Protection of estrogen in portal hypertension gastropathy: an experimental model

Morgan-Martins, María Isabel; Jacques, Simone Iahnig; Hartmann, Renata Minuzzo; Marques, Camila Moraes; Marroni, Cláudio Augusto; Marroni, Norma Possa

doi:10.1590/s0004-28032011000300011

Cited by 10 publications

(14 citation statements)

References 35 publications

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“…Moreover, it can provide measurements in the portal circulation [29] that cannot be performed accurately in humans because of ethical and technical limitations [30]. In the current study, portal pressure in the PPVL group was significantly increased in comparison with the control group.…”

Section: Discussionmentioning

confidence: 57%

“…PPVL is an experimental model used in rats to study the histopathological mechanisms involved in prehepatic PHT with a maintained liver integrity and a hyperdynamic circulation that develops in a short and predicted period 1 week after induction [29]. Moreover, it can provide measurements in the portal circulation [29] that cannot be performed accurately in humans because of ethical and technical limitations [30].…”

Section: Discussionmentioning

confidence: 99%

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Effect of experimentally induced portal hypertension on the fundic mucosa of adult male albino rats and the possible protective role of quercetin supplementation

El-Haleem¹,

Soliman²,

Motteleb

2013

The Egyptian Journal of Histology

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Portal hypertension (PHT) is a hyperdynamic circulation disorder. Its precise effect on the fundic mucosa remains a matter of controversy . Aim of studyEvaluation of the effect of long -term experimental induction of PHT on the rat fundic mucosa and the possible protective role of quercetin. Materials and methodsForty rats were divided into the following three main groups; control, partial portal vein ligation (PPVL) and PPVL receiving 50 mg/kg /day of quercetin given intraperitoneal. After ten weeks from PPVL induction, samples from fundus of stomach were prepared for light and electron microscope. Tissue and blood samples were examined for inflammatory, oxidative stress and antioxidant markers. The number of parietal cells, area % of collagen fibers, PAS -alcian blue reaction, nitrotyrosine-and caspase-3 positive reaction were measured morphometrically and statistically analyzed. ResultsFundic mucosa of PPVL group showed loss of normal architecture, exfoliation of the surface epithelium, inflammatory cellular infiltration and congestion of blood vessels in lamina propria. Parietal cells showed dilatation of their intracellular canaliculi. Many mucous cells had apoptotic nuclei. Chief cells had few secretory granules and dilated RER. Statistically, there was significant increase in the area% of collagen fibers, nitrotyrosine, caspase-3 and inflammatory markers while area% of PAS-alcian blue reaction, number of parietal cells and tissue antioxidant enzymes showed significant reduction comparing with the control. Quercetin markedly protect fundic mucosa from histological and biochemical deleterious effects of PHT. Conclusion PHT exerts a deleterious histological and biochemical effects on the fundic mucosa. Both antioxidant and antiinflammatory effects of Quercetin offer degree of protection for fundic mucosa, therefore, it may protect from gastropathy resulted from PHT.Specimens from the fundus of the stomach were fixed in 10% buffered formalin overnight at a temperature of 4°C. Tissue samples were dehydrated in alcohol, cleared in xylol, and embedded in paraffin. Tissue sections (5 µm thickness) were stained with H&E stain [25], Periodic Acid Schieff -Alcian Blue stain (PAS-AB stain) [26], and Mallory's trichrome stain [26].Immunohistochemical study [27] Immunohistochemical studies were carried out using the peroxidase-labeled Streptavidin-Biotin Technique. Paraffin sections were deparaffinized and rehydrated

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Section: Discussionmentioning

confidence: 57%

Section: Discussionmentioning

confidence: 99%

Effect of experimentally induced portal hypertension on the fundic mucosa of adult male albino rats and the possible protective role of quercetin supplementation

El-Haleem¹,

Soliman²,

Motteleb

2013

The Egyptian Journal of Histology

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“…Experimental studies have shown that E 2 reduced portal pressure and increased hepatic blood flow in castrated and cirrhotic model rats, but the effect was significantly inhibited by ICI-182780 [62,81]. E 2 played a protective role by acting as an antioxidant, because the hemodynamic changes involved in PHT led to increased ROS, which triggered oxidative stress [82].…”

