RhoA/ROCK signaling is essential for multiple aspects of VEGF‐mediated angiogenesis

Bryan, Brad Allen; Dennstedt, Emily A; Mitchell, Donald E.; Walshe, Tony E.; Noma, Kazuhiro; Loureiro, Robyn; Saint‐Geniez, Magali; Campaigniac, Jean-Paul; Liao, James K.; D'Amore, Patricia A.

doi:10.1096/fj.09-145102

Cited by 234 publications

(243 citation statements)

References 64 publications

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“…We have previously demonstrated that ablation of ROCK1 & 2 kinase activity with the non-selective ROCK1 & 2 pharmacological inhibitor Y27632 resulted in disrupted angiogenesis [7]. To determine the contribution of the individual ROCK paralogs to capillary network formation, the endothelial cell panel stably overexpressing non-targeting, ROCK1, or ROCK2 shRNA plasmids was subjected to matrigel network formation assays.…”

Section: Resultsmentioning

confidence: 99%

“…MS1 mouse pancreatic endothelial cells (ATCC# CRL-2279), SVR mouse engineered angiosarcoma cells (ATCC# CRL-2280), and B16F1 mouse melanoma cells (ATCC# CRL-6323) were maintained in Dulbecco’s modified Eagle’s media (DMEM) supplemented with 10% fetal bovine serum (FBS), 80 U/ml penicillin, and 50 µg/ml streptomycin C. Cells were treated as indicated with the following concentrations: human recombinant VEGF 165 (VEGF) (2.5 ng/ml) or Y27632 (10 mM) as previously described [7]. shRNA vectors (SABiosciences) (Table 1 ) were transfected using Lipofectamine 2000, and cell pools were stably selected with hygromycin ( MS1 cells ) or puromycin ( SVR cells ).…”

Section: Methodsmentioning

confidence: 99%

“…ROCK1(-/-) mice result in lethality soon after birth, displaying failure of eyelid and ventral body wall closure [3], while ROCK2(-/-) mice experience embryonic lethality due to interuterine growth retardation and placental dysfunction [4]. Viable fertile litters have been reported for ROCK1(+/-) and ROCK2(+/-) mice, however ROCK1(+/-) mice exhibit increased resistance to perivascular fibrosis and reduced vascular injury-induced neointima formation [5, 6], while ROCK2(+/-) mice display decreased platelet endothelial cell adhesion molecule staining of endothelial cells in the lung [7]. Only a handful of recent reports have utilized RNAi technology to singularly disrupt each ROCK paralog in vitro , demonstrating unique roles for each protein in the control of actin-cytoskeleton dynamics and cell morphogenesis, migration, cell fate decisions, and extracellular matrix assembly [7-13].…”

Section: Introductionmentioning

confidence: 99%

“…Viable fertile litters have been reported for ROCK1(+/-) and ROCK2(+/-) mice, however ROCK1(+/-) mice exhibit increased resistance to perivascular fibrosis and reduced vascular injury-induced neointima formation [5, 6], while ROCK2(+/-) mice display decreased platelet endothelial cell adhesion molecule staining of endothelial cells in the lung [7]. Only a handful of recent reports have utilized RNAi technology to singularly disrupt each ROCK paralog in vitro , demonstrating unique roles for each protein in the control of actin-cytoskeleton dynamics and cell morphogenesis, migration, cell fate decisions, and extracellular matrix assembly [7-13]. These data collectively suggest that ROCK1 and 2 paralogs perform, at least to some degree, unique biological roles in cell function.…”

Section: Introductionmentioning

confidence: 99%

“…Using in vivo and in vitro angiogenic assays, several labs have reported that disruption of RhoA/ROCK signaling inhibits vascular endothelial growth factor (VEGF)-mediated endothelial cell activation [7, 14-19]. Moreover, tumor derived endothelial cells display an enhanced ability to organize into capillary networks, correlating with a constitutively high level of RhoA/ROCK signaling [20].…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Rock1 & 2 Perform Overlapping and Unique Roles in Angiogenesis and Angiosarcoma Tumor Progression

Montalvo¹,

Spencer²,

Hackathorn³

et al. 2012

CMM

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The serine/threonine protein kinase paralogs ROCK1 & 2 have been implicated as essential modulators of angiogenesis; however their paralog-specific roles in endothelial function are unknown. shRNA knockdown of ROCK1 or 2 in endothelial cells resulted in a significant disruption of in vitro capillary network formation, cell polarization, and cell migration compared to cells harboring non-targeting control shRNA plasmids. Knockdowns led to alterations in cytoskeletal dynamics due to ROCK1 & 2-mediated reductions in actin isoform expression, and ROCK2-specific reduction in myosin phosphatase and cofilin phosphorylation. Knockdowns enhanced cell survival and led to ROCK1 & 2-mediated reduction in caspase 6 and 9 cleavage, and a ROCK2-specific reduction in caspase 3 cleavage. Microarray analysis of ROCK knockdown lines revealed overlapping and unique control of global transcription by the paralogs, and a reduction in the transcriptional regulation of just under 50% of VEGF responsive genes. Finally, paralog knockdown in xenograft angiosarcoma tumors resulted in a significant reduction in tumor formation. Our data reveals that ROCK1 & 2 exhibit overlapping and unique roles in normal and dysfunctional endothelial cells, that alterations in cytoskeletal dynamics are capable of overriding mitogen activated transcription, and that therapeutic targeting of ROCK signaling may have profound impacts for targeting angiogenesis.

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Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Rock1 & 2 Perform Overlapping and Unique Roles in Angiogenesis and Angiosarcoma Tumor Progression

Montalvo¹,

Spencer²,

Hackathorn³

et al. 2012

CMM

View full text Add to dashboard Cite

show abstract

The relationship between mesenchymal stromal cells and endothelial cells

Nassiri

Rahbarghazi‬

2016

The Biology and Therapeutic Application of Mesenchymal Cells

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Intercellular Tension Negatively Regulates Angiogenic Sprouting of Endothelial Tip Cells via Notch1‐Dll4 Signaling

et al. 2017

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Mechanical force plays pivotal roles in vascular development during tissue growth and regeneration. Nevertheless, the process by which mechanical force controls the vascular architecture remains poorly understood. Using a systems bioengineering approach, it is shown that intercellular tension negatively regulates tip cell formation via Notch1‐Dll4 signaling in mouse retinal angiogenesis in vivo, sprouting embryoid bodies, and human endothelial cell networks in vitro. Reducing the intercellular tension pharmacologically by a Rho‐associated protein kinase inhibitor or physically by single cell photothermal ablation of the capillary networks promotes the expression of Dll4, enhances angiogenic sprouting of tip cells, and increases the vascular density. Computational biomechanics, RNA interference, and single cell gene expression analysis reveal that a reduction of intercellular tension attenuates the inhibitory effect of Notch signaling on tip cell formation and induces angiogenic sprouting. Taken together, the results reveal a mechanoregulation scheme for the control of vascular architecture by modulating angiogenic tip cell formation via Notch1‐Dll4 signaling.

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RhoA/ROCK signaling is essential for multiple aspects of VEGF‐mediated angiogenesis

Cited by 234 publications

References 64 publications

Rock1 & 2 Perform Overlapping and Unique Roles in Angiogenesis and Angiosarcoma Tumor Progression

Rock1 & 2 Perform Overlapping and Unique Roles in Angiogenesis and Angiosarcoma Tumor Progression

The relationship between mesenchymal stromal cells and endothelial cells

Intercellular Tension Negatively Regulates Angiogenic Sprouting of Endothelial Tip Cells via Notch1‐Dll4 Signaling

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