1993
DOI: 10.1016/0952-3278(93)90086-c
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Prostaglandin and portal hypertension

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Cited by 14 publications
(5 citation statements)
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“…Hence, there is a specific increase in adrenoceptor-linked PGI2 synthesis in portal hypertensive animals, which may contribute to arterial vasodilation in this experimental PVL model. Agonist-stimulated PGI2 production, in general, may be enhanced because several studies have demonstrated that vasopressor-induced changes in splanchnic blood flow in portal hypertensives and cirrhotics are enhanced after inhibition of COX activity with indomethacin [97][98][99][100][101]. Furthermore, evidence for a role of agonist-induced PGI2 release in PHT also is derived from studies on the beneficial effects of long-term TNF-␣ inhibition on systemic hemodynamics in PHT.…”
Section: Cyclooxygenase-dependent Aa Metabolitesmentioning
confidence: 95%
“…Hence, there is a specific increase in adrenoceptor-linked PGI2 synthesis in portal hypertensive animals, which may contribute to arterial vasodilation in this experimental PVL model. Agonist-stimulated PGI2 production, in general, may be enhanced because several studies have demonstrated that vasopressor-induced changes in splanchnic blood flow in portal hypertensives and cirrhotics are enhanced after inhibition of COX activity with indomethacin [97][98][99][100][101]. Furthermore, evidence for a role of agonist-induced PGI2 release in PHT also is derived from studies on the beneficial effects of long-term TNF-␣ inhibition on systemic hemodynamics in PHT.…”
Section: Cyclooxygenase-dependent Aa Metabolitesmentioning
confidence: 95%
“…This circulatory change is caused by a variety of vasoactive factors, such as cytokines, prostacyclins, and nitric oxide [14][15][16][17][18] . Infection or bleeding, which are frequent complications in cirrhotic patients, increase the nitric oxide production and result in aggravation of the hyperdynamic circulation [19] .…”
Section: Introductionmentioning
confidence: 99%
“…The activation of contractile elements in the fat-storing cells may play a particular role. These cells are controlled by numerous regulatory systems, including those for glucagon, nitric ox-ide, endothelin, cytokines and prostaglandins (11,(38)(39)(40)(41)(42). It is important to note that recent experiments have indicated that splanchnic and hepatic nitric oxide synthase activity is decreased in experimental cirrhosis, and that transfection of the nitric oxide synthase gene reduces portal pressure substantially (43,44).…”
Section: Hepatosplanchnic Circulation In Cirrhosismentioning
confidence: 99%