Section: Role Of Estrogens In the Improvement Of Portal Hypertension mentioning

confidence: 99%

“…E 2 played a protective role by acting as an antioxidant, because the hemodynamic changes involved in PHT led to increased ROS, which triggered oxidative stress [82]. In castrated rats, a significant increase in the activity of antioxidant enzymes and lipid peroxidase was observed, which might occur to compensate for the absence of circulating E 2 , promoted by castration, but even then it was not effective in reducing lipid peroxidase [81,83,84]. Estrogen replacement could reverse this effect, reverting to the values of the control animals [84].…”

Section: Role Of Estrogens In the Improvement Of Portal Hypertension mentioning

confidence: 99%

Estrogen derivatives

Zhang

Wu²

2013

European Journal of Gastroenterology & Hepatology

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Sex differences in the incidence of liver cirrhosis and portal hypertension have been reported by epidemiological studies. Previous studies have indicated that estrogen therapy improved hepatic fibrosis, inhibited the activation of hepatic stellate cells, and reduced portal pressure, whereas the administration of exogenous estrogens resulted in some potential risks, limiting their clinical use. However, the biological actions of estrogens are mediated by three subtypes of estrogen receptors (ERs): ERα, ERβ, and G-protein-coupled ER. These ER subtypes act in distinct ways and exert different biological effects that mediate genomic and nongenomic events, resulting in tissue-specific responses. In addition, active estrogen metabolites, with little or no affinity for ERs, could mediate the fibrosuppressive effect of estrogens through an ER-independent pathway. Taken together, such specific estrogen derivatives as ER selective agonists, or active estrogen metabolites, would provide novel therapeutic opportunities, stratifying this hormonal treatment, thereby reducing undesired side-effects in the treatment of liver cirrhosis and portal hypertension.

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“…In the portal hypertension dilation of the splanchnic veins occurs, and collateral circulation is developed. This situation may happen with diseases in pre, intra or post-hepatics stages 10 . Thrombosis of the portal vein or splenic vein triggers pre-hepatic portal hypertension.…”

Section: Introductionmentioning

confidence: 99%

Constriction rate variation produced by partial ligation of the portal vein at pre-hepatic portal hypertension induced in rats

Rodrigues¹,

Silva²,

Serigiolle³

et al. 2014

ABCD, arq. bras. cir. dig.

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BackgroundPartial portal vein ligation causes an increase in portal pressure that remains stable even after the appearance of collateral circulation, with functional adaptation to prolonged decrease in portal blood flow.AimTo assess whether different constriction rates produced by partial ligation of the vein interfere with the results of this experimental model in rats.MethodsThree groups of five rats each were used; in group 1 (sham-operated), dissection and measurement of portal vein diameters were performed. Portal hypertension was induced by partial portal vein ligation, reducing its size to 0.9 mm in the remaining 10 animals, regardless of the initial diameter of the veins. Five animals with portal hypertension (group 2) underwent reoperation after 15 days and the rats in group 3 after 30 days. The calculation of the constriction rate was performed using a specific mathematical formula (1 - π r 2 / π R2) x 100% and the statistical analysis with the Student t test.ResultsThe initial diameter of the animal's portal vein was 2.06 mm, with an average constriction rate of the 55.88%; although the diameter of the veins and the constriction rate in group 2 were lower than in group 3 (2.06 mm - 55,25% and 2.08 mm - 56.51%, respectively), portal hypertension was induced in all rats and no significant macroscopic differences were found between the animals that were reoperated after 15 days and after 30 days respectively, being the shorter period considered enough for the evaluation. Comparing the initial diameter of the vein and the rate of constriction performed in groups 2 and 3, no statistic significance was found (p>0.05).ConclusionPre-hepatic portal hypertension in rat can be induced by the reduction of the portal vein diameter to 0.9 mm, regardless the initial diameter of the vein and the vessel constriction rate.

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Protection of estrogen in portal hypertension gastropathy: an experimental model

Cited by 10 publications

References 35 publications

Effect of experimentally induced portal hypertension on the fundic mucosa of adult male albino rats and the possible protective role of quercetin supplementation

Effect of experimentally induced portal hypertension on the fundic mucosa of adult male albino rats and the possible protective role of quercetin supplementation

Estrogen derivatives

Constriction rate variation produced by partial ligation of the portal vein at pre-hepatic portal hypertension induced in rats

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