Effect of mTOR Signal Transduction Pathway on Proliferation of HumanEndometrial Carcinoma Cells Ishikawa

DENG Shou-heng; SHI Jian-guo; KE Xian-zhu; CHEN Ping; LI Fang; SHI Xiao-yan

doi:CNKI:11-3495/R.20110407.1323.005

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Effect of mTOR Signal Transduction Pathway on Proliferation of HumanEndometrial Carcinoma Cells Ishikawa

更新时间：2024-01-04

- Effect of mTOR Signal Transduction Pathway on Proliferation of HumanEndometrial Carcinoma Cells Ishikawa
- Chinese Journal of Experimental Traditional Medical Formulae Vol. 17, Issue 12, Pages: 223-226(2011)
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- DOI：CNKI:11-3495/R.20110407.1323.005
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- Published：2011
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DENG Shou-heng, SHI Jian-guo, KE Xian-zhu, et al. Effect of mTOR Signal Transduction Pathway on Proliferation of HumanEndometrial Carcinoma Cells Ishikawa [J]. Chinese journal of experimental traditional medical formulae, 2011, 17(12): 223-226.
DOI：

DENG Shou-heng, SHI Jian-guo, KE Xian-zhu, et al. Effect of mTOR Signal Transduction Pathway on Proliferation of HumanEndometrial Carcinoma Cells Ishikawa [J]. Chinese journal of experimental traditional medical formulae, 2011, 17(12): 223-226. DOI： CNKI:11-3495/R.20110407.1323.005.

摘要

目的: 观察经抑制剂作用后人子宫内膜癌细胞株ishikawa细胞生长和mTOR信号通路的变化

了解子宫内膜癌的发病机制。方法: MTT法和细胞克隆形成法检测抑制剂对细胞增殖的影响;RT-PCR和Western blot法从mRNA和蛋白质水平分别检测mTOR mRNA和下游磷酸化靶蛋白S6K1和STAT3表达。结果: 雷帕霉素(rapamycin

RA)与酪氨酸磷酸化抑制剂(RG-14260

RG)可抑制ishikawa细胞增殖、降低其存活率

二者联合呈协同效应(P<0.01);ishikawa细胞中存在mTOR mRNA和下游磷酸化靶蛋白S6K1和STAT3高表达

经RA单独或联合RG作用后

各指标均下降

且二者合用效果更明显(P<0.01)。结论: mTOR信号通路参与了子宫内膜癌的形成和发展。

Abstract

Objective: To observe the change of the growth and mTOR signal transduction pathway after treatment with inhibitor in human endometrial carcinoma cell ishikawa in vitro.To provide an experimental foundation of the research on the pathogenesis of human endometrial carcinomas. Method: MTT and Clone formation test were used to determine the proliferative effects of two inhibitors on tumor cells.The mRNA levels of mTOR

the downstream phosporylated substrate S6K1 and STAT3 protein were assayed by RT-PCR and Western blot

respectively. Result: Rapamycin alone or combined with RG-14260 could inhibite cell proliferation and lower survival rate of ishikawa cells.The effect of rapamycin combinated with RG-14260was better than that of RG-14260 and rapamycin alone.There were high expression of mTOR mRNA and downstream phosporylated substrate S6K1 and STAT3 protein in ishikawa cells.But these index above were decreased after treatment with inhibitor. The effect of Rapamycin combinated with RG-14260 was more obvious than that of Rapamycin alone. Conclusion: mTOR signal transduction pathway play an important role in the formation and progress of endometrial carcinoma cells.

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