Search

Your search keyword '"Garcia-Pras E"' showing total 23 results
Start Over Author "Garcia-Pras E"
23 results on '"Garcia-Pras E"'

4. Ductular reaction cells promote angiogenesis via SLIT2/ROBO1 pathway in chronic liver disease

Author

Coll, M., primary, Garcia-Pras, E., additional, Aguilar-Bravo, B., additional, Gallego, J., additional, Blaya, D., additional, Vallverdú, J., additional, Perea, L., additional, Graupera, I., additional, Pose, E., additional, Lozano, J., additional, Bataller, R., additional, Ginès, P., additional, Geng, J.-G., additional, Fernandez, M., additional, and Sancho-Bru, P., additional

Published
2018
Full Text
View/download PDF

12. Ductular reaction promotes intrahepatic angiogenesis through Slit2-Roundabout 1 signaling.

Author

Coll M, Ariño S, Martínez-Sánchez C, Garcia-Pras E, Gallego J, Moles A, Aguilar-Bravo B, Blaya D, Vallverdú J, Rubio-Tomás T, Lozano JJ, Pose E, Graupera I, Fernández-Vidal A, Pol A, Bataller R, Geng JG, Ginès P, Fernandez M, and Sancho-Bru P

Subjects
Animals, Blood Vessels metabolism, Chronic Disease, Disease Progression, Gene Expression, Gene Ontology, Hepatitis, Alcoholic pathology, Hepatitis, Alcoholic physiopathology, Humans, Intercellular Signaling Peptides and Proteins metabolism, Liver metabolism, Liver Diseases, Alcoholic genetics, Liver Diseases, Alcoholic metabolism, Liver Diseases, Alcoholic pathology, Mice, Neovascularization, Pathologic pathology, Neovascularization, Physiologic genetics, Nerve Tissue Proteins metabolism, Organoids, Patient Acuity, Receptors, Immunologic metabolism, Signal Transduction genetics, Stem Cells, Up-Regulation, Vascular Remodeling, Wound Healing, Roundabout Proteins, Intercellular Signaling Peptides and Proteins genetics, Liver physiopathology, Liver Diseases, Alcoholic physiopathology, Neovascularization, Pathologic genetics, Nerve Tissue Proteins genetics, Receptors, Immunologic genetics
Abstract

Background and Aims: Ductular reaction (DR) expands in chronic liver diseases and correlates with disease severity. Besides its potential role in liver regeneration, DR plays a role in the wound-healing response of the liver, promoting periductular fibrosis and inflammatory cell recruitment. However, there is no information regarding its role in intrahepatic angiogenesis. In the current study we investigated the potential contribution of DR cells to hepatic vascular remodeling during chronic liver disease., Approach and Results: In mouse models of liver injury, DR cells express genes involved in angiogenesis. Among angiogenesis-related genes, the expression of Slit2 and its receptor Roundabout 1 (Robo1) was localized in DR cells and neoangiogenic vessels, respectively. The angiogenic role of the Slit2-Robo1 pathway in chronic liver disease was confirmed in ROBO1/2 -/+ mice treated with 3,5-diethoxycarbonyl-1,4-dihydrocollidine, which displayed reduced intrahepatic neovascular density compared to wild-type mice. However, ROBO1/2 deficiency did not affect angiogenesis in partial hepatectomy. In patients with advanced alcohol-associated disease, angiogenesis was associated with DR, and up-regulation of SLIT2-ROBO1 correlated with DR and disease severity. In vitro, human liver-derived organoids produced SLIT2 and induced tube formation of endothelial cells., Conclusions: Overall, our data indicate that DR expansion promotes angiogenesis through the Slit2-Robo1 pathway and recognize DR cells as key players in the liver wound-healing response., (© 2021 The Authors. Hepatology published by Wiley Periodicals LLC on behalf of American Association for the Study of Liver Diseases.)

Published
2022
Full Text
View/download PDF

13. Targeting the cytoplasmic polyadenylation element-binding protein CPEB4 protects against diet-induced obesity and microbiome dysbiosis.

