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Repurposing anthelmintic agents to eradicate resistant leukemia

机译:重新调整抗牙本质以根除抗性白血病

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Despite rapid progress in genomic profiling in acute lymphoblastic leukemia (ALL), identification of actionable targets and prediction of response to drugs remains challenging. To identify specific vulnerabilities in ALL, we performed a drug screen using primary human ALL samples cultured in a model of the bone marrow microenvironment combined with high content image analysis. Among the 2487 FDA-approved compounds tested, anthelmintic agents of the class of macrocyclic lactones exhibited potent anti-leukemia activity, similar to the already known anti-leukemia agents currently used in induction chemotherapy. Ex vivo validation in 55 primary ALL samples of both precursor B cell and T-ALL including refractory relapse cases confirmed strong anti-leukemia activity with IC50 values in the low micromolar range. Anthelmintic agents increased intracellular chloride levels in primary leukemia cells, inducing mitochondrial outer membrane depolarization and cell death. Supporting the notion that simultaneously targeting cell death machineries at different angles may enhance the cell death response, combination of anthelmintic agents with the BCL-2 antagonist navitoclax or with the chemotherapeutic agent dexamethasone showed synergistic activity in primary ALL. These data reveal anti-leukemia activity of anthelmintic agents and support exploiting drug repurposing strategies to identify so far unrecognized anti-cancer agents with potential to eradicate even refractory leukemia.
机译:尽管在急性淋巴细胞白血病(全部)中的基因组分析中进行了快速进展,但鉴定了可行的目标和对药物的反应预测仍然具有挑战性。为了鉴定所有特定的漏洞,我们使用在骨髓微环境模型中培养的初级人类所有样品进行药物筛网,与高含量的图像分析相结合。在测试的2487个批准的FDA批准的化合物中,宏环内酯类的尖锐剂表现出效力的抗白血病活性,类似于目前用于诱导化疗的已知的抗白血病药剂。在55项中的所有样品中验证前体B细胞和T-all的所有样品包括耐火复发案件,确认了低微摩尔范围内的IC 50值强的抗白血病活性。 Anthelmintic代理在原发性白血病细胞中增加细胞内氯化物水平,诱导线粒体外膜去极化和细胞死亡。支持在不同角度同时靶向细胞死亡机械的观念可以增强细胞死亡反应,使得具有Bcl-2拮抗剂Navitoclax或与化学治疗剂地塞米松的化学治疗剂的组合在原代中显示出协同活性。这些数据揭示了抗白血病患者的抗白血病活性,并支持剥削毒品重新训练策略,以鉴定迄今为止无法识别的抗癌剂,潜在的潜在甚至难治性白血病。

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