Vascular endothelial growth factor-A inhibits EphB4 and stimulates delta-like ligand 4 expression in adult endothelial cells

Yang, Chenzi; Guo, Yuanyuan; Jadlowiec, Caroline C.; Li, Xin; Lv, Wei; Model, Lynn; Collins, Michael J.; Kondo, Yuka; Muto, Akihito; Shu, Chang; Dardik, Alan

doi:10.1016/j.jss.2013.01.009

Cited by 25 publications

(17 citation statements)

References 43 publications

(60 reference statements)

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“…Thus, the early phase increase in VEGF-A inhibits the expression of Eph-B4 and upregulates the expression of Dll4 (a Notch ligand), but without stimulating its downstream signaling events such as Notch activation or ephrin-B2 expression in these adult ECs. These results are consistent with the effects of blocking the VEGF/COUP-TFII-Notch signaling-Eph-B4/ephrin-B2 pathway in adult ECs [55]. Therefore, vein grafts lose their venous identity markers without acquiring arterial identity.…”

Section: Vein Graftssupporting

confidence: 86%

Pathophysiologic Role of Molecules Determining Arteriovenous Differentiation in Adult Life

et al. 2020

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The structural differences between arteries and veins are genetically predetermined. Vascular identity markers, the molecular markers specific to veins and arteries, determine the differential development of vessels during embryogenesis and their expression persists in adult vessels. It is revealed that they can be reactivated under various pathophysiologic conditions even after vessel differentiation. Thus, once considered as quiescent in adults, vascular identity markers may actually play significant roles in vascular remodeling. Manipulation of vascular identity and the underlying molecular mechanisms might be a novel strategy to improve vascular remodeling for clinical application.

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Section: Vein Graftssupporting

confidence: 86%

Pathophysiologic Role of Molecules Determining Arteriovenous Differentiation in Adult Life

et al. 2020

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“…We previously showed that MLEC express both Eph-B4 and Ephrin-B2, consistent with a venous phenotype. 16 As expected, stimulation of endothelial cells with Ephrin-B2/Fc stimulated Eph-B4 phosphorylation, in a bimodal temporal distribution, with an early peak at approximately 1 minute and a later peak at approximately 30-60 minutes ( Figure 1A). In addition to Ephrin-B2/Fc stimulating Eph-B4 phosphorylation, Ephrin-B2/Fc also stimulated eNOS phosphorylation, in a similar bimodal pattern ( Figure 1B), that was inhibited in cells pretreated with the Eph-B4 inhibitor NVP-BHG712 ( Figure 1C).…”

Section: Resultssupporting

confidence: 78%

Eph-B4 Mediates Vein Graft Adaptation By Regulation of eNOS

Wang

Collins

Bai

et al. 2015

Journal of Vascular Surgery

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Objectives-Vein graft adaptation is characterized by loss of expression of the tyrosine kinase receptor Eph-B4, the embryonic determinant of venous identity, without increased expression of its ligand Ephrin-B2, the embryonic determinant of arterial identity. eNOS is an important mediator of vessel remodeling. We hypothesized that the mechanism of action of Eph-B4 during vein graft adaptation might be via regulation of downstream eNOS activity. Methods-Mouse lung endothelial cells (MLEC)were stimulated with Ephrin-B2/Fc, without and with preclustering, without and with the eNOS inhibitor L-NAME or the Eph-B4 inhibitor NVP-BHG712, and assessed by Western blot and immunofluorescence for eNOS and Eph-B4 phosphorylation. Nitric oxide (NO) production was assessed using a NO-specific chemiluminescence analyzer. Cell migration was assessed using a transwell assay. Human and mouse vein graft specimens were examined for eNOS activity by Western blot, and vessel remodeling was assessed in vein grafts in wild-type (WT) or eNOS-knockout (KO) mice.Results-Ephrin-B2/Fc stimulated both Eph-B4 and eNOS phosphorylation in a bimodal temporal distribution (n=4; p<.05), with preclustered Ephrin-B2/Fc causing prolonged peak Eph-B4 and eNOS phosphorylation as well as altered subcellular localization (n=4; p<.05). Ephrin-B2/Fc increased NO release (n=3; p<.01) as well as increased endothelial cell migration (n=6; p<. 05) in an eNOS-dependent fashion. Both human and mouse vein grafts showed increased eNOS phosphorylation compared with normal veins (n=3; p<.05). Vein grafts from eNOS-KO mice showed less dilation and less wall thickening compared with WT vein grafts (n=7; p<.05).

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“…44 Another study showed that VEGF upregulates Delta-like 4 (DLL4) and presenilin expression, and increases activation of Notch4, leading to upregulation of ephrinB2 and downregulation of EphB4 in venous ECs. 45 In contrast, Yang et al 46 found that VEGF-A inhibits expression of EphB4 and stimulates expression of DLL4, but does not stimulate either Notch or ephrinB2 expression in adult venous ECs. Pretreatment with a VEGFR-2 neutralizing antibody abolishes VEGF-stimulated downregulation of EphB4, but not the upregulation of DLL4.…”

Section: Figmentioning

confidence: 92%

Coculture of Stem Cells from Apical Papilla and Human Umbilical Vein Endothelial Cell Under Hypoxia Increases the Formation of Three-Dimensional Vessel-Like Structuresin Vitro

Yuan

Wang²,

Zhu

et al. 2015

Tissue Engineering Part A

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Vascular endothelial growth factor-A inhibits EphB4 and stimulates delta-like ligand 4 expression in adult endothelial cells

Cited by 25 publications

References 43 publications

Pathophysiologic Role of Molecules Determining Arteriovenous Differentiation in Adult Life

Pathophysiologic Role of Molecules Determining Arteriovenous Differentiation in Adult Life

Eph-B4 Mediates Vein Graft Adaptation By Regulation of eNOS

Coculture of Stem Cells from Apical Papilla and Human Umbilical Vein Endothelial Cell Under Hypoxia Increases the Formation of Three-Dimensional Vessel-Like Structuresin Vitro

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