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内皮抑素通过改变P物质水平增强乳腺癌细胞的放射反应。

Endostatin enhances radioresponse in breast cancer cells via alteration of substance P levels.

作者信息

Arslan Aydemir Esra, Simsek Oz Ece, Fidan Korcum Aylin, Fiskin Kayahan

机构信息

Department of Biology, Art and Science Faculty, Akdeniz University, 07058 Antalya, Turkey.

出版信息

Oncol Lett. 2011 Sep 1;2(5):879-886. doi: 10.3892/ol.2011.335. Epub 2011 Jul 4.

Abstract

Radiotherapy is widely used in the treatment of cancer. On the other hand, endostatin is considered to be a potent inhibitor of angiogenesis. Therefore, to test whether ES combined with RT overcomes the limitations of each monotherapy the present study investigated the effects of endostatin (ES), radiotherapy (RT) or combination therapy on the growth of mouse breast cancer cells as well as on the expression of substance P in vitro. The breast cancer cell lines 4T1 and 4THMpc were treated with recombinant murine ES (0.5, 1, 2, 4 and 8 µg/ml) alone, RT (45 Gy) alone or as a combination therapy. Cell proliferation was evaluated using an MTS assay and the results were verified by the Live/Dead assay. Immunoprecipitation and Western blotting analysis were performed to determine whether the substance P levels of the two cell lines occurred due to substance P content. Results showed that ES alone resulted in a low but significant inhibition in the growth of 4T1 and 4THMpc cell lines (27.63 and 21.75%, respectively). RT alone inhibited the growth of 4T1 (30.81%) and 4THMpc (39.64%) cells. A combination of ES with RT enhanced growth inhibition in the cells (83% in 4T1 and 80% in 4THMpc). The amount of substance P, both in the conditioned media and the cell lysates, increased within 72 h after RT. This increase was inhibited when ES and RT were applied in combination. These data indicate that ES inhibits the in vitro growth of breast cancer cells and potentiates the anti-tumor effects of RT at appropriate doses via alteration of the amount of substance P and thus an increase of radioresponse.

摘要

放射疗法在癌症治疗中被广泛应用。另一方面,内皮抑素被认为是一种有效的血管生成抑制剂。因此,为了测试内皮抑素(ES)联合放疗是否能克服每种单一疗法的局限性,本研究调查了内皮抑素(ES)、放射疗法(RT)或联合疗法对小鼠乳腺癌细胞生长以及体外P物质表达的影响。乳腺癌细胞系4T1和4THMpc分别单独用重组鼠ES(0.5、1、2、4和8μg/ml)、单独用RT(45 Gy)或作为联合疗法进行处理。使用MTS试验评估细胞增殖,并通过活/死试验验证结果。进行免疫沉淀和蛋白质印迹分析以确定两种细胞系中P物质水平是否因P物质含量而产生。结果表明,单独使用ES对4T1和4THMpc细胞系的生长有低但显著的抑制作用(分别为27.63%和21.75%)。单独使用RT抑制了4T1(30.81%)和4THMpc(39.64%)细胞的生长。ES与RT联合增强了对细胞生长的抑制作用(4T1中为83%,4THMpc中为80%)。RT后72小时内,条件培养基和细胞裂解物中的P物质含量均增加。当ES和RT联合应用时,这种增加受到抑制。这些数据表明,ES抑制乳腺癌细胞的体外生长,并通过改变P物质的量从而增加放射反应性,在适当剂量下增强RT的抗肿瘤作用。

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