Author

Pell N, Garcia-Pras E, Gallego J, Naranjo-Suarez S, Balvey A, Suñer C, Fernandez-Alfara M, Chanes V, Carbo J, Ramirez-Pedraza M, Reina O, Thingholm L, Bang C, Rühlemann M, Franke A, Schierwagen R, Rheinwalt KP, Trebicka J, Mendez R, and Fernandez M

Subjects
Adult, Diet, High-Fat adverse effects, Dysbiosis microbiology, Female, Gastrointestinal Microbiome, Humans, Male, Obesity microbiology, Polyadenylation, Dysbiosis metabolism, Obesity metabolism, RNA-Binding Proteins metabolism
Abstract

Objective: Obesity represents a growing health problem that is reaching pandemic dimensions and lacks effective cures, thus highlighting an urgent need for better mechanistic understanding and new therapeutic strategies. Unlike transcription, the function of translation in obesity has hardly been investigated. Here, we fill this knowledge gap by pinpointing a crucial function for gene regulation at the step of translation in diet-induced obesity., Methods: We performed studies with human adipose tissue, high-fat-diet-induced obese mice and rats, CPEB4-knockout mice, and adipocyte lines. Cells were transfected with small-interfering RNAs that knockdown CPEB4. Transcriptome-wide identification and validation of CPEB4 targets in adipocytes were obtained by RNA-protein coimmunoprecipitation and high-throughput sequencing. The effect of CPEB4 depletion on high-fat-diet-induced dysbiosis was determined by 16S ribosomal-RNA gene sequencing and microbiome bioinformatics., Results: We show that cytoplasmic polyadenylation element-binding protein 4 (CPEB4), which controls the translation of specific mRNAs by modulating their poly(A) tails, is highly expressed in visceral fat of obese but not lean humans and rodents (mice and rats), where it orchestrates an essential post-transcriptional reprogramming for aggravation of high-fat-diet-induced obesity. Mechanistically, CPEB4 overexpression in obese adipocytes activates the translation of factors essential for adipose tissue expansion (Cebpb, Stat5a) and adipocyte-intrinsic immune-like potential (Ccl2, Tlr4), as demonstrated by RNA-immunoprecipitation and high-throughput sequencing and experimentally validated in vivo. Consistently blocking CPEB4 production in knockout mice protects against diet-induced body weight gain and reduces adipose tissue enlargement and inflammation. In addition, the depletion of CPEB4 specifically in obese adipocytes using short hairpin RNAs decreases cell differentiation, lipid accumulation, and the proinflammatory and migratory capacity of macrophages. The absence of CPEB4 also attenuates high-fat diet-induced dysbiosis, shaping the microbiome composition toward a more beneficial profile, as shown by microbiome bioinformatics analysis., Conclusion: Our study identifies CPEB4 as a driver and therapeutic target to combat obesity., Competing Interests: Conflict of interest Authors declare that they have no competing interests., (Copyright © 2021 The Author(s). Published by Elsevier GmbH.. All rights reserved.)

Published
2021
Full Text
View/download PDF

14. Therapeutic siRNA targeting endothelial KDR decreases portosystemic collateralization in portal hypertension.

Author

Gallego J, Garcia-Pras E, Mejias M, Pell N, Schaeper U, and Fernandez M

Subjects
Animals, Humans, Male, Mice, Mice, Inbred BALB C, Endothelium, Vascular metabolism, Endothelium, Vascular pathology, Hypertension, Portal genetics, Hypertension, Portal metabolism, Hypertension, Portal pathology, Hypertension, Portal therapy, Neovascularization, Pathologic genetics, Neovascularization, Pathologic metabolism, Neovascularization, Pathologic pathology, Neovascularization, Pathologic therapy, RNA, Small Interfering genetics, RNA, Small Interfering pharmacology, Vascular Endothelial Growth Factor Receptor-2 antagonists & inhibitors, Vascular Endothelial Growth Factor Receptor-2 biosynthesis, Vascular Endothelial Growth Factor Receptor-2 genetics
Abstract

Development of portosystemic collateral vessels and gastroesophageal varices is responsible for the most serious clinical consequences of portal hypertension, but effective clinical therapies are limited. Here we developed and investigated the therapeutic potential of an innovative liposomally-formulated short-interfering RNA (siRNA) technology based on clinical stage components, capable to attenuate production of the endothelial kinase insert domain receptor (KDR), which controls portosystemic collateralization and contributes to disease progression and aggravation. These siRNAs were first validated in vitro, and then, their therapeutic potential on portosystemic collateralization and pathological angiogenesis was tested in vivo in mouse models of portal hypertension (portal vein-ligation). siRNA KDR -lipoplexes efficiently transported siRNA KDR to vascular endothelial cells in mesenteric microvenules and portal vein of portal hypertensive mice, where collaterogenesis and angiogenesis take place. This systemic treatment significantly downregulated pathological KDR overexpression, without causing complete KDR knockout, preserving homeostatic baseline KDR levels and thus limiting adverse effects. siRNA KDR -lipoplex-induced endothelial-specific KDR knockdown drastically reduced by 73% the portosystemic collateralization, and impaired the pathologic angiogenic potential of vascular endothelial cells at different levels (cell proliferation, sprouting and remodeling). Targeting endothelial KDR with therapeutic siRNA KDR -lipoplexes could be a promising and plausible treatment modality for attenuating the formation of portosystemic collaterals in a clinical setting.

