用多西他赛或TRAIL抑制CIB1可增强三阴性乳腺癌细胞的死亡。
CIB1 depletion with docetaxel or TRAIL enhances triple-negative breast cancer cell death.
作者信息
Chung Alexander H, Leisner Tina M, Dardis Gabrielle J, Bivins Marissa M, Keller Alana L, Parise Leslie V
机构信息
1Department of Pharmacology, University of North Carolina at Chapel Hill, CB #7365, Chapel Hill, NC 27599 USA.
2Department of Biochemistry and Biophysics, University of North Carolina at Chapel Hill, CB #7260, Chapel Hill, NC 27599 USA.
出版信息
Cancer Cell Int. 2019 Feb 4;19:26. doi: 10.1186/s12935-019-0740-2. eCollection 2019.
BACKGROUND
Patients diagnosed with triple negative breast cancer (TNBC) have limited treatment options and often suffer from resistance and toxicity due to chemotherapy. We previously found that depleting calcium and integrin-binding protein 1 (CIB1) induces cell death selectively in TNBC cells, while sparing normal cells. Therefore, we asked whether CIB1 depletion further enhances tumor-specific killing when combined with either the commonly used chemotherapeutic, docetaxel, or the cell death-inducing ligand, TRAIL.
METHODS
We targeted CIB1 by RNA interference in MDA-MB-436, MDA-MB-231, MDA-MB-468, docetaxel-resistant MDA-MB-436 TNBC cells and ME16C normal breast epithelial cells alone or combination with docetaxel or TRAIL. Cell death was quantified via trypan blue exclusion using flow cytometry and cell death mechanisms were analyzed by Western blotting. Cell surface levels of TRAIL receptors were measured by flow cytometry analysis.
RESULTS
CIB1 depletion combined with docetaxel significantly enhanced tumor-specific cell death relative to each treatment alone. The enhanced cell death strongly correlated with caspase-8 activation, a hallmark of death receptor-mediated apoptosis. The death receptor TRAIL-R2 was upregulated in response to CIB1 depletion, which sensitized TNBC cells to the ligand TRAIL, resulting in a synergistic increase in cell death. In addition to death receptor-mediated apoptosis, both combination treatments activated a non-apoptotic mechanism, called paraptosis. Interestingly, these combination treatments also induced nearly complete death of docetaxel-resistant MDA-MB-436 cells, again via apoptosis and paraptosis. In contrast, neither combination treatment induced cell death in normal ME16C cells.
CONCLUSION
Novel combinations of CIB1 depletion with docetaxel or TRAIL selectively enhance naive and docetaxel-resistant TNBC cell death while sparing normal cell. Therefore, combination therapies that target CIB1 could prove to be a safe and durable strategy for treatment of TNBC and potentially other cancers.
背景
被诊断为三阴性乳腺癌(TNBC)的患者治疗选择有限,且常常因化疗而产生耐药性和毒性。我们之前发现,耗尽钙整合素结合蛋白1(CIB1)可在TNBC细胞中选择性地诱导细胞死亡,而对正常细胞无影响。因此,我们探讨了与常用化疗药物多西他赛或细胞死亡诱导配体TRAIL联合使用时,耗尽CIB1是否能进一步增强肿瘤特异性杀伤作用。
方法
我们通过RNA干扰单独或与多西他赛或TRAIL联合靶向MDA-MB-436、MDA-MB-231、MDA-MB-468、多西他赛耐药的MDA-MB-436 TNBC细胞以及ME16C正常乳腺上皮细胞中的CIB1。通过流式细胞术使用台盼蓝排斥法对细胞死亡进行定量,并通过蛋白质印迹分析细胞死亡机制。通过流式细胞术分析测量TRAIL受体的细胞表面水平。
结果
与单独的每种治疗相比,耗尽CIB1与多西他赛联合使用显著增强了肿瘤特异性细胞死亡。增强的细胞死亡与半胱天冬酶-8激活密切相关,这是死亡受体介导的细胞凋亡的标志。死亡受体TRAIL-R2在耗尽CIB1后上调,这使TNBC细胞对配体TRAIL敏感,导致细胞死亡协同增加。除了死亡受体介导的细胞凋亡外,两种联合治疗均激活了一种称为副凋亡的非凋亡机制。有趣的是,这些联合治疗同样通过凋亡和副凋亡诱导多西他赛耐药的MDA-MB-436细胞几乎完全死亡。相比之下,两种联合治疗均未在正常ME16C细胞中诱导细胞死亡。
结论
耗尽CIB1与多西他赛或TRAIL的新型联合疗法可选择性增强幼稚和多西他赛耐药的TNBC细胞死亡,同时不影响正常细胞。因此,靶向CIB1的联合疗法可能是治疗TNBC以及潜在其他癌症的安全且持久的策略。
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