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埃布罗替尼治疗胃溃疡愈合过程中胃黏膜表皮生长因子和血小板衍生生长因子受体的表达

Gastric mucosal EGF and PDGF receptor expression with ulcer healing by ebrotidine.

作者信息

Slomiany B L, Piotrowski J, Czajkowski A, Yotsumoto F, Slomiany A

机构信息

Research Center, University of Medicine and Dentistry of New Jersey, Newark.

出版信息

Am J Gastroenterol. 1994 Jun;89(6):894-7.

PMID:8198101
Abstract

OBJECTIVES

Epidermal growth factor (EGF) and platelet-derived growth factor (PDGF) play important roles in the process of mucosal repair and restitution, and their biological effects are mediated by receptors located on the target cell surfaces. The purpose of this study was to assess the effect of the antiulcer agent, ebrotidine, on the expression of EGF and PDGF receptors with chronic ulcer healing.

METHODS

Chronic gastric ulcers were developed in the rat by acetic acid technique. The animal were divided into two groups and were treated twice daily for 14 consecutive days, either with ebrotidine at 100 mg/kg, or placebo. At different stages of treatment, the animals were sacrificed and used for the isolation and quantification of gastric mucosal EGF and PDGF receptors.

RESULTS

The binding assays revealed that ulcer healing was accompanied by an increase in mucosal expression of both types of receptors. A 1.7-1.8-fold increase in PDGF and EGF receptors occurred by the 4th day after the development of ulcer and reached a maximum of 3-fold increase by the 14th day, when the ulcer was essentially healed. Treatment with ebrotidine caused accelerated ulcer healing (7 days) which was accompanied by a significant enhancement in receptor expression. Compared to the controls, a 1.5-fold increase in EGF and 1.7-fold increase in PDGF receptor expression occurred by the 7th day of ebrotidine treatment, and a 1.4- to 1.5-fold increase was still observed at the 14th day of treatment.

CONCLUSIONS

The results suggest that ebrotidine is capable of enhancement of gastric mucosal proliferative activities associated with ulcer healing through the stimulation of EGF and PDGF receptor expression.

摘要

目的

表皮生长因子(EGF)和血小板衍生生长因子(PDGF)在黏膜修复和再生过程中发挥重要作用,它们的生物学效应由位于靶细胞表面的受体介导。本研究旨在评估抗溃疡药物依罗替丁对慢性溃疡愈合过程中EGF和PDGF受体表达的影响。

方法

采用醋酸法在大鼠身上制备慢性胃溃疡。将动物分为两组,连续14天每天给药两次,一组给予100mg/kg依罗替丁,另一组给予安慰剂。在治疗的不同阶段,处死动物,用于分离和定量胃黏膜EGF和PDGF受体。

结果

结合试验显示,溃疡愈合伴随着两种受体在黏膜表达的增加。溃疡形成后第4天,PDGF和EGF受体表达增加1.7 - 1.8倍,到溃疡基本愈合的第14天,增加至最多3倍。依罗替丁治疗使溃疡加速愈合(7天),同时受体表达显著增强。与对照组相比,依罗替丁治疗第7天,EGF受体表达增加1.5倍,PDGF受体表达增加1.7倍,治疗第14天仍观察到增加1.4 - 1.5倍。

结论

结果表明,依罗替丁能够通过刺激EGF和PDGF受体表达,增强与溃疡愈合相关的胃黏膜增殖活性。

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