Receptors of the protein C activation and activated protein C signaling pathways are colocalized in lipid rafts of endothelial cells

Bae, Jong‐Sup; Yang, Likui; Rezaie, Alireza R.

doi:10.1073/pnas.0611493104

Cited by 174 publications

(224 citation statements)

References 40 publications

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“…Our findings further indicate that PAR1 and β-arrestins are preassembled and coexist in caveolar microdomains. These results are consistent with the importance of PAR1 compartmentalization in caveolar microdomains for APCinduced cytoprotective signaling (5,6). This work also indicates that the β-arrestin-2 isoform is the predominant mediator of APC-induced cytoprotective signaling and is consistent with previous studies demonstrating a protective role in vivo for β-arrestin-2 in mouse models of experimentally induced sepsis lethality (23,24).…”

Section: Discussionsupporting

confidence: 81%

“…1A). These findings confirm that PAR1 is present in caveolar microdomains (5,6). In addition, both β-arrestin-1 and -2 isoforms were detected in caveolin-1-enriched fractions in control cells (Fig.…”

supporting

confidence: 76%

“…partmentalization in caveolae (5,6). We found that endogenous PAR1 and β-arrestins exist in a preassembled complex and localize to caveolar microdomains, consistent with a function in cytoprotective signaling.…”

Section: Discussionmentioning

confidence: 73%

“…In addition, APC bound to EPCR on endothelial cells promotes anti-inflammatory and cytoprotective signaling through the activation of PAR1 (4). APC cytoprotective signaling also requires the compartmentalization of PAR1 and its coreceptor EPCR in cholesterol-enriched caveolar microdomains (5,6). A previous study further showed that the cytoprotective activity of a noncoagulant APC is critical for reducing mortality associated with sepsis in an experimental mouse model (7).…”

mentioning

confidence: 99%

“…These findings reveal a unique function for β-arrestin and Dvl-2 scaffolds in APC-promoted PAR1 cytoprotective signaling in cultured human endothelial cells and provide further support for β-arrestins as negative regulators of sepsis-induced inflammatory responses observed in vivo (23,24). The compartmentalization of PAR1 in caveolar microdomains is critical for APC-promoted Rac1 activation and endothelial barrier protection (5,6). To define the mediators of APC-activated PAR1 signaling, we examined whether Gα i and/or β-arrestins localize to caveolar microdomains together with PAR1 in human umbilical vein endothelial cell-derived EA.hy926 cells using sucrose densitygradient fractionation.…”

mentioning

confidence: 99%

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Activated protein C promotes protease-activated receptor-1 cytoprotective signaling through β-arrestin and dishevelled-2 scaffolds

Soh

Trejo

2011

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

140

171

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Protease-activated receptor-1 (PAR1) is a guanine nucleotidebinding (G) protein-coupled receptor that elicits cellular responses to coagulant and anticoagulant proteases. Activation of PAR1 by the coagulant protease thrombin results in Ras homolog gene family member A (RhoA) activation, disassembly of adherens junctions, and disruption of the endothelial barrier. In contrast, activation of PAR1 with the anticoagulant protease activated protein C (APC) results in activation of Ras-related C3 botulinum toxin substrate 1 (Rac1) and endothelial barrier protection. We previously showed that APC cytoprotective signaling requires the compartmentalization of PAR1 in caveolar microdomains. However, the mechanism by which APC-activated PAR1 promotes cytoprotective signaling in human endothelial cells remains poorly understood. Here we show that APC-activated PAR1 cytoprotective signaling is mediated by β-arrestin recruitment and activation of the dishevelled-2 (Dvl-2) scaffold and not by G protein α inhibiting activity polypeptide 2 (Gα i ) signaling. In human endothelial cells, PAR1 and β-arrestins form a preassembled complex and cosegregate in caveolin-1-enriched fractions. Remarkably, we found that depletion of β-arrestin expression by RNA interference resulted in the loss of APC-induced Rac1 activation but not of thrombin-stimulated RhoA signaling. APC also failed to protect against thrombin-induced endothelial barrier permeability in cells deficient in β-arrestin expression. We further demonstrate that APC activation of PAR1 results in β-arrestin-dependent recruitment of Dvl-2, which is critical for Rac1 signaling and endothelial barrier protection but not for thrombin-induced RhoA signaling. Our findings identify a role for β-arrestin and Dvl-2 scaffolds in APC-activated PAR1 cytoprotective signaling in human endothelial cells.biased agonism | endothelial dysfunction | inflammation | sepsis

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Section: Discussionsupporting

confidence: 81%

supporting

confidence: 76%

Section: Discussionmentioning

confidence: 73%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Activated protein C promotes protease-activated receptor-1 cytoprotective signaling through β-arrestin and dishevelled-2 scaffolds

Soh

Trejo

2011

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

140

171

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Xenoimmunity

Cowan

d’Apice

2014

Textbook of Organ Transplantation

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Barrier Enhancing Signals in Pulmonary Edema

Birukov

Zebda

Birukova

2013

Comprehensive Physiology

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Increased endothelial permeability and reduction of alveolar liquid clearance capacity are two leading pathogenic mechanisms of pulmonary edema, which is a major complication of acute lung injury, severe pneumonia, and acute respiratory distress syndrome, the pathologies characterized by unacceptably high rates of morbidity and mortality. Besides the success in protective ventilation strategies, no efficient pharmacological approaches exist to treat this devastating condition. Understanding of fundamental mechanisms involved in regulation of endothelial permeability is essential for development of barrier protective therapeutic strategies. Ongoing studies characterized specific barrier protective mechanisms and identified intracellular targets directly involved in regulation of endothelial permeability. Growing evidence suggests that, although each protective agonist triggers a unique pattern of signaling pathways, selected common mechanisms contributing to endothelial barrier protection may be shared by different barrier protective agents. Therefore, understanding of basic barrier protective mechanisms in pulmonary endothelium is essential for selection of optimal treatment of pulmonary edema of different etiology. This article focuses on mechanisms of lung vascular permeability, reviews major intracellular signaling cascades involved in endothelial monolayer barrier preservation and summarizes a current knowledge regarding recently identified compounds which either reduce pulmonary endothelial barrier disruption and hyperpermeability, or reverse preexisting lung vascular barrier compromise induced by pathologic insults.

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Receptors of the protein C activation and activated protein C signaling pathways are colocalized in lipid rafts of endothelial cells

Cited by 174 publications

References 40 publications

Activated protein C promotes protease-activated receptor-1 cytoprotective signaling through β-arrestin and dishevelled-2 scaffolds

Activated protein C promotes protease-activated receptor-1 cytoprotective signaling through β-arrestin and dishevelled-2 scaffolds

Xenoimmunity

Barrier Enhancing Signals in Pulmonary Edema

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