Published
2017
Full Text
View/download PDF

15. Role and therapeutic potential of vascular stem/progenitor cells in pathological neovascularisation during chronic portal hypertension.

Author

Garcia-Pras E, Gallego J, Coch L, Mejias M, Fernandez-Miranda G, Pardal R, Bosch J, Mendez R, and Fernandez M

Subjects
Animals, Cell Differentiation, Cell Proliferation, Mice, Rats, Hypertension, Portal pathology, Neovascularization, Pathologic, RNA-Binding Proteins metabolism, Stem Cells cytology
Abstract

Objective: Pathological neovascularisation is intimately involved in portal hypertension (PH). Here, we determined the contribution of vascular stem/progenitor cells (VSPCs) to neovessel growth in PH and whether the RNA-binding protein cytoplasmic polyadenylation element binding protein-4 (CPEB4) was behind the mechanism controlling VSPC function., Design: To identify and monitor VSPCs in PH rats (portal vein-ligated), we used a combinatorial approach, including sphere-forming assay, assessment of self-renewal, 5-bromo-2'-desoxyuridine label retention technique, in vitro and in vivo stem/progenitor cell (SPC) differentiation and vasculogenic capability, cell sorting, as well as immunohistochemistry, immunofluorescence and confocal microscopy expression analysis. We also determined the role of CPEB4 on VSPC proliferation using genetically engineered mouse models., Results: We demonstrated the existence in the mesenteric vascular bed of VSPCs displaying capability to form cellular spheres in suspension culture, self-renewal ability, expression of molecules commonly found in SPCs, slow-cycling features, in addition to other cardinal properties exhibited by SPCs, like capacity to differentiate into endothelial cells and pericytes with remarkable vasculogenic activity. Such VSPCs showed, after PH induction, an early switch in proliferation, and differentiated in vivo into endothelial cells and pericytes, contributing, structurally and functionally, to abnormal neovessel formation. Quantification of VSPC-dependent neovessel formation in PH further illustrated the key role played by VSPCs. We also demonstrated that CPEB4 regulates the proliferation of the activated VSPC progeny upon PH induction., Conclusions: These findings demonstrate that VSPC-derived neovessel growth (ie, vasculogenesis) and angiogenesis cooperatively stimulate mesenteric neovascularisation in PH and identify VSPC and CPEB4 as potential therapeutic targets., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.)

Published
2017
Full Text
View/download PDF

16. Sequential Functions of CPEB1 and CPEB4 Regulate Pathologic Expression of Vascular Endothelial Growth Factor and Angiogenesis in Chronic Liver Disease.

Author

Calderone V, Gallego J, Fernandez-Miranda G, Garcia-Pras E, Maillo C, Berzigotti A, Mejias M, Bava FA, Angulo-Urarte A, Graupera M, Navarro P, Bosch J, Fernandez M, and Mendez R

Subjects
3' Untranslated Regions, Adult, Animals, Case-Control Studies, Cell Line, Chronic Disease, Disease Models, Animal, Female, Gene Expression Regulation, Humans, Hypertension, Portal genetics, Hypertension, Portal pathology, Liver Cirrhosis pathology, Liver Cirrhosis virology, Liver Cirrhosis, Biliary genetics, Liver Cirrhosis, Biliary pathology, Male, Mice, 129 Strain, Mice, Inbred C57BL, Middle Aged, Polyadenylation, RNA Interference, RNA, Messenger genetics, RNA, Messenger metabolism, RNA-Binding Proteins genetics, Rats, Sprague-Dawley, Signal Transduction, Time Factors, Transcription Factors deficiency, Transcription Factors genetics, Transfection, mRNA Cleavage and Polyadenylation Factors deficiency, mRNA Cleavage and Polyadenylation Factors genetics, Hypertension, Portal metabolism, Liver Cirrhosis metabolism, Liver Cirrhosis, Biliary metabolism, Neovascularization, Pathologic, RNA-Binding Proteins metabolism, Transcription Factors metabolism, Vascular Endothelial Growth Factor A metabolism, mRNA Cleavage and Polyadenylation Factors metabolism
Abstract

