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Oncolytic Reovirus Effectively Targets Breast Cancer Stem Cells

机译:溶瘤性呼肠孤病毒有效靶向乳腺癌干细胞

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摘要

Recent evidence suggests that cancer stem cells (CSCs) play an important role in cancer, as these cells possess enhanced tumor-forming capabilities and are resistant to current anticancer therapies. Hence, novel cancer therapies will need to be tested for both tumor regression and CSC targeting. Herein we show that oncolytic reovirus that induces regression of human breast cancer primary tumor samples xenografted in immunocompromised mice also effectively targets and kills CSCs in these tumors. CSCs were identified based on CD24CD44+ cell surface expression and overexpression of aldehyde dehydrogenase. Upon reovirus treatment, the CSC population was reduced at the same rate as non-CSCs within the tumor. Immunofluorescence of breast tumor tissue samples from the reovirus- and mock-treated mice confirmed that both CSCs and non-CSCs were infectible by reovirus, and terminal deoxynucleotidyl transferase biotin-dUTP nick end labeling (TUNEL) assay showed that both populations died by apoptosis. Ras, which has been shown to mediate reovirus oncolysis, was found to be present at similar levels in all cell types, and this is consistent with their comparable sensitivity to reovirus. These experiments indicate that oncolytic reovirus has the potential to induce tumor regression in breast cancer patients. More important, the CSC population was equally reduced and was as susceptible to reovirus treatment as the non-CSC population.
机译:最近的证据表明,癌症干细胞(CSC)在癌症中起着重要作用,因为这些细胞具有增强的肿瘤形成能力,并且对目前的抗癌疗法有抵抗力。因此,需要针对肿瘤消退和CSC靶向测试新的癌症疗法。本文中,我们显示溶瘤呼肠孤病毒可诱导人乳腺癌原代肿瘤样品在免疫功能低下小鼠体内异种移植的消退,也可有效靶向并杀死这些肿瘤中的CSC。根据CD24 - CD44 + 细胞表面表达和醛脱氢酶过表达来鉴定CSC。在呼肠孤病毒治疗后,CSC群体的减少速度与肿瘤内非CSC的减少速度相同。来自呼肠孤病毒和模拟治疗小鼠的乳腺肿瘤组织样品的免疫荧光证实,呼肠孤病毒可感染CSC和非CSC,并且末端脱氧核苷酸转移酶生物素-dUTP缺口末端标记(TUNEL)检测表明两个种群均因凋亡而死亡。已经发现,Ras介导了呼肠孤病毒的溶瘤作用,在所有细胞类型中均以相似的水平存在,这与它们对呼肠孤病毒的可比敏感性相一致。这些实验表明溶瘤呼肠孤病毒有可能在乳腺癌患者中诱导肿瘤消退。更重要的是,与非CSC人群一样,CSC人群也同样减少,并且容易受到呼肠孤病毒治疗。

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