Luo Ming, Shen Na, Shang Li, Fang Zeng, Xin Ying, Ma Yuxi, Du Min, Yuan Yuan, Hu Chenchen, Tang Yun, Huang Jing, Wei Wei, Lee Myung Ryul, Hergenrother Paul J, Wicha Max S
Department of Breast and Thyroid Surgery, Peking University Shenzhen Hospital, Shenzhen, China.
Division of Hematology and Oncology, Department of Internal Medicine, University of Michigan, Ann Arbor, Michigan.
Cancer Res. 2024 Dec 16;84(24):4264-4282. doi: 10.1158/0008-5472.CAN-24-0800.
Triple-negative breast cancer (TNBC) contains the highest proportion of cancer stem-like cells (CSC), which display intrinsic resistance to currently available cancer therapies. This therapeutic resistance is partially mediated by an antioxidant defense coordinated by the transcription factor NRF2 and its downstream targets that include NAD(P)H quinone oxidoreductase 1 (NQO1). In this study, we identified the antioxidant enzymes NQO1 and superoxide dismutase 1 (SOD1) as therapeutic vulnerabilities of ALDH+ epithelial-like CSCs and CD24-/loCD44+/hi mesenchymal-like CSCs in TNBC. Effective targeting of these CSC states was achieved by using isobutyl-deoxynyboquinone (IB-DNQ), a potent and specific NQO1-bioactivatable futile redox cycling molecule, which generated large amounts of reactive oxygen species including superoxide and hydrogen peroxide. Furthermore, the CSC killing effect was specifically enhanced by genetic or pharmacologic inhibition of SOD1, a copper-containing superoxide dismutase highly expressed in TNBC. Mechanistically, a significant portion of NQO1 resides in the mitochondrial intermembrane space, catalyzing futile redox cycling from IB-DNQ to generate high levels of mitochondrial superoxide, and SOD1 inhibition markedly potentiated this effect, resulting in mitochondrial oxidative injury, cytochrome c release, and activation of the caspase-3-mediated apoptotic pathway. Treatment with IB-DNQ alone or together with SOD1 inhibition effectively suppressed tumor growth, metastasis, and tumor-initiating potential in xenograft models of TNBC expressing different levels of NQO1. This futile oxidant-generating strategy, which targets CSCs across the epithelial-mesenchymal continuum, could be a promising therapeutic approach for treating patients with TNBC. Significance: Combining NQO1-bioactivatable futile oxidant generators with SOD1 inhibition eliminates breast cancer stem cells, providing a therapeutic strategy that may have wide applicability, as NQO1 and SOD1 are overexpressed in several cancers.
三阴性乳腺癌(TNBC)含有比例最高的癌症干细胞样细胞(CSC),这些细胞对目前可用的癌症治疗表现出内在抗性。这种治疗抗性部分由转录因子NRF2及其下游靶点(包括NAD(P)H醌氧化还原酶1(NQO1))协调的抗氧化防御介导。在本研究中,我们确定抗氧化酶NQO1和超氧化物歧化酶1(SOD1)是TNBC中ALDH+上皮样CSC和CD24-/loCD44+/hi间充质样CSC的治疗脆弱点。通过使用异丁基脱氧奈醌(IB-DNQ)实现了对这些CSC状态的有效靶向,IB-DNQ是一种强效且特异性的NQO1可生物激活的无效氧化还原循环分子,它能产生大量活性氧,包括超氧化物和过氧化氢。此外,通过对SOD1进行基因或药理学抑制可特异性增强CSC杀伤效果,SOD1是一种在TNBC中高度表达的含铜超氧化物歧化酶。从机制上讲,相当一部分NQO1存在于线粒体外膜间隙,催化从IB-DNQ开始的无效氧化还原循环以产生高水平的线粒体超氧化物,而SOD1抑制显著增强了这种效应,导致线粒体氧化损伤、细胞色素c释放以及caspase-3介导的凋亡途径激活。单独使用IB-DNQ或与SOD1抑制联合治疗可有效抑制表达不同水平NQO1的TNBC异种移植模型中的肿瘤生长、转移和肿瘤起始潜能。这种针对上皮-间充质连续体中CSC的无效氧化剂生成策略可能是治疗TNBC患者的一种有前景的治疗方法。意义:将NQO1可生物激活的无效氧化剂生成剂与SOD1抑制相结合可消除乳腺癌干细胞,提供一种可能具有广泛适用性的治疗策略,因为NQO1和SOD1在多种癌症