Background & Aims: Vascular endothelial growth factor (VEGF) regulates angiogenesis, yet therapeutic strategies to disrupt VEGF signaling can interfere with physiologic angiogenesis. In a search for ways to inhibit pathologic production or activities of VEGF without affecting its normal production or functions, we investigated the post-transcriptional regulation of VEGF by the cytoplasmic polyadenylation element-binding proteins CPEB1 and CPEB4 during development of portal hypertension and liver disease., Methods: We obtained transjugular liver biopsies from patients with hepatitis C virus-associated cirrhosis or liver tissues removed during transplantation; healthy human liver tissue was obtained from a commercial source (control). We also performed experiments with male Sprague-Dawley rats and CPEB-deficient mice (C57BL6 or mixed C57BL6/129 background) and their wild-type littermates. Secondary biliary cirrhosis was induced in rats by bile duct ligation, and portal hypertension was induced by partial portal vein ligation. Liver and mesenteric tissues were collected and analyzed in angiogenesis, reverse transcription polymerase chain reaction, polyA tail, 3' rapid amplification of complementary DNA ends, Southern blot, immunoblot, histologic, immunohistochemical, immunofluorescence, and confocal microscopy assays. CPEB was knocked down with small interfering RNAs in H5V endothelial cells, and translation of luciferase reporters constructs was assessed., Results: Activation of CPEB1 promoted alternative nuclear processing within noncoding 3'-untranslated regions of VEGF and CPEB4 messenger RNAs in H5V cells, resulting in deletion of translation repressor elements. The subsequent overexpression of CPEB4 promoted cytoplasmic polyadenylation of VEGF messenger RNA, increasing its translation; the high levels of VEGF produced by these cells led to their formation of tubular structures in Matrigel assays. We observed increased levels of CPEB1 and CPEB4 in cirrhotic liver tissues from patients, compared with control tissue, as well as in livers and mesenteries of rats and mice with cirrhosis or/and portal hypertension. Mice with knockdown of CPEB1 or CPEB4 did not overexpress VEGF or have signs of mesenteric neovascularization, and developed less-severe forms of portal hypertension after portal vein ligation., Conclusions: We identified a mechanism of VEGF overexpression in liver and mesentery that promotes pathologic, but not physiologic, angiogenesis, via sequential and nonredundant functions of CPEB1 and CPEB4. Regulation of CPEB4 by CPEB1 and the CPEB4 autoamplification loop induces pathologic angiogenesis. Strategies to block the activities of CPEBs might be developed to treat chronic liver and other angiogenesis-dependent diseases., (Copyright © 2016 AGA Institute. Published by Elsevier Inc. All rights reserved.)

Published
2016
Full Text
View/download PDF

17. Antiangiogenic and antifibrogenic activity of pigment epithelium-derived factor (PEDF) in bile duct-ligated portal hypertensive rats.

Author

Mejias M, Coch L, Berzigotti A, Garcia-Pras E, Gallego J, Bosch J, and Fernandez M

Subjects
Animals, Bile Ducts, Humans, Ligation, Male, Portal Pressure, Rats, Rats, Sprague-Dawley, Eye Proteins physiology, Eye Proteins therapeutic use, Hypertension, Portal etiology, Hypertension, Portal prevention & control, Liver Cirrhosis prevention & control, Neovascularization, Pathologic prevention & control, Nerve Growth Factors physiology, Nerve Growth Factors therapeutic use, Serpins physiology, Serpins therapeutic use
Abstract

Objective: Antiangiogenic strategies have been proposed as a promising new approach for the therapy of portal hypertension and chronic liver disease. Pigment epithelium-derived factor (PEDF) is a powerful endogenous angiogenesis inhibitor whose role in portal hypertension remains unknown. Therefore, we aimed at determining the involvement of PEDF in cirrhotic portal hypertension and the therapeutic efficacy of its supplementation., Design: PEDF expression profiling and its relationship with vascular endothelial growth factor (VEGF), neovascularisation and fibrogenesis was determined in bile duct-ligated (BDL) rats and human cirrhotic livers. The ability of exogenous PEDF overexpression by adenovirus-mediated gene transfer (AdPEDF) to inhibit angiogenesis, fibrogenesis and portal pressure was also evaluated in BDL rats, following prevention and intervention trials., Results: PEDF was upregulated in cirrhotic human and BDL rat livers. PEDF and VEGF protein expression and localisation in mesentery and liver increased in parallel with portal hypertension progression, being closely linked in time and space with mesenteric neovascularisation and liver fibrogenesis in BDL rats. Furthermore, AdPEDF increased PEDF bioavailability in BDL rats, shifting the net balance in the local abundance of positive (VEGF) and negative (PEDF) angiogenesis drivers in favour of attenuation of portal hypertension-associated pathological neovascularisation. The antiangiogenic effects of AdPEDF targeted only pathological angiogenesis, without affecting normal vasculature, and were observed during early stages of disease. AdPEDF also significantly decreased liver fibrogenesis (through metalloproteinase upregulation), portosystemic collateralisation and portal pressure in BDL rats., Conclusions: This study provides compelling experimental evidence indicating that PEDF could be a novel therapeutic agent worthy of assessment in portal hypertension and cirrhosis., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://group.bmj.com/group/rights-licensing/permissions.)

