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依溴替丁和硫糖铝治疗胃溃疡愈合过程中的细胞周期进程

Cell cycle progression during gastric ulcer healing by ebrotidine and sucralfate.

作者信息

Slomiany B L, Piotrowski J, Slomiany A

机构信息

Research Center, University of Medicine and Dentistry of New Jersey, Newark 07103-2400, USA.

出版信息

Gen Pharmacol. 1997 Sep;29(3):367-70. doi: 10.1016/s0306-3623(96)00472-7.

DOI:10.1016/s0306-3623(96)00472-7
PMID:9378241
Abstract
  1. The effect of antiulcer agents, ebrotidine and sucralfate, on the expression of gastric mucosal proliferating cell nuclear antigen (PCNA) and cyclin-dependent kinase (p34Cdk2) during chronic ulcer healing was examined. 2. Rats with experimentally induced gastric ulcers were treated twice daily for 14 days with either ebrotidine at 100 mg/kg, sucralfate at 100 mg/kg or vehicle, and at different stages of treatment their stomachs were used for quantitization of gastric mucosal PCNA and Cdk2 expression. 3. The assays revealed that the ulcer healing was accompanied by a marked elevation in mucosal expression of PCNA and Cdk2. The maximum increase in PCNA (4.7-fold) occurred by the second day of healing, and the expression of Cdk2 reached a maximum increase (2.3-fold) by the fourth day. 4. Accelerated ulcer healing with ebrotidine (7 days) and sucralfate (8 days) treatments was reflected in a significant enhancement of PCNA and Cdk2 expression. By the second day of treatment, ebrotidine evoked a 15-fold increase in PCNA expression, and sucralfate produced an 11.8-fold enhancement. The mucosal expression of Cdk2 attained a maximum of 4.3-fold increase over that of the controls by the sixth day of healing with ebrotidine, and a fivefold increase in Cdk2 expression occurred by the fourth day of ulcer treatment with sucralfate. 5. The findings implicate cell cycle regulatory proteins in the processes to leading to mucosal repair and suggest that the two drugs exert a similar effect on the expression of proteins that control cell cycle progression.
摘要
  1. 研究了抗溃疡药物依罗替丁和硫糖铝在慢性溃疡愈合过程中对胃黏膜增殖细胞核抗原(PCNA)和细胞周期蛋白依赖性激酶(p34Cdk2)表达的影响。2. 用实验方法诱导胃溃疡的大鼠,每天接受两次治疗,持续14天,治疗药物分别为100mg/kg的依罗替丁、100mg/kg的硫糖铝或赋形剂,在治疗的不同阶段,取它们的胃来定量检测胃黏膜PCNA和Cdk2的表达。3. 检测显示,溃疡愈合伴随着黏膜PCNA和Cdk2表达的显著升高。PCNA的最大增幅(4.7倍)出现在愈合的第二天,Cdk2的表达在第四天达到最大增幅(2.3倍)。4. 依罗替丁(7天)和硫糖铝(8天)治疗加速了溃疡愈合,这表现为PCNA和Cdk2表达的显著增强。在治疗的第二天,依罗替丁使PCNA表达增加了15倍,硫糖铝使PCNA表达增强了11.8倍。在用依罗替丁治疗愈合的第六天,黏膜Cdk2的表达比对照组最多增加了4.3倍,在用硫糖铝治疗溃疡的第四天,Cdk2表达增加了5倍。5. 这些发现表明细胞周期调节蛋白参与了导致黏膜修复的过程,并提示这两种药物对控制细胞周期进程的蛋白质表达具有相似的作用。

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