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Identification of Selective Inhibitors of Cancer Stem Cells by High-Throughput Screening

机译:通过高通量筛选鉴定癌症干细胞的选择性抑制剂

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Screens for agents that specifically kill epithelial cancer stem cells (CSCs) have not been possible due to the rarity of these cells within tumor cell populations and their relative instability in culture. We describe here an approach to screening for agents with epithelial CSC-specific toxicity. We implemented this method in a chemical screen and discovered compounds showing selective toxicity for breast CSCs. One compound, salinomycin, reduces the proportion of CSCs by > 100-fold relative to paclitaxel, a commonly used breast cancer chemotherapeutic drug. Treatment of mice with salinomycin inhibits mammary tumor growth in vivo and induces increased epithelial differentiation of tumor cells. In addition, global gene expression analyses show that salinomycin treatment results in the loss of expression of breast CSC genes previously identified by analyses of breast tissues isolated directly from patients. This study demonstrates the ability to identify agents with specific toxicity for epithelial CSCs.
机译:由于这些细胞在肿瘤细胞群体中的稀有性及其在培养中的相对不稳定性,因此无法筛选特异性杀死上皮癌干细胞(CSC)的药物。我们在这里描述了一种筛选具有上皮CSC特异性毒性的药物的方法。我们在化学筛选中实施了该方法,并发现了对乳腺CSC具有选择性毒性的化合物。相对于紫杉醇(一种常用的乳腺癌化疗药物),一种化合物沙利霉素可将CSC的比例降低100倍以上。用沙利霉素治疗小鼠在体内抑制乳腺肿瘤生长并诱导肿瘤细胞上皮分化增加。此外,全球基因表达分析表明,盐霉素治疗导致先前通过直接从患者体内分离出的乳房组织进行分析而鉴定出的乳腺CSC基因的表达丧失。这项研究证明了鉴定对上皮CSC具有特定毒性的药物的能力。

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