Published
2015
Full Text
View/download PDF

18. Disruption of negative feedback loop between vasohibin-1 and vascular endothelial growth factor decreases portal pressure, angiogenesis, and fibrosis in cirrhotic rats.

Author

Coch L, Mejias M, Berzigotti A, Garcia-Pras E, Gallego J, Bosch J, Mendez R, and Fernandez M

Subjects
Adenoviridae genetics, Animals, Cell Cycle Proteins genetics, Chronic Disease, Feedback, Physiological physiology, Gene Expression physiology, Hepatic Stellate Cells metabolism, Homeostasis physiology, Humans, Hyperemia metabolism, Hyperemia physiopathology, Hypertension, Portal metabolism, Hypertension, Portal physiopathology, Liver Cirrhosis physiopathology, Male, Neovascularization, Pathologic physiopathology, Rats, Rats, Sprague-Dawley, Splanchnic Circulation physiology, Vascular Endothelial Growth Factor A genetics, Cell Cycle Proteins metabolism, Liver Cirrhosis metabolism, Neovascularization, Pathologic metabolism, Vascular Endothelial Growth Factor A metabolism
Abstract

Unlabelled: Pathological angiogenesis represents a critical hallmark for chronic liver diseases. Understanding the mechanisms regulating angiogenesis is essential to develop new therapeutic strategies that specifically target pathological angiogenesis without affecting physiological angiogenesis. Here we investigated the contribution and therapeutic impact of the endogenous angioinhibitor vasohibin-1 in portal hypertension and cirrhosis. The spatiotemporal expression profiling of vasohibin-1 and its relationship with vascular endothelial growth factor (VEGF), angiogenesis, and fibrogenesis was determined through the analysis of human cirrhotic liver specimens, widely accepted in vivo animal models of portal hypertension and cirrhosis, and in vitro angiogenesis assays. Effects of vasohibin-1 overexpression by adenoviral-mediated gene transfer on angiogenesis, fibrogenesis, and portal hypertension-associated hemodynamic alterations were also studied in rats. We found that vasohibin-1 and VEGF are up-regulated, in mesentery and liver, in cirrhotic and precirrhotic portal hypertensive rats and cirrhosis patients. Our results are consistent with vasohibin-1/VEGF cascades being spatially and temporally coordinated through a negative-feedback loop driving pathological angiogenesis. Paradoxically, further overexpression of vasohibin-1 by adenoviral gene transfer exerts multifold beneficial effects in portal hypertension and cirrhosis: reduction of pathologic angiogenesis, attenuation of liver fibrogenesis partly mediated through inhibition of hepatic stellate cell activation, and significant decreases in portocollateralization, splanchnic blood flow, portohepatic resistance, and portal pressure. The explanation for this apparent contradiction is that, unlike endogenous vasohibin-1, the ectopic overexpression is not regulated by VEGF and therefore disrupts the negative-feedback loop, thus generating constant, but lower levels of VEGF synthesis sufficient to maintain vascular homeostasis but not pathological angiogenesis., Conclusion: Our study provides evidence that vasohibin-1 regulates portal hypertension-associated pathological angiogenesis and highlights that increasing vasohibin-1 might be a promising novel therapeutic strategy for portal hypertension and cirrhosis., (© 2014 by the American Association for the Study of Liver Diseases.)

Published
2014
Full Text
View/download PDF

19. Relevance of the mTOR signaling pathway in the pathophysiology of splenomegaly in rats with chronic portal hypertension.

