-1-null mice is, at least in part, the result of enhanced eNOS activity.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Altered Angiogenesis in Caveolin-1 Gene–Deficient Mice Is Restored by Ablation of Endothelial Nitric Oxide Synthase

Morais

Ebrahem

Anand‐Apte

et al. 2012

The American Journal of Pathology

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“…The established Cav-1 knockout mouse line has confirmed the importance of Cav-1 for the formation of morphologically distinct caveolae [9,10] . In addition, Cav-1 is also involved in the maintenance of cellular cholesterol homeostasis and lipid transport.…”

Section: Introductionmentioning

confidence: 88%

Ezetimibe suppresses cholesterol accumulation in lipid-loaded vascular smooth muscle cells in vitro via MAPK signaling

Qin

Yang

et al. 2014

Acta Pharmacol Sin

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Aim: To investigate the mechanisms of anti-atherosclerotic action of ezetimibe in rat vascular smooth muscle cells (VSMCs) in vitro. Methods: VSMCs of SD rats were cultured in the presence of Chol:MβCD (10 μg/mL) for 72 h, and intracellular lipid droplets and cholesterol levels were evaluated using Oil Red O staining, HPLC and Enzymatic Fluorescence Assay, respectively. The expression of caveolin-1, sterol response element-binding protein-1 (SREBP-1) and ERK1/2 were analyzed using Western blot assays. Translocation of SREBP-1 and ERK1/2 was detected with immunofluorescence. Results: Treatment with Chol:MβCD dramatically increased the cellular levels of total cholesterol (TC), cholesterol ester (CE) and free cholesterol (FC) in VSMCs, which led to the formation of foam cells. Furthermore, Chol:MβCD treatment significantly decreased the expression of caveolin-1, and stimulated the expression and nuclear translocation of SREBP-1 in VSMCs. Co-treatment with ezetimibe (3 μmol/L) significantly decreased the cellular levels of TC, CE and FC, which was accompanied by elevation of caveolin-1 expression, and by a reduction of SREBP-1 expression and nuclear translocation. Co-treatment with ezetimibe dose-dependently decreased the expression of phosphor-ERK1/2 (p-ERK1/2) in VSMCs. The ERK1/2 inhibitor PD98059 (50 μmol/L) altered the cholesterol level and the expression of p-ERK1/2, SREBP-1 and caveolin-1 in the same manner as ezetimibe did. Conclusion: Ezetimibe suppresses cholesterol accumulation in rat VSMCs in vitro by regulating SREBP-1 and caveolin-1 expression, possibly via the MAPK signaling pathway.

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Caveolae

Tse¹,

Stan²

2011

Cellular Domains

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Vascular Permeability and Pathological Angiogenesis in Caveolin-1-Null Mice

Cited by 87 publications

References 59 publications

Altered Angiogenesis in Caveolin-1 Gene–Deficient Mice Is Restored by Ablation of Endothelial Nitric Oxide Synthase

Altered Angiogenesis in Caveolin-1 Gene–Deficient Mice Is Restored by Ablation of Endothelial Nitric Oxide Synthase

Ezetimibe suppresses cholesterol accumulation in lipid-loaded vascular smooth muscle cells in vitro via MAPK signaling

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