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Combination therapy targeting both cancer stem-like cells and bulk tumor cells for improved efficacy of breast cancer treatment

机译:针对癌症干细胞样和块状肿瘤细胞的联合疗法可提高乳腺癌治疗的疗效

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Many types of tumors are organized in a hierarchy of heterogeneous cell populations. The cancer stem-like cells (CSCs) hypothesis suggests that tumor development and metastasis are driven by a minority population of cells, which are responsible for tumor initiation, growth and recurrences. The inability to efficiently eliminate CSCs during chemotherapy, together with CSCs being highly tumorigenic and invasive, may result in treatment failure due to cancer relapse and metastases. CSCs are emerging as a promising target for the development of translational cancer therapies. Ideal panacea for cancer would kill all malignant cells, including CSCs and bulk tumor cells. Since both chemotherapy and CSCs-specific therapy are insufficient to cure cancer, we propose combination therapy with CSCs-targeted agents and chemotherapeutics for improved breast cancer treatment. We generated in vitro mammosphere of 2 breast cancer cell lines, and demonstrated ability of mammospheres to grow and enrich cancer cells with stem-like properties, including self-renewal, multilineage differentiation and enrichment of cells expressing breast cancer stem-like cell biomarkers CD44(+)/CD24(-/low). The formation of mammospheres was significantly inhibited by salinomycin, validating its pharmacological role against the cancer stem-like cells. In contrast, paclitaxel showed a minimal effect on the proliferation and growth of breast cancer stem-like cells. While combination therapies of salinomycin with conventional chemotherapy (paclitaxel or lipodox) showed a potential to improve tumor cell killing, different subtypes of breast cancer cells showed different patterns in response to the combination therapies. While optimization of combination therapy is warranted, the design of combination therapy should consider phenotypic attributes of breast cancer types.
机译:许多类型的肿瘤组织在异质细胞群体的层次结构中。癌干样细胞(CSC)假说表明,肿瘤的发展和转移是由少数细胞驱动的,这些细胞负责肿瘤的发生,生长和复发。化疗期间无法有效消除CSC,以及CSC具有高度致瘤性和侵袭性,可能由于癌症复发和转移而导致治疗失败。 CSC正在成为发展转化癌症疗法的有希望的目标。理想的灵丹妙药可以杀死所有恶性细胞,包括CSC和大量肿瘤细胞。由于化学疗法和CSCs特异性疗法均不足以治愈癌症,因此我们建议将CSCs靶向药物与化学疗法联合治疗以改善乳腺癌的治疗。我们产生了2个乳腺癌细胞系的体外乳房球,并证明了乳房球能够生长和富集具有干样特性的癌细胞,包括自我更新,多系分化和富集表达乳腺癌干样细胞生物标记CD44( +)/ CD24(-/低)。沙利霉素可显着抑制乳球的形成,从而证实其对癌症干细胞样细胞的药理作用。相反,紫杉醇对乳腺癌干细胞样细胞的增殖和生长影响很小。沙利霉素与常规化学疗法(紫杉醇或lipodox)的联合疗法显示出改善肿瘤细胞杀伤力的潜力,而不同亚型的乳腺癌细胞对联合疗法的反应则不同。尽管有必要优化联合疗法,但联合疗法的设计应考虑乳腺癌类型的表型属性。

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