Angiopoietin 1 causes vessel enlargement, without angiogenic sprouting,during a critical developmental period

Thurston, Gavin; Wang, Quan; Baffert, Fabienne; Rudge, John S.; Papadopoulos, Nicholas; Jean-Guillaume, Danielle; Wiegand, Stanley J.; Yancopouloš, George D.; McDonald, Donald M.

doi:10.1242/dev.01888

Cited by 100 publications

(106 citation statements)

References 48 publications

(65 reference statements)

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“…In ES cell tumors, VE-PTP KO blood vessels were enlarged, extending the findings in yolk sacs of VE-PTP-deficient embryos (9,10), and strongly supporting the findings in explant models (31). Such a phenotype also resembles the effect of tissue-specific transgenic overexpression of the Tie2 ligand, Ang1 (21,32) or prolonged treatment with exogenous Ang1 (20,22). Importantly, the enlarged vessels in ES tumors could be returned to normal size by treatment with angiopoietin inhibitors.…”

Section: Discussionsupporting

confidence: 76%

“…The vessel enlargement seen in VE-PTP-null vessels resembled previous findings that activation of the angiopoietin-Tie2 pathway also results in an increase in vessel diameter (20)(21)(22)(23), although the effects of this pathway on vessel size have not yet been explored in tumor angiogenesis. To explore the role of the angiopoietin-Tie2 pathway, and possible regulation by VE-PTP, during tumor angiogenesis, we first asked whether manipulating the angiopoietin-Tie2 pathway could regulate blood vessel diameter in ES tumors.…”

Section: Treatment With Exogenous Tie2 Activators Can Also Increase Tsupporting

confidence: 80%

“…To explore the role of the angiopoietin-Tie2 pathway, and possible regulation by VE-PTP, during tumor angiogenesis, we first asked whether manipulating the angiopoietin-Tie2 pathway could regulate blood vessel diameter in ES tumors. Therefore, teratomabearing mice were treated systemically with recombinant angiopoietin-1 protein (24), a reagent shown to activate Tie2 receptor tyrosine kinase in vivo through ligand-receptor interaction and to increase blood vessel diameter in certain settings (22).…”

Section: Treatment With Exogenous Tie2 Activators Can Also Increase Tmentioning

confidence: 99%

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Embryonic stem cell tumor model reveals role of vascular endothelial receptor tyrosine phosphatase in regulating Tie2 pathway in tumor angiogenesis

Huang

Boland

et al. 2009

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

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Inhibiting angiogenesis has become an effective approach for treating cancer and other diseases. However, our understanding of signaling pathways in tumor angiogenesis has been limited by the embryonic lethality of many gene knockouts. To overcome this limitation, we used the plasticity of embryonic stem (ES) cells to develop a unique approach to study tumor angiogenesis. Murine ES cells can be readily manipulated genetically; in addition, ES cells implanted subcutaneously in mice develop into tumors that contain a variety of cell types (teratomas). We show that ES cells differentiate into bona fide endothelial cells within the teratoma, and that these ES-derived endothelial cells form part of the functional tumor vasculature. Using this powerful and flexible system, the Angiopoietin/Tie2 system is shown to have a key role in the regulation of tumor vessel size. Endothelial differentiation in the ES teratoma model allows gene-targeting methods to be used in the study of tumor angiogenesis.teratoma ͉ endothelial cells ͉ VEGF-R2 ͉ VE-PTP

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Section: Discussionsupporting

confidence: 76%

Section: Treatment With Exogenous Tie2 Activators Can Also Increase Tsupporting

confidence: 80%

Section: Treatment With Exogenous Tie2 Activators Can Also Increase Tmentioning

confidence: 99%

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Embryonic stem cell tumor model reveals role of vascular endothelial receptor tyrosine phosphatase in regulating Tie2 pathway in tumor angiogenesis

Huang

Boland

et al. 2009

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

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“…26 Our results in vivo support FTY720-induced increases in cell migration and proliferation, as evidenced by increased length density, diameter, and branching on venules, a metric indicative of sprouting angiogenesis. 3,27 In contrast, other studies have reported that FTY720 actually inhibits vascular endothelial growth factor-induced vascular permeability and angiogenesis. [28][29][30] The antiangiogenic effects of FTY720, though surprising based on its potent agonist activity, are proposed to occur as a result of functional antagonism.…”

mentioning

confidence: 87%

Selective Activation of Sphingosine 1-Phosphate Receptors 1 and 3 Promotes Local Microvascular Network Growth

Sefcik

Aronin

Awojoodu

et al. 2011

Tissue Engineering Part A

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Proper spatial and temporal regulation of microvascular remodeling is critical to the formation of functional vascular networks, spanning the various arterial, venous, capillary, and collateral vessel systems. Recently, our group has demonstrated that sustained release of sphingosine 1-phosphate (S1P) from biodegradable polymers promotes microvascular network growth and arteriolar expansion. In this study, we employed S1P receptorspecific compounds to activate and antagonize different combinations of S1P receptors to elucidate those receptors most critical for promotion of pharmacologically induced microvascular network growth. We show that S1P 1 and S1P 3 receptors act synergistically to enhance functional network formation via increased functional length density, arteriolar diameter expansion, and increased vascular branching in the dorsal skinfold window chamber model. FTY720, a potent activator of S1P 1 and S1P 3 , promoted a 107% and 153% increase in length density 3 and 7 days after implantation, respectively. It also increased arteriolar diameters by 60% and 85% 3 and 7 days after implantation. FTY720-stimulated branching in venules significantly more than unloaded poly(D, L-lactic-co-glycolic acid). When implanted on the mouse spinotrapezius muscle, FTY720 stimulated an arteriogenic response characterized by increased tortuosity and collateralization of branching microvascular networks. Our results demonstrate the effectiveness of S1P 1 and S1P 3 receptor-selective agonists (such as FTY720) in promoting microvascular growth for tissue engineering applications.

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“…However, studies on the ability of Ang1 to stimulate proliferation of cultured endothelial cells are controversial, ranging from no effect Witzenbichler et al, 1998;Fujikawa et al, 1999) to mild effects (Koblizek et al, 1998;Teichert-Kuliszewska et al, 2001) to substantial effects (Kanda et al, 2005). The in vivo studies with Ang1 and COMP-Ang1 in newborns (Cho et al, 2005;Thurston et al, 2005;Kim et al, 2007) suggest that vessel enlargement was accompanied by endothelial cell proliferation, establishing that Tie-2 can stimulate proliferation of endothelial cells in vivo.…”

Section: Reagents and Antibodiesmentioning

confidence: 99%

VE-PTP controls blood vessel development by balancing Tie-2 activity

Winderlich¹,

Keller²,

Cagna³

et al. 2009

J Exp Med

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Angiopoietin 1 causes vessel enlargement, without angiogenic sprouting,during a critical developmental period

Cited by 100 publications

References 48 publications

Embryonic stem cell tumor model reveals role of vascular endothelial receptor tyrosine phosphatase in regulating Tie2 pathway in tumor angiogenesis

Embryonic stem cell tumor model reveals role of vascular endothelial receptor tyrosine phosphatase in regulating Tie2 pathway in tumor angiogenesis

Selective Activation of Sphingosine 1-Phosphate Receptors 1 and 3 Promotes Local Microvascular Network Growth

VE-PTP controls blood vessel development by balancing Tie-2 activity

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