Author

Mejias M, Garcia-Pras E, Gallego J, Mendez R, Bosch J, and Fernandez M

Subjects
Animals, Apoptosis drug effects, Apoptosis immunology, Cell Division drug effects, Cell Division immunology, Fibrosis, Hematocrit, Hypertension, Portal drug therapy, Immunosuppressive Agents pharmacology, Lymphocytes cytology, Lymphocytes drug effects, Lymphoid Tissue metabolism, Lymphoid Tissue pathology, Male, Neovascularization, Pathologic drug therapy, Neovascularization, Pathologic metabolism, Neovascularization, Pathologic physiopathology, Organ Size, Rats, Rats, Sprague-Dawley, Signal Transduction drug effects, Spleen blood supply, Spleen metabolism, Spleen pathology, Splenomegaly drug therapy, TOR Serine-Threonine Kinases, Hypertension, Portal metabolism, Hypertension, Portal physiopathology, Intracellular Signaling Peptides and Proteins metabolism, Protein Serine-Threonine Kinases metabolism, Signal Transduction physiology, Sirolimus pharmacology, Splenomegaly metabolism, Splenomegaly physiopathology
Abstract

Background & Aims: Splenomegaly is a frequent hallmark of portal hypertension that, in some cases, can be very prominent and cause symptoms like abdominal pain, splenic infarction, and cytopenia. This study characterizes the pathogenetic mechanisms leading to spleen enlargement in portal hypertensive rats and focuses on mTOR pathway as a potential modulator of splenomegaly in portal hypertension., Methods: Characterization of splenomegaly was performed by histological, hematological, immunohistochemical and Western blot analyses in rats with portal hypertension induced by portal vein ligation, and compared with sham-operated animals. The contribution of the mTOR signaling pathway to splenomegaly was determined in rats with fully developed portal hypertension and control rats by treatment with rapamycin or vehicle., Results: Our results illustrate that splenomegaly in portal hypertensive rats arises as a consequence of the interplay of several factors, including not only spleen congestion, as traditionally thought, but also enlargement and hyperactivation of the splenic lymphoid tissue, as well as increased angiogenesis and fibrogenesis. Since mTOR signaling plays a central role in immunological processes, angiogenesis and fibrogenesis, we next determined the involvement of mTOR in splenomegaly. Interestingly, mTOR signaling was overactivated in the spleen of portal hypertensive rats, and mTOR blockade by rapamycin profoundly ameliorated splenomegaly, causing a 44% decrease in spleen size. This effect was most likely accounted for the inhibitory action of rapamycin on lymphocyte proliferation, neovascularization and fibrosis., Conclusions: These findings shed light on the pathogenesis of splenomegaly in portal hypertension, and identify mTOR signaling as a potential target for therapeutic intervention in this disease.

Published
2010
Full Text
View/download PDF

20. Beneficial effects of sorafenib on splanchnic, intrahepatic, and portocollateral circulations in portal hypertensive and cirrhotic rats.

Author

Mejias M, Garcia-Pras E, Tiani C, Miquel R, Bosch J, and Fernandez M

Subjects
Animals, Benzenesulfonates pharmacology, Collateral Circulation drug effects, Enteritis drug therapy, Enteritis etiology, Heme Oxygenase-1 metabolism, Hepatitis drug therapy, Hepatitis etiology, Hypertension, Portal etiology, Liver metabolism, Liver Cirrhosis complications, Male, Neovascularization, Physiologic drug effects, Niacinamide analogs & derivatives, Nitric Oxide Synthase Type III metabolism, Phenylurea Compounds, Protein Kinase Inhibitors pharmacology, Pyridines pharmacology, Rats, Rats, Sprague-Dawley, Sorafenib, Benzenesulfonates therapeutic use, Hypertension, Portal drug therapy, Liver Cirrhosis drug therapy, Protein Kinase Inhibitors therapeutic use, Pyridines therapeutic use, Splanchnic Circulation drug effects
Abstract

Unlabelled: Portal hypertension, the most important complication in patients with cirrhosis of the liver, is a serious and life-threatening disease for which there are few therapeutic options. Because angiogenesis is a pathological hallmark of portal hypertension, the goal of this study was to determine the effects of sorafenib-a potent inhibitor of proangiogenic vascular endothelial growth factor receptor 2 (VEGFR-2), platelet-derived growth factor receptor beta (PDGFR-beta), and Raf kinases-on splanchnic, intrahepatic, systemic, and portosystemic collateral circulations in two different experimental models of portal hypertension: rats with prehepatic portal hypertension induced by partial portal vein ligation and rats with intrahepatic portal hypertension and secondary biliary cirrhosis induced by bile duct ligation. Such a comprehensive approach is necessary for any translational research directed toward defining the efficacy and potential clinical application of new therapeutic agents. Sorafenib administered orally once a day for 2 weeks in experimental models of portal hypertension and cirrhosis effectively inhibited VEGF, PDGF, and Raf signaling pathways, and produced several protective effects by inducing an approximately 80% decrease in splanchnic neovascularization and a marked attenuation of hyperdynamic splanchnic and systemic circulations, as well as a significant 18% decrease in the extent of portosystemic collaterals. In cirrhotic rats, sorafenib treatment also resulted in a 25% reduction in portal pressure, as well as a remarkable improvement in liver damage and intrahepatic fibrosis, inflammation, and angiogenesis. Notably, beneficial effects of sorafenib against tissue damage and inflammation were also observed in splanchnic organs., Conclusion: Taking into account the limitations of translating animal study results into humans, we believe that our findings will stimulate consideration of sorafenib as an effective therapeutic agent in patients suffering from advanced portal hypertension.

