Mild increases in portal pressure upregulate vascular endothelial growth factor and endothelial nitric oxide synthase in the intestinal microcirculatory bed, leading to a hyperdynamic state

Abraldes, Juan G.; Iwakiri, Yasuko; Loureiro-Silva, Maurício R.; Haq, Omar; Sessa, William C.; Groszmann, Roberto J.

doi:10.1152/ajpgi.00336.2005

Cited by 190 publications

(155 citation statements)

References 43 publications

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“…Though the reduction in peripheral resistance is slow, compensatory mechanisms play a pivotal role in maintaining and further worsening the hyperdynamic circulation ( Fig. 1) [12][13][14][15][16]. Plasma volume expansion is relevant in these cirrhotic patients, even if distribution between the central and peripheral vascular areas is often not balanced [6,17].…”

Section: Hemodynamic Changes Contributing To Hyperdynamic Syndromementioning

confidence: 99%

Clinical implications of the hyperdynamic syndrome in cirrhosis

Licata

Mazzola

Ingrassia

et al. 2014

European Journal of Internal Medicine

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The hyperdynamic syndrome is a late consequence of portal hypertension in cirrhosis. The principal hemodynamic manifestations of the hyperdynamic syndrome are high cardiac output, and increased heart rate and total blood volume, accompanied by reduced total systemic vascular resistance. Pathophysiology involves a complex of humoral and neural mechanisms that can determine hemodynamic changes, and lead to hyperdynamic circulation. In this review we focus our attention on the manifestations of the hyperdynamic syndrome. Some of these are well described and directly related to portal hypertension (varices, ascites, hepatic encephalopathy, and hepatorenal syndrome), while others, such as hepatopulmonary syndrome, portopulmonary hypertension, and cirrhotic cardiomyopathy, are less known as clinical manifestations related to cirrhosis and, therefore, merit further investigation.

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Section: Hemodynamic Changes Contributing To Hyperdynamic Syndromementioning

confidence: 99%

Clinical implications of the hyperdynamic syndrome in cirrhosis

Licata

Mazzola

Ingrassia

et al. 2014

European Journal of Internal Medicine

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“…26 NO appears to be the primary vasodilator in the arterial vasodilatation and the hyperdynamic circulatory state of liver cirrhosis. Degree of portal hypertension correlates with eNOS activation in the splanchnic circulation, in an animal model of portal hypertension 27 and is initiated by physical stimuli that induce Akt-dependent eNOS activation as well as through increased production of VEGF. [27][28][29] Thus, portal pressure itself, may be an important factor that regulates vasodilatation in the splanchnic arterial circulation by means of eNOS activation in the splanchnic circulation.…”

Section: New Concepts In the Vascular Biology Of Cirrhosis And Portalmentioning

confidence: 99%

“…Degree of portal hypertension correlates with eNOS activation in the splanchnic circulation, in an animal model of portal hypertension 27 and is initiated by physical stimuli that induce Akt-dependent eNOS activation as well as through increased production of VEGF. [27][28][29] Thus, portal pressure itself, may be an important factor that regulates vasodilatation in the splanchnic arterial circulation by means of eNOS activation in the splanchnic circulation. 27 The formation of portosystemic collateral vessels and gastroesophageal varices are another important feature of portal hypertension that result in esophageal variceal hemorrhage.…”

Section: New Concepts In the Vascular Biology Of Cirrhosis And Portalmentioning

confidence: 99%

“…[27][28][29] Thus, portal pressure itself, may be an important factor that regulates vasodilatation in the splanchnic arterial circulation by means of eNOS activation in the splanchnic circulation. 27 The formation of portosystemic collateral vessels and gastroesophageal varices are another important feature of portal hypertension that result in esophageal variceal hemorrhage. Recent studies have focused on the potential role of angiogenic factors in the formation of portosystemic collateral vessels in portal hypertension as well as therapeutic implications of antiangiogenic therapies.…”

Section: New Concepts In the Vascular Biology Of Cirrhosis And Portalmentioning

confidence: 99%

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Vascular biology and pathobiology of the liver: Report of a single-topic symposium

2008

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Portal hypertension and its complications account for the majority of morbidity and mortality that occurs in patients with cirrhosis. In addition to portal hypertension, a number of other vascular syndromes are also of great importance, especially the ischemia-reperfusion (IR) injury. With the identification of major vascular defects that could account for many of the clinical sequelae of these syndromes, the liver vasculature field has now integrated very closely with the broader vascular biology discipline. In that spirit, the Vascular Cell Signaling Mediated by NO. Endothelial cells (ECs) produce NO through the enzyme endothelial NO synthase (eNOS). NO then regulates important vascular functions, such as vascular tone, angiogenesis, and arterial remodeling. 1 eNOS is regulated in a multiprotein complex (Fig. 1), which includes the activating kinase, Akt1 and putative negative regulator caveolin-1 (Cav-1). Although eNOS Ϫ/Ϫ mice evidence impaired angiogenesis, overexpression of a constitutively active allele of eNOS that mimics the phosphorylated and active state rescues these angiogenic defects. 2 Because eNOS is an EC-specific Akt substrate, ECs from mice lacking the Akt1 isoform also have defects in eNOS phosphorylation, NO production, and angiogenesis which are correspondingly rescued by Akt1 overexpression. 3 One key mechanism by which the Akt-eNOS axis promotes angiogenesis in vivo is through mobilization of endothelial progenitor cells and EC migration to sites of vascular injury. In contradistinction to AKT, Cav-1 is a negative regulator of eNOS. Mice deficient in Cav-1 have defective mechanotransduction, calcium signaling, prostacyclin production, and elevated NO production indicating that endothelial Cav-1 also importantly regulates vascular function by regulating eNOS and other signaling pathways. 4 Upon its generation in ECs, NO also acts on adjacent vascular effector cells to modulate vascular tone, cellular proliferation, apoptosis, migration, and synthesis of extracellular matrix (Fig. 2). NO acts in part by stimulating soluble guanylate cyclase (sGC) to produce intracellular Abbreviations: Cav-

