The fibrinolytic system and the regulation of lung epithelial cell proteolysis, signaling, and cellular viability

Shetty, Sreerama; Padijnayayveetil, Joseph; Tucker, Torry A.; Stankowska, Dorota; Idell, Steven

doi:10.1152/ajplung.90349.2008

Cited by 71 publications

(83 citation statements)

References 91 publications

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“…A feedback loop between TP53 and uPA expression has been demonstrated in lung epithelial cells. 27,28 Reintroduction of TP53 in TP53-deficient lung epithelial cells suppressed uPA expression. PAI-1, a family member of SerpinA5, was shown to be minimally expressed in TP53-deficient lung carcinoma cells.…”

Section: Serpina5 Expression In Serous Tumorsmentioning

confidence: 99%

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Loss of SerpinA5 protein expression is associated with advanced-stage serous ovarian tumors

et al. 2011

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Epithelial ovarian cancer, the most lethal neoplasm of the female genital tract, is usually diagnosed at an advanced stage as obvious symptoms are absent at early stages. This disease is believed to originate from malignant transformation of the ovarian surface epithelium or fallopian tube. Histologically, several subtypes are being recognized, with serous histology accounting for the majority of cases. Serous tumors include serous borderline tumors and serous carcinomas. A better understanding of the tumor biology and molecular mechanisms involved in these tumors is needed, as both patient management and prognosis differ substantially. Previous microarray analysis identified SerpinA5, a uPA inhibitor, as key regulator for indolent borderline behavior. As carcinomas are characterized by loss of SerpinA5 mRNA expression, we hypothesized that SerpinA5 protein expression is reduced or lost in carcinomas when compared with borderline tumors. We performed SerpinA5 immunohistochemical staining on 32 serous borderline tumors, 187 primary serous carcinomas and 62 serous omental metastases. Reduced or absent SerpinA5 protein staining was observed in carcinomas when compared with borderline tumors (Po0.001). SerpinA5 protein expression was significantly lowered in the omental metastases (Po0.001) when compared with the matching primary carcinoma. Interestingly, SerpinA5 protein expression was reduced in advanced-stage borderline tumors, often characterized by micropapillary growth and/or microinvasion, when compared with early-stage borderline tumors (P ¼ 0.015). In conclusion, SerpinA5 expression is significantly reduced in advanced-stage serous borderline tumors and serous carcinomas when compared with the early-stage counterparts, and reduction of expression is linked to more aggressive features of borderline tumors.

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Section: Serpina5 Expression In Serous Tumorsmentioning

confidence: 99%

“…PAI-1, a family member of SerpinA5, was shown to be minimally expressed in TP53-deficient lung carcinoma cells. 28 In serous carcinomas, TP53 mutations occur in up to 80% of cases. It is reasonable that SerpinA5 is downregulated in serous carcinomas as a result of this mutation.…”

Section: Serpina5 Expression In Serous Tumorsmentioning

confidence: 99%

Loss of SerpinA5 protein expression is associated with advanced-stage serous ovarian tumors

et al. 2011

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“…This association has been investigated in animal models with a number of different causes of lung injury, such as endotoxin, hyperoxia, trauma, hemorrhage, or pneumonia (2,7,8,14,44,54), but not in Cl 2 -induced lung injury. Moreover, pulmonary inflammation can cause local disturbances in fibrin turnover whereas increased intra-alveolar fibrin deposition with decreased breakdown may induce inflammation (44). Given this tight cross talk between coagulation and inflammation, the administration of an agent (such as heparin) that has both anti-coagulant as well as anti-inflammatory properties (53) may reduce the disturbance in pulmonary coagulopathy and inflammation, thereby ameliorating the clinical course of ALI.…”

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confidence: 99%

Postexposure aerosolized heparin reduces lung injury in chlorine-exposed mice

Zarogiannis

Wagener

Basappa

et al. 2014

American Journal of Physiology-Lung Cellular and Molecular Phys

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“…The fibrinolytic system helps limit the deposition of fibrin in the small airways and alveolar compartment of the normal lung (1). Bronchoalveolar lavage (BAL) fluid from healthy individuals contains detectable amounts of urokinase-type plasminogen activator (uPA) (2,3).…”

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confidence: 99%

“…Bronchoalveolar lavage (BAL) fluid from healthy individuals contains detectable amounts of urokinase-type plasminogen activator (uPA) (2,3). The exuberant expression of plasminogen activator inhibitor-1 (PAI-1) and the inhibition of plasmin are characteristic of the fibrinolytic defect in patients with acute respiratory distress syndrome (ARDS) and various forms of lung injury associated with the persistence of alveolar hyaline membranes and disordered lung remodeling (1,4). Furthermore, intraalveolar fibrin fails to deposit in response to hyperoxia in mice deficient in PAI-1, suggesting that the balance between plasminogen activators and their major inhibitor plays a crucial role in preventing the clearance of alveolar fibrin (5).…”

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confidence: 99%

Urokinase Plasminogen Activator Regulates Pulmonary Arterial Contractility and Vascular Permeability in Mice

Nassar

Yarovoi

Fanne

et al. 2011

Am J Respir Cell Mol Biol

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The concentration of urokinase plasminogen activator (uPA) is elevated in pathological settings such as acute lung injury, where pulmonary arterial contractility and permeability are disrupted. uPA limits the accretion of fibrin after injury. Here we investigated whether uPA also regulates pulmonary arterial contractility and permeability. Contractility was measured using isolated pulmonary arterial rings. Pulmonary blood flow was measured in vivo by Doppler and pulmonary vascular permeability, according to the extravasation of Evans blue. Our data show that uPA regulates the in vitro pulmonary arterial contractility induced by phenylephrine in a dose-dependent manner through two receptor-dependent pathways, and regulates vascular contractility and permeability in vivo. Physiological concentrations of uPA (<1 nM) stimulate the contractility of pulmonary arterial rings induced by phenylephrine through the low-density lipoprotein receptor-related protein receptor. The procontractile effect of uPA is independent of its catalytic activity. At pathophysiological concentrations, uPA (20 nM) inhibits contractility and increases vascular permeability. The inhibition of vascular contractility and increase of vascular permeability is mediated through a two-step process that involves docking to N-methyl-Daspartate receptor-1 (NMDA-R1) on pulmonary vascular smooth muscle cells, and requires catalytic activity. Peptides that specifically inhibit the docking of uPA to NMDA-R, or the uPA variant with a mutated receptor docking site, abolished both the effects of uPA on vascular contractility and permeability, without affecting its catalytic activity. These data show that uPA, at concentrations found under pathological conditions, reduces pulmonary arterial contractility and increases permeability though the activation of NMDA-R1. The selective inhibition of NMDAR-1 activation by uPA can be accomplished without a loss of fibrinolytic activity.

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The fibrinolytic system and the regulation of lung epithelial cell proteolysis, signaling, and cellular viability

Cited by 71 publications

References 91 publications

Loss of SerpinA5 protein expression is associated with advanced-stage serous ovarian tumors

Loss of SerpinA5 protein expression is associated with advanced-stage serous ovarian tumors

Postexposure aerosolized heparin reduces lung injury in chlorine-exposed mice

Urokinase Plasminogen Activator Regulates Pulmonary Arterial Contractility and Vascular Permeability in Mice

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