Published
2009
Full Text
View/download PDF

21. Apelin signaling modulates splanchnic angiogenesis and portosystemic collateral vessel formation in rats with portal hypertension.

Author

Tiani C, Garcia-Pras E, Mejias M, de Gottardi A, Berzigotti A, Bosch J, and Fernandez M

Subjects
Animals, Apelin, Apelin Receptors, Carrier Proteins analysis, Carrier Proteins genetics, Collateral Circulation, Extracellular Signal-Regulated MAP Kinases metabolism, Heme Oxygenase (Decyclizing) genetics, Hypertension, Portal physiopathology, Intercellular Signaling Peptides and Proteins, Male, Myosin Light Chains genetics, Nitric Oxide Synthase Type III genetics, Phosphorylation, Rats, Rats, Sprague-Dawley, Receptors, G-Protein-Coupled analysis, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled physiology, Ribosomal Protein S6 Kinases, 70-kDa metabolism, Tumor Necrosis Factor-alpha biosynthesis, Carrier Proteins physiology, Neovascularization, Physiologic, Portal System physiopathology, Signal Transduction physiology, Splanchnic Circulation
Abstract

Background/aims: Angiogenesis is a pathological hallmark of portal hypertension. Although VEGF is considered to be the most important proangiogenic factor in neoangiogenesis, this process requires the coordinated action of a variety of factors. Identification of novel molecules involved in angiogenesis is highly relevant, since they may represent potential new targets to suppress pathological neovascularization in angiogenesis-related diseases like portal hypertension. The apelin/APJ signaling pathway plays a crucial role in angiogenesis. Therefore, we determined whether the apelin system modulates angiogenesis-driven processes in portal hypertension., Methods: Partial portal vein-ligated rats were treated with the APJ antagonist F13A for seven days. Splanchnic neovascularization and expression of angiogenesis mediators (Western blotting) was determined. Portosystemic collateral formation (microspheres), and hemodynamic parameters (flowmetry) were also assessed., Results: Apelin and its receptor APJ were overexpressed in the splanchnic vasculature of portal hypertensive rats. F13A effectively decreased, by 52%, splanchnic neovascularization and expression of proangiogenic factors VEGF, PDGF and angiopoietin-2 in portal hypertensive rats. F13A also reduced, by 35%, the formation of portosystemic collateral vessels., Conclusions: This study provides the first experimental evidence showing that the apelin/APJ system contributes to portosystemic collateralization and splanchnic neovascularization in portal hypertensive rats, presenting a potential novel therapeutic target for portal hypertension.

Published
2009
Full Text
View/download PDF

22. The somatostatin analogue octreotide inhibits angiogenesis in the earliest, but not in advanced, stages of portal hypertension in rats.

Author

Mejias M, Garcia-Pras E, Tiani C, Bosch J, and Fernandez M

Subjects
Animals, Gene Expression Regulation drug effects, Heme Oxygenase-1 genetics, Heme Oxygenase-1 metabolism, Hemodynamics drug effects, Hypertension, Portal genetics, Hypertension, Portal metabolism, Male, Neovascularization, Pathologic genetics, Neovascularization, Pathologic metabolism, Nitric Oxide Synthase Type III genetics, Nitric Oxide Synthase Type III metabolism, Octreotide chemistry, Rats, Rats, Sprague-Dawley, Receptors, Somatostatin metabolism, Vascular Endothelial Growth Factor A genetics, Vascular Endothelial Growth Factor A metabolism, Hypertension, Portal drug therapy, Hypertension, Portal pathology, Neovascularization, Pathologic drug therapy, Octreotide therapeutic use, Somatostatin analogs & derivatives
Abstract

