替西罗莫司
肺癌
癌症研究
PI3K/AKT/mTOR通路
人口
医学
内科学
肿瘤科
药理学
mTOR抑制剂的发现与发展
生物
细胞凋亡
生物化学
环境卫生
作者
Toshiaki Ohara,Munenori Takaoka,Shinichi Toyooka,Yasuko Tomono,Toshio Nishikawa,Yasuhiro Shirakawa,Tomoki Yamatsuji,Noriaki Tanaka,Toshiyoshi Fujiwara,Yoshio Naomoto
出处
期刊:Cancer Science
[Wiley]
日期:2011-04-26
卷期号:102 (7): 1344-1349
被引量:32
标识
DOI:10.1111/j.1349-7006.2011.01967.x
摘要
Temsirolimus (CCI‐779), a recently synthesized analogue of rapamycin, specifically inhibits mTOR and has been approved for clinical use in renal cell carcinoma. Recent reports have indicated the growth inhibitory effect of temsirolimus in some cancers including non‐small‐cell lung carcinoma (NSCLC). In this study, we aimed to explore the potential therapeutic use of temsirolimus as a treatment for NSCLC. Using cultured NSCLC cells (A549, H1299, and H358), we determined the effect of temsirolimus on cell proliferation and its antitumor effects on subcutaneous tumors, as well as its contribution to the survival of mice having pleural dissemination of cancer cells, mimicking advanced NSCLC. Temsirolimus suppressed proliferation of NSCLC cells in a dose‐dependent manner, with an IC 50 of <1 nM. Western blot analysis revealed that temsirolimus treatment specifically inhibited the phosphorylation of mTOR and its downstream effectors in 1 h, accompanied by an increased cell population in the G 0 /G 1 phase, but according to flow cytometry, the cell population did not increase in the sub‐G 0 phase. When NSCLC subcutaneous tumor‐bearing mice were treated with temsirolimus, tumor volume was significantly reduced (tumor volume on day 35: vehicle vs temsirolimus = 1239 vs 698 cm 3 ; P < 0.05). Furthermore, prolonged survival was observed in pleural disseminated tumor‐bearing mice with temsirolimus treatment (median survival: vehicle vs temsirolimus = 53.5 vs 72.5 days; P < 0.05). These results suggest that temsirolimus could be useful for NSCLC treatment, due to its antiproliferative effect, and could be a potential treatment for advanced NSCLC, giving prolonged survival. ( Cancer Sci 2011; 102: 1344–1349)
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