Weakness of mucosal barrier in portal hypertensive gastropathy of alcoholic cirrhosis. Effects of propranolol and enprostil

被引:28
作者
Payen, JL
Cales, P
Pienkowski, P
Sozzani, P
Kervran, A
Frexinos, J
Pascal, JP
机构
[1] CHU ANGERS,SERV HEPATOGASTROENTEROL,F-49033 ANGERS 01,FRANCE
[2] CHU PURPAN,SERV HEPATOGASTROENTEROL,TOULOUSE,FRANCE
[3] CHU RANGUEIL,SERV HEPATOGASTROENTEROL,F-31054 TOULOUSE,FRANCE
[4] CHU RANGUEIL,INSERM U151,F-31054 TOULOUSE,FRANCE
[5] CNRS,INSERM U376,CTR PHARMACOL ENDOCRINOL,MONTPELLIER,FRANCE
关键词
aspirin; cirrhosis; gastrin; gastrotoxicity; glucagon; PGE2; portal hypertension; portal hypertensive gastropathy; potential difference; stomach;
D O I
10.1016/0168-8278(95)80035-2
中图分类号
R57 [消化系及腹部疾病];
学科分类号
摘要
Background/Aims: It has been suggested that the vulnerability of gastric mucosa is increased in patients with cirrhosis as a result of a PGE2 deficiency. Therefore, we evaluated whether PGE2 mucosal generation, and gastric potential difference - a reflection of the gastric mucosal barrier - were correlated to endoscopic features and whether these alterations could be alleviated. Methods: The potential difference was measured before (basal) and after a stimulation test by aspirin. The serum levels of gastrin and glucagon were also determined. Finally, the effects of a 1-week administration of propranolol or enprostil were tested on potential difference. The endoscopic grade of portal hypertensive gastropathy was assessed according to McCormack et al. The results are presented respectively for controls, patients with mild gastropathy, and patients with severe gastropathy. Comparisons were made using variance or covariance analysis after adjustment with age. Results: Basal potential difference was significantly different between the three groups: -30.6, -28.8, -24.9 mV, p<0.05, respectively. The effects of aspirin administration on potential difference parameters were significantly different between the three groups (irritability index: 35+/-25, 92+/-98, 114+/-74 mv(2) . min, p<0.05, respectively) when non-responders to aspirin were excluded. PGE2 mucosal generation was significantly increased in both the antrum (9.8, 19.5, 19.7 ng/mg proteins, p<0.05, respectively) and in the corpus (8.1, 14.0, 20.2 ng/mg proteins, p<0.05, respectively). PGE2 generation was not related to potential difference. Glucagon serum levels were related to the grade of gastropathy. A 1-week administration of 160 mg/d long-acting propranolol, 35 mu g/d enprostil or placebo did not significantly modify basal potential difference. Conclusions: Portal hypertensive gastropathy is characterized by a decreased potential difference proportional to the endoscopic severity. The gastric mucosa of patients with cirrhosis seems to be more susceptible to aspirin than that of healthy subjects. It appears that the role of PGE2 is controversial in portal hypertensive gastropathy. Propranolol and enprostil do not improve this decreased potential difference.
引用
收藏
页码:689 / 696
页数:8
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