Time Course of Endothelial Cell Proliferation and Microvascular Remodeling in Chronic Inflammation

Ezaki, Taichi; Bałuk, Peter; Thurston, Gavin; Barbara, Allyson La; Woo, Carolyn; McDonald, Donald M.

doi:10.1016/s0002-9440(10)64676-7

Cited by 118 publications

(125 citation statements)

References 40 publications

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“…To confirm that the dextran injection method could precisely mark blood vessels in tumors, we did a coinjection experiment with the Texas red-conjugated dextran and FITC-conjugated LEL, which specifically binds to endothelial cells (19). Using confocal microscopy, we observed that the majority of dextran-marked channels in the tumors were colocalized with FITC-LEL staining ( Fig.…”

Section: Resultsmentioning

confidence: 82%

Macrophages Regulate the Angiogenic Switch in a Mouse Model of Breast Cancer

Lin¹,

Li²,

Gnatovskiy³

et al. 2006

Cancer Research

928

782

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The development of a tumor vasculature or access to the host vasculature is a crucial step for the survival and metastasis of malignant tumors. Although therapeutic strategies attempting to inhibit this step during tumor development are being developed, the biological regulation of this process is still largely unknown. Using a transgenic mouse susceptible to mammary cancer, PyMT mice, we have characterized the development of the vasculature in mammary tumors during their progression to malignancy. We show that the onset of the angiogenic switch, identified as the formation of a highdensity vessel network, is closely associated with the transition to malignancy. More importantly, both the angiogenic switch and the progression to malignancy are regulated by infiltrated macrophages in the primary mammary tumors. Inhibition of the macrophage infiltration into the tumor delayed the angiogenic switch and malignant transition whereas genetic restoration of the macrophage population specifically in these tumors rescued the vessel phenotype. Furthermore, premature induction of macrophage infiltration into premalignant lesions promoted an early onset of the angiogenic switch independent of tumor progression. Taken together, this study shows that tumor-associated macrophages play a key role in promoting tumor angiogenesis, an essential step in the tumor progression to malignancy. (Cancer Res 2006; 66(23): 11238-46)

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Section: Resultsmentioning

confidence: 82%

Macrophages Regulate the Angiogenic Switch in a Mouse Model of Breast Cancer

Lin¹,

Li²,

Gnatovskiy³

et al. 2006

Cancer Research

928

782

View full text Add to dashboard Cite

show abstract

“…Lectin staining was performed as described in ref. 20. Immunostaining was performed with anti-CD31 (MEC13.3, Pharmingen) and anti-SMC-␣-actin (anti-␣-SMA) (1A4-AP, Sigma).…”

Section: Methodsmentioning

confidence: 99%

Endothelial expression of constitutively active Notch4 elicits reversible arteriovenous malformations in adult mice

Carlson

Yan

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

177

213

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Direct communication between arteries and veins without intervening capillary beds is the primary pathology of arteriovenous malformations (AVMs). Although Notch signaling is implicated in embryonic arteriovenous (AV) differentiation, its function in the adult mammalian vasculature has not been established due to the embryonic lethality that often occurs in both gain- and loss-of-function mutants. We expressed a constitutively active Notch4, int3, in the adult mouse endothelium by using the tetracycline-repressible system to suppress int3 during embryogenesis. int3 caused profound blood vessel enlargement and AV shunting, which are hallmarks of AVM, and led to lethality within weeks of its expression. Vessel enlargement, a manifestation of AVM, occurred in an apparently tissue-specific fashion; the liver, uterus, and skin were affected. int3-mediated vascular defects were accompanied by arterialization, including ectopic venous expression of ephrinB2, increased smooth muscle cells, and up-regulation of endogenous Notch signaling. Remarkably, the defective vessels and illness were reversed upon repression of int3 expression. Finally, endothelial expression of a constitutively active Notch1 induced similar hepatic vascular lesions. Our results provide gain-of-function evidence that Notch signaling in the adult endothelium is sufficient to render arterial characteristics and lead to AVMs

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“…Briefly, frozen sections were digested with 0.005% pepsin (Sigma, St. Louis, Missouri) in 0.01 HCl for 30 min at 37 °C followed by treatment with 4 N HCl for 30 min at room temperature. Sections were then blocked by incubation in 5% goat serum in PBS for 30 min [43] prior to incubation with antibody. Fluorescence microscopic imaging of endothelial (CD31 + CD105 + flk1) [38,39], pericyte (NG2 or PDGF β-receptor) [13,18,19], and nuclear (BrdU) markers [43] was performed according to the published methods.…”

Section: Tissue Processing Immunohistochemistry and Imagingmentioning

confidence: 99%

Pathological angiogenesis is reduced by targeting pericytes via the NG2 proteoglycan

2004

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The NG2 proteoglycan is expressed by nascent pericytes during the early stages of angiogenesis. To investigate the functional role of NG2 in neovascularization, we have compared pathological retinal and corneal angiogenesis in wild type and NG2 null mice. During ischemic retinal neovascularization, ectopic vessels protruding into the vitreous occur twice as frequently in wild type retinas as in NG2 null retinas. In the NG2 knock-out retina, proliferation of both pericytes and endothelial cells is significantly reduced, and the pericyte:endothelial cell ratio falls to 0.24 from the wild type value of 0.86. Similarly, bFGF-induced angiogenesis is reduced more than four-fold in the NG2 null cornea compared to that seen in the wild type retina. Significantly, NG2 antibody is effective in reducing angiogenesis in the wild type cornea, suggesting that the proteoglycan can be an effective target for anti-angiogenic therapy. These experiments therefore demonstrate both the functional importance of NG2 in pericyte development and the feasibility of using pericytes as antiangiogenic targets. Keywords

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Time Course of Endothelial Cell Proliferation and Microvascular Remodeling in Chronic Inflammation

Cited by 118 publications

References 40 publications

Macrophages Regulate the Angiogenic Switch in a Mouse Model of Breast Cancer

Macrophages Regulate the Angiogenic Switch in a Mouse Model of Breast Cancer

Endothelial expression of constitutively active Notch4 elicits reversible arteriovenous malformations in adult mice

Pathological angiogenesis is reduced by targeting pericytes via the NG2 proteoglycan

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