YAP and the RhoC regulator ARHGAP18, are required to mediate flow-dependent endothelial cell alignment

Coleman, Paul R.; Lay, Angelina J.; Ting, Ka Ka; Zhao, Yang; Li, Jia; Jarrah, Sorour; Vadas, Mathew A.; Gamble, Jennifer R.

doi:10.1186/s12964-020-0511-7

Cited by 17 publications

(17 citation statements)

References 38 publications

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“…The hub gene of the black module was ARHGAP18. ARHGAP18 (SENEX) is a negative regulator of YAP and RhoC (Coleman et al, 2020). Overexpression of RhoC destroys the actin cytoskeleton and cell junctions.…”

Section: Discussionmentioning

confidence: 99%

Weighted Gene Co-expression Network Analysis Identifies Crucial Genes Mediating Progression of Carotid Plaque

Chen

Yang

et al. 2021

Front. Physiol.

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BackgroundSurface rupture of carotid plaque can cause severe cerebrovascular disease, including transient ischemic attack and stroke. The aim of this study was to elucidate the molecular mechanism governing carotid plaque progression and to provide candidate treatment targets for carotid atherosclerosis.MethodsThe microarray dataset GSE28829 and the RNA-seq dataset GSE104140, which contain advanced plaque and early plaque samples, were utilized in our analysis. Differentially expressed genes (DEGs) were screened using the “limma” R package. Gene modules for both early and advanced plaques were identified based on co-expression networks constructed by weighted gene co-expression network analysis (WGCNA). Gene Ontology (GO) and Kyoto Encyclopedia of Genes Genomes (KEGG) analyses were employed in each module. In addition, hub genes for each module were identified. Crucial genes were identified by molecular complex detection (MCODE) based on the DEG co-expression network and were validated by the GSE43292 dataset. Gene set enrichment analysis (GSEA) for crucial genes was performed. Sensitivity analysis was performed to evaluate the robustness of the networks that we constructed.ResultsA total of 436 DEGs were screened, of which 335 were up-regulated and 81 were down-regulated. The pathways related to inflammation and immune response were determined to be concentrated in the black module of the advanced plaques. The hub gene of the black module was ARHGAP18 (Rho GTPase activating protein 18). NCF2 (neutrophil cytosolic factor 2), IQGAP2 (IQ motif containing GTPase activating protein 2) and CD86 (CD86 molecule) had the highest connectivity among the crucial genes. All crucial genes were validated successfully, and sensitivity analysis demonstrated that our results were reliable.ConclusionTo the best of our knowledge, this study is the first to combine DEGs and WGCNA to establish a DEG co-expression network in carotid plaques, and it proposes potential therapeutic targets for carotid atherosclerosis.

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Section: Discussionmentioning

confidence: 99%

Weighted Gene Co-expression Network Analysis Identifies Crucial Genes Mediating Progression of Carotid Plaque

Chen

Yang

et al. 2021

Front. Physiol.

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“…Recently, the role of ARHGAP18 has been extensively studied in the context of atherosclerosis, a chronic inflammatory disease of the arteries [ 43 ]. ARHGAP18 was shown to act as an anti-inflammatory and athero-protective gene that facilitates flow-responsive endothelial cell alignment via ARHGAP18/YAP axis [ 29 , 30 ]. Interestingly, PKN3 was identified in a module of genes associated to transendothelial migration of leukocytes leading to coronary artery disease [ 44 ].…”

Section: Discussionmentioning

confidence: 99%

“…Overexpression of ARHGAP18 leads to premature senescence of endothelial cells [ 28 ]. Recently, it was shown to facilitate athero-protective endothelial cell alignment in response to laminar shear flow [ 29 , 30 ].…”

Section: Introductionmentioning

confidence: 99%

A Screen for PKN3 Substrates Reveals an Activating Phosphorylation of ARHGAP18

Dibus

Brábek

Rösel

2020

IJMS

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Protein kinase N3 (PKN3) is a serine/threonine kinase implicated in tumor progression of multiple cancer types, however, its substrates and effector proteins still remain largely understudied. In the present work we aimed to identify novel PKN3 substrates in a phosphoproteomic screen using analog sensitive PKN3. Among the identified putative substrates we selected ARHGAP18, a protein from RhoGAP family, for validation of the screen and further study. We confirmed that PKN3 can phosphorylate ARHGAP18 in vitro and we also characterized the interaction of the two proteins, which is mediated via the N-terminal part of ARHGAP18. We present strong evidence that PKN3-ARHGAP18 interaction is increased upon ARHGAP18 phosphorylation and that the phosphorylation of ARHGAP18 by PKN3 enhances its GAP domain activity and contributes to negative regulation of active RhoA. Taken together, we identified new set of potential PKN3 substrates and revealed a new negative feedback regulatory mechanism of Rho signaling mediated by PKN3-induced ARHGAP18 activation.

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“…Human umbilical vein endothelial cells (HUVECs) were obtained from umbilical cords by collagenase treatment [ 40 ], after donor informed consent, under Ethics approval by the Sydney Local Health District Human Ethics Committee, X16-0225. HUVECs were isolated and maintained in culture in MesoEndo growth medium (Lonza, Basel, Switzerland) in 5% CO 2 incubator.…”

Section: Methodsmentioning

confidence: 99%

Thromboinflammation Model-on-A-Chip by Whole Blood Microfluidics on Fixed Human Endothelium

et al. 2021

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Microfluidic devices have an established role in the study of platelets and coagulation factors in thrombosis, with potential diagnostic applications. However, few microfluidic devices have assessed the contribution of neutrophils to thrombus formation, despite increasing knowledge of neutrophils’ importance in cardiovascular thrombosis. We describe a thromboinflammation model which uses straight channels, lined with fixed human umbilical vein endothelial cells, after treatment with tumour necrosis factor-alpha. Re-calcified whole blood is perfused over the endothelium at venous and arterial shear rate. Neutrophil adhesion, platelet and fibrin thrombus formation, is measured over time by the addition of fluorescent antibodies to a whole blood sample. Fixed endothelium retains surface expression of adhesion molecules ICAM-1 and E-Selectin. Neutrophils adhere preferentially to platelet thrombi on the endothelium. Inhibitors of neutrophil adhesion and anti-inflammatory agents, such as isoquercetin, decrease neutrophil adhesion. Our model offers the advantage of the use of (1) fixed endothelium, (2) whole blood, instead of isolated neutrophils, and (3) a small amount of blood (1 mL). The characteristics of this thromboinflammation model provide the potential for further development for drug screening and point-of-care applications.

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YAP and the RhoC regulator ARHGAP18, are required to mediate flow-dependent endothelial cell alignment

Cited by 17 publications

References 38 publications

Weighted Gene Co-expression Network Analysis Identifies Crucial Genes Mediating Progression of Carotid Plaque

Weighted Gene Co-expression Network Analysis Identifies Crucial Genes Mediating Progression of Carotid Plaque

A Screen for PKN3 Substrates Reveals an Activating Phosphorylation of ARHGAP18

Thromboinflammation Model-on-A-Chip by Whole Blood Microfluidics on Fixed Human Endothelium

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