Endothelial Expression of β1 Integrin Is Required for Embryonic Vascular Patterning and Postnatal Vascular Remodeling

Li, Lei; Liu, Dinggang; Huang, Yan; Jovin, Ion S.; Shai, Shaw‐Yung; Kyriakides, Themis R.; Ross, Robert S.; Giordano, Frank J.

doi:10.1128/mcb.00443-07

Cited by 87 publications

(86 citation statements)

References 39 publications

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“…Also of interest is that inhibition of ␣5␤1 integrin ligation increases PKA activation and may be an important mechanism whereby agents that alter intregrin function can inhibit angiogenesis (27). Recently we showed that endothelial cell-specific loss of the ␤1 integrin causes embryonic lethality and profound abnormalities in vascular development (28). It is interesting to consider that a PKA-mediated final common pathway may be involved in the vascular effects of Ucn2 and of altered integrin function.…”

Section: Discussionmentioning

confidence: 99%

Urocortin2 inhibits tumor growth via effects on vascularization and cell proliferation

Hao

Huang

Cleman

et al. 2008

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

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The corticotropin-releasing factor (CRF) receptor CRFR2 is expressed widely in peripheral tissues and in the vasculature, although its functional roles in those tissues have only recently begun to be elucidated. Previously we found that genetic deletion of CRFR2 resulted in profound postnatal hypervascularization in mice, characterized by both an increase in total vessel number and a dramatic increase in vessel diameter. These data strongly suggested that ligands for CRFR2 act to limit tissue vascularity, perhaps as a counterbalance to factors that promote neovascularization. Urocortin 2 (Ucn2) is a specific ligand for the CRFR2. We hypothesized that activation of CRFR2 by Ucn2 might thus suppress tumor vascularization and consequently limit tumor growth. Here, we show that viral-mediated expression of Ucn2 strikingly inhibits the growth and vascularization of Lewis Lung Carcinoma Cell (LLCC) tumors in vivo. Further, we found that this effect on tumor growth inhibition was independent of whether exposure to Ucn2 occurred before or after establishment of measurable tumors. In vitro, Ucn2 directly inhibited the proliferation of LLCC, suggesting that the tumor-suppressing effects of CRFR2 activation involve a dual mechanism of both a direct inhibition of tumor cell cycling and the suppression of tumor vascularization. These results establish that Ucn2 inhibits tumor growth, suggesting a potential therapeutic role for CRFR2 ligands in clinical malignancies.anti-angiogenic ͉ cancer ͉ CRF ͉ peptide ͉ CRFR2

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Section: Discussionmentioning

confidence: 99%

Urocortin2 inhibits tumor growth via effects on vascularization and cell proliferation

Hao

Huang

Cleman

et al. 2008

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

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“…Illustrations were prepared by O. Karengina based on an image of a mouse embryo at E13.5. (Furuta, 1995;Ilic et al, 2003) Vinculin Focal adhesions Total Death by E10, with embryos displaying 30-40% reduction in size, lack of midline fusion of the rostral neural tube and developmental defects in heart, somites and limbs (Xu et al, 1998) Zyxin Focal adhesions Total Viable, fertile, no obvious abnormalities (Hoffman et al, 2003) α4 integrin Integrins Total Embryonic lethality, defects in placenta and vascular system, cardiac hemmorhages (Yang et al, 1995) αv integrin Integrins Total Partial embryonic lethality, intracerebral and intestinal hemorrhages and cleft palates (Bader et al, 1998) α5 integrin Integrins Total Embryonic lethal and E10-11 with migration-type defects in posterior trunk and yolk sac mesodermal structures (Yang et al, 1993) Lei et al, 2008;Tanjore, 2008) Total Death shortly after implantation (Fassler and Meyer, 1995) In vitro studies of cells from knockout mice…”

Section: Note On Nomenclaturementioning

confidence: 99%

Cell biology of embryonic migration

Kurosaka¹,

Kashina²

2008

Birth Defects Research Pt C

111

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Cell migration is an evolutionarily conserved mechanism that underlies the development and functioning of uni-and multicellular organisms and takes place in normal and pathogenic processes, including various events of embryogenesis, wound healing, immune response, cancer metastases, and angiogenesis. Despite the differences in the cell types that take part in different migratory events, it is believed that all of these migrations occur by similar molecular mechanisms, whose major components have been functionally conserved in evolution and whose perturbation leads to severe developmental defects. These mechanisms involve intricate cytoskeleton-based molecular machines that can sense the environment, respond to signals, and modulate the entire cell behavior. A big question that has concerned the researchers for decades relates to the coordination of cell migration in situ and its relation to the intracellular aspects of the cell migratory mechanisms. Traditionally, this question has been addressed by researchers that considered the intra-and extracellular mechanisms driving migration in separate sets of studies. As more data accumulate researchers are now able to integrate all of the available information and consider the intracellular mechanisms of cell migration in the context of the developing organisms that contain additional levels of complexity provided by extracellular regulation. This review provides a broad summary of the existing and emerging data in the cell and developmental biology fields regarding cell migration during development.

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“…45 This involves the polarity gene Par3 which is down regulated in b1-deficient endothelial cells and animals lacking endothelial b1 die at E9.5 and 10. 46 Recently, Barry and colleagues showed the importance of VE-cadherin and the small GTPase Cdc42 in opening the vascular lumen. 47 Hence, b1-integrins may be directly or indirecty linked to VEcadherin during vessel development.…”

Section: Introductionmentioning

confidence: 99%

Small Rho GTPase-mediated actin dynamics at endothelial adherens junctions

Buul

Timmerman

2016

Small GTPases

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VE-cadherin-based cell-cell junctions form the major restrictive barrier of the endothelium to plasma proteins and blood cells. The function of VE-cadherin and the actin cytoskeleton are intimately linked. Vascular permeability factors and adherent leukocytes signal through small Rho GTPases to tightly regulate actin cytoskeletal rearrangements in order to open and re-assemble endothelial cell-cell junctions in a rapid and controlled manner. The Rho GTPases are activated by guanine nucleotide exchange factors (GEFs), conferring specificity and context-dependent control of cell-cell junctions. Although the molecular mechanisms that couple cadherins to actin filaments are beginning to be elucidated, specific stimulus-dependent regulation of the actin cytoskeleton at VEcadherin-based junctions remains unexplained. Accumulating evidence has suggested that depending on the vascular permeability factor and on the subcellular localization of GEFs, cell-cell junction dynamics and organization are differentially regulated by one specific Rho GTPase. In this Commentary, we focus on new insights how the junctional actin cytoskeleton is specifically and locally regulated by Rho GTPases and GEFs in the endothelium.

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Endothelial Expression of β1 Integrin Is Required for Embryonic Vascular Patterning and Postnatal Vascular Remodeling

Cited by 87 publications

References 39 publications

Urocortin2 inhibits tumor growth via effects on vascularization and cell proliferation

Urocortin2 inhibits tumor growth via effects on vascularization and cell proliferation

Cell biology of embryonic migration

Small Rho GTPase-mediated actin dynamics at endothelial adherens junctions

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