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首页> 外文期刊>Scientific reports. >An anticancer Os(II) bathophenanthroline complex as a human breast cancer stem cell-selective, mammosphere potent agent that kills cells by necroptosis
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An anticancer Os(II) bathophenanthroline complex as a human breast cancer stem cell-selective, mammosphere potent agent that kills cells by necroptosis

机译:作为人乳腺癌干细胞选择性,乳腺椎间工间有效剂的抗癌OS(II)洗浴膜络合物杀死细胞

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Conventional chemotherapy is mostly effective in the treatment of rapidly-dividing differentiated tumor cells but has limited application toward eliminating cancer stem cell (CSC) population. The presence of a very small number of CSCs may contribute to the development of therapeutic resistance, metastases, and relapse. Thus, treatment failure by developing novel anticancer drugs capable of effective targeting of CSCs is at present a major challenge for research focused on chemotherapy of cancer. Here, we show that Os(II) complex 2 [Os(ηsup6/sup-pcym)(bphen)(dca)]PFsub6/sub (pcym?=?p-cymene, bphen?=?bathophenanthroline, and dca?=?dichloroacetate), is capable of efficient and selective killing CSCs in heterogeneous populations of human breast cancer cells MCF-7 and SKBR-3. Notably, its remarkable submicromolar potency to kill CSCs is considerably higher than that of its Ru analog, [Ru(ηsup6/sup-pcym)(bphen)(dca)]PFsub6/sub (complex 1) and salinomycin, one of the most selective CSC-targeting compounds hitherto identified. Furthermore, Os(II) complex 2 reduces the formation, size, and viability of three-dimensional mammospheres which more closely reflect the tumor microenvironment than cells in traditional two-dimensional cultures. The antiproliferation studies and propidium iodide staining using flow cytometry suggest that Os(II) complex 2 induces human breast cancer stem cell death predominantly by necroptosis, a programmed form of necrosis. The results of this study demonstrate the promise of Os(II) complex 2 in treating human breast tumors. They also represent the foundation for further preclinical and clinical studies and applications of Os(II) complex 2 to comply with the emergent need for human breast CSCs-specific chemotherapeutics capable to treat chemotherapy-resistant and relapsed human breast tumors.
机译:常规化疗主要有效地治疗快速分化的分化肿瘤细胞,但在消除癌症干细胞(CSC)群体的应用有限。非常少数CSC的存在可能导致治疗抵抗,转移和复发的发展。因此,通过开发能够有效靶向CSCs的新型抗癌药物的治疗失败目前对重点进行了研究的主要挑战,重点是癌症的化疗。在这里,我们表明OS(ii)复杂2 [OS(η 6 -pcym)(bphen)(dca)] pf 6 (pcym?=Δp-cymene ,Bphen?=α=?洗涤酚和DCA?=β-二氯乙酸酯),能够有效和选择性地杀死人乳腺癌细胞MCF-7和SKBR-3的异质群中的CSC。值得注意的是,其杀灭CSC的显着亚微粒溶胀性远高于其Ru模拟,[Ru(η 6 -pccom)(bphen)(dca)] pf 6 (络合物1)和蝾螈,迄今鉴定的最选择性的CSC靶向化合物之一。此外,OS(II)复合物2减少了三维辐射体的形成,尺寸和活力,其比传统的二维培养物中的细胞更紧密地反映肿瘤微环境。使用流式细胞术的抗溶解研究和碘化丙啶染色表明OS(II)复合物2主要通过虐鼠,一种编程的坏死形式诱导人乳腺癌干细胞死亡。该研究的结果证明了OS(II)复合物2治疗人乳腺肿瘤的承诺。他们还代表了OS(II)复合物2的进一步临床前和临床研究和应用的基础,符合人乳腺CSCS特异性化学治疗能够治疗抗化疗和复发的人乳腺肿瘤的必需品。

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