Background: Angiogenesis is an important determinant of the pathophysiology of portal hypertension contributing to the formation of portosystemic collateral vessels and the hyperdynamic splanchnic circulation associated to this syndrome. Somatostatin and its analogues, like octreotide, have been shown to be powerful inhibitors of experimental angiogenesis., Aim: To determine whether octreotide has angioinhibitory effects in portal hypertensive rats., Methods: Partial portal vein-ligated (PPVL) rats were treated with octreotide or vehicle during 4 or 7 days. Splanchnic neovascularization and VEGF expression were determined by histological analysis and western blotting. Expression of the somatostatin receptor subtype 2 (SSTR2), which mediates the anti-angiogenic effects of octreotide, was also analyzed. Formation of portosystemic collaterals (radioactive microspheres) and hemodynamic parameters were also measured., Results: Octreotide treatment during 4 days markedly and significantly decreased splanchnic neovascularization, VEGF expression by 63% and portal pressure by 15%, whereas portosystemic collateralization and splanchnic blood flow were not modified. After 1 week of octreotide injection, portal pressure was reduced by 20%, but inhibition of angiogenesis escaped from octreotide therapy, a phenomenon that could be related to the finding that expression of SSTR2 receptor decreased progressively (up to 78% reduction) during the evolution of portal hypertension., Conclusion: This study provides the first experimental evidence showing that octreotide may be an effective anti-angiogenic therapy early after induction of portal hypertension, but not in advanced stages most likely due to SSTR2 down-regulation during the progression of portal hypertension in rats. These findings shed light on new mechanisms of action of octreotide in portal hypertension.

Published
2008
Full Text
View/download PDF

23. Reversal of portal hypertension and hyperdynamic splanchnic circulation by combined vascular endothelial growth factor and platelet-derived growth factor blockade in rats.

Author

Fernandez M, Mejias M, Garcia-Pras E, Mendez R, Garcia-Pagan JC, and Bosch J

Subjects
Animals, Benzamides, Disease Models, Animal, Drug Therapy, Combination, Hypertension, Portal drug therapy, Hypertension, Portal metabolism, Imatinib Mesylate, Immunosuppressive Agents therapeutic use, Ligation, Male, Mesenteric Artery, Superior physiopathology, Neovascularization, Pathologic drug therapy, Piperazines therapeutic use, Platelet-Derived Growth Factor metabolism, Portal Vein physiopathology, Protein Kinase Inhibitors therapeutic use, Pyrimidines therapeutic use, Rats, Rats, Sprague-Dawley, Regional Blood Flow physiology, Signal Transduction physiology, Sirolimus therapeutic use, Vascular Endothelial Growth Factor A metabolism, Hypertension, Portal physiopathology, Neovascularization, Pathologic metabolism, Platelet-Derived Growth Factor antagonists & inhibitors, Splanchnic Circulation physiology, Vascular Endothelial Growth Factor A antagonists & inhibitors
Abstract

Unlabelled: Vascular endothelial growth factor (VEGF) and platelet-derived growth factor (PDGF) pathways are crucial to angiogenesis, a process that contributes significantly to the pathogenesis of portal hypertension. This study determined the effects of inhibition of VEGF and/or PDGF signaling on hyperdynamic splanchnic circulation and portosystemic collateralization in rats with completely established portal hypertension, thus mimicking the situation in patients. Portal vein-ligated rats were treated with rapamycin (VEGF signaling inhibitor), Gleevec (PDGF signaling inhibitor), or both simultaneously when portal hypertension was already fully developed. Hemodynamic studies were performed by transit-time flowmetry. The extent of portosystemic collaterals was measured by radioactive microspheres. The expression of angiogenesis mediators was determined by Western blotting and immunohistochemistry. Combined inhibition of VEGF and PDGF signaling significantly reduced splanchnic neovascularization (i.e., CD31 and VEGFR-2 expression) and pericyte coverage of neovessels (that is, alpha-smooth muscle actin and PDGFR-beta expression) and translated into hemodynamic effects as marked as a 40% decrease in portal pressure, a 30% decrease in superior mesenteric artery blood flow, and a 63% increase in superior mesenteric artery resistance, yielding a significant reversal of the hemodynamic changes provoked by portal hypertension in rats. Portosystemic collateralization was reduced as well., Conclusions: Our results provide new insights into how angiogenesis regulates portal hypertension by demonstrating that the maintenance of increased portal pressure, hyperkinetic circulation, splanchnic neovascularization, and portosystemic collateralization is regulated by VEGF and PDGF in portal hypertensive rats. Importantly, these findings also suggest that an extended antiangiogenic strategy (that is, targeting VEGF/endothelium and PDGF/pericytes) may be a novel approach to the treatment of portal hypertension.

Published
2007
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results