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“…El ON media los efectos endoteliales del VEGF, facilitando la proliferación de cé-lulas endoteliales y la migración, y también estimula la liberación de progenitores de células endoteliales de la mé-dula ósea, contribuyendo a la vasculogénesis (46). Por su parte, el VEGF promueve la producción de ON e induce la expresión de la eONS (47); experimentalmente se ha demostrado que un aumento leve de la presión portal estimula la producción de VEGF en la microcirculación yeyunal, y esta señal es suficiente para inducir la actividad de la eONS (48). Este conjunto de datos indica que tanto la eONS como el VEGF son dianas potenciales para modular la formación de colaterales portosistémicas (varices) en la hipertensión portal.…”

Section: Fisiopatología De La Hipertensión Portal En La Cirrosisunclassified

Profilaxis preprimaria de la hemorragia por varices

González-Alonso

Gómez

Martínez

2007

Rev. esp. enferm. dig.

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INTRODUCCIÓNLas varices esofágicas son una manifestación clínica de la hipertensión portal, cuya causa más frecuente en nuestro medio es la cirrosis. La hemorragia digestiva alta por rotura de varices esofágicas es su complicación más grave, con una mortalidad elevada y una reducción de la supervivencia del 50% al año (1). El tratamiento actual de la hipertensión portal consiste en identificar a los pacientes que presentan varices, para administrar fármacos que al reducir la presión portal, también disminuyan la presión y la tensión variceal y con ello el riesgo de rotura y hemorragia. Otra estrategia que se ha planteado es identificar a los enfermos con presión portal elevada, pero que aún no han desarrollado varices, con objeto de tratarlos con fármacos reductores de la presión portal y así evitar que las varices lleguen a formarse. Este artículo describe las bases fisiopatológicas en las que se fundamenta REV ESP ENFERM DIG (Madrid) Vol. 99. N.°12, pp. 714-721, 2007 Correspondencia: Agustín Albillos Martínez. Servicio de Gastroenterología. Hospital Universitario Ramón y Cajal. Ctra. de Colmenar km 9,600. 28034 Madrid: e-mail: aalbillosm@meditex.es 2007; 99: 714-721. González-Alonso R, Garrido Gómez E, Albillos Martínez A. Profilaxis preprimaria de la hemorragia por varices. Rev Esp Enferm Dig RESUMENLa formación de colaterales portosistémicas, en especial en la unión esofagogástrica, es una de las consecuencias más graves de la hipertensión portal. El aumento de la presión portal es la fuerza más importante que dirige la formación de varices esofagogástri-cas, siendo necesario para que esto ocurra que la presión portal (estimada por el gradiente de presión venosa hepática) alcance un valor mínimo de 10 mmHg. Posteriormente, la hiperemia esplác-nica también contribuye al desarrollo de las varices. Las colaterales portosistémicas se forman por repermeabilización de vasos preexistentes, remodelado vascular y angiogénesis. El objetivo de la profilaxis preprimaria es evitar o retrasar la formación de varices esofagogástricas. En modelos experimentales de hipertensión portal, la administración precoz de vasoconstrictores esplácnicos como los beta-bloqueantes, de inhibidores de la síntesis de óxido nítrico o de sustancias anti-angiogénicas, inhibe la formación de colaterales portosistémicas. Sin embargo, los ensayos clínicos con beta-bloqueantes realizados en pacientes con cirrosis sin varices con objeto de retrasar su formación no han alcanzado los resultados esperados.Palabras clave: Hipertensión portal. Varices esofágicas. Hemorragia digestiva alta. Profilaxis. Cirrosis hepática. ABSTRACTPortosystemic collateral formation, particularly at the gastroesophageal junction, is a most serious consequence of portal hypertension. Increased portal pressure is the most significant force underlying gastroesophageal variceal formation, to which end portal pressure (estimated from the hepatic venous pressure gradient) must reach at least 10 mmHg. Subsequently, splanchnic hyperemia also contributes to variceal development. ...

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Mild increases in portal pressure upregulate vascular endothelial growth factor and endothelial nitric oxide synthase in the intestinal microcirculatory bed, leading to a hyperdynamic state

Cited by 190 publications

References 43 publications

Clinical implications of the hyperdynamic syndrome in cirrhosis

Clinical implications of the hyperdynamic syndrome in cirrhosis

Vascular biology and pathobiology of the liver: Report of a single-topic symposium

Profilaxis preprimaria de la hemorragia por varices

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