首页> 外文期刊>Stem cells translational medicine. >Simvastatin radiosensitizes differentiated and stem-like breast cancer cell lines and is associated with improved local control in inflammatory breast cancer patients treated with postmastectomy radiation
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Simvastatin radiosensitizes differentiated and stem-like breast cancer cell lines and is associated with improved local control in inflammatory breast cancer patients treated with postmastectomy radiation

机译:辛伐他汀对敏化的分化和干细胞样乳腺癌细胞系具有放射敏感性,并与接受乳房切除术后放疗的炎性乳腺癌患者改善局部控制有关

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Reported rates of local failure after adjuvant radiation for women with inflammatory breast cancer (IBC) and triple-negative non-IBC are higher than those of women with receptor-expressing non-IBC. These high rates of locoregional recurrence are potentially influenced by the contribution of radioresistant cancer stem cells to these cancers. Statins have been shown to target stem cells and improve disease-free survival among IBC patients. We examined simvastatin radiosensitization of multiple subtypes of breast cancer cell lines in vitro in monolayer and mammosphere-based clonogenic assays and examined the therapeutic benefit of statin use on local control after postmastectomy radiation (PMRT) among IBC patients. We found that simvastatin radiosensitizes mammosphere-initiating cells (MICs) of IBC cell lines (MDA-IBC3, SUM149, SUM190) and of the metaplastic, non-IBC triple-negative receptor cell line (SUM159). However, simvastatin radioprotects MICs of non-IBC cell lines MCF-7 and SKBR3. In a retrospective clinical study of 519 IBC patients treated with PMRT, 53 patients used a statin. On univariate analysis, actuarial 3-year local recurrence-free survival (LRFS) was higher among statin users, and on multivariate analysis, triple negative breast cancer, absence of lymphatic invasion, neoadjuvant pathological tumor response to preoperative chemotherapy, and statin use were independently associated with higher LRFS. In conclusion, patients with IBC and triple-negative non-IBC breast cancer have the highest rates of local failure, and there are no available known radiosensitizers. We report significant improvement in local control after PMRT among statin users with IBC and significant radiosensitization across triple-negative and IBC cell lines of multiple subtypes using simvastatin. These data suggest that simvastatin should be justified as a radiosensitizing agent by a prospective clinical trial.
机译:炎症性乳腺癌(IBC)和三阴性非IBC妇女的辅助放射治疗后局部失败的报道率高于表达受体的非IBC妇女。这些高局部复发率可能受辐射抗癌干细胞对这些癌症的贡献的影响。他汀类药物已被证明可靶向干细胞并改善IBC患者的无病生存期。我们在单层和基于乳球的克隆形成试验中,体外研究了多种亚型乳腺癌细胞系的辛伐他汀放射增敏作用,并研究了IBC患者在乳房切除术后放疗(PMRT)后使用他汀类药物对局部控制的治疗益处。我们发现辛伐他汀对IBC细胞系(MDA-IBC3,SUM149,SUM190)和化生性非IBC三阴性受体细胞系(SUM159)的乳球起始细胞(MIC)致敏。但是,辛伐他汀可以保护非IBC细胞系MCF-7和SKBR3的MIC。在对519名接受PMRT治疗的IBC患者的回顾性临床研究中,有53名患者使用他汀类药物。在单因素分析中,他汀类药物使用者的精算3年局部无复发生存率(LRFS)较高;在多变量分析中,三阴性乳腺癌,无淋巴管浸润,术前化疗对新辅助病理肿瘤的反应以及他汀类药物的使用是独立的与较高的LRFS相关。总之,IBC和三阴性非IBC乳腺癌患者的局部失败率最高,并且没有可用的已知放射增敏剂。我们报告了他汀类药物使用者与IBC之间PMRT后PMRT的局部控制的显着改善,以及使用辛伐他汀的多种亚型的三阴性和IBC细胞系之间的显着放射增敏作用。这些数据表明,前瞻性临床试验应证明辛伐他汀可以作为放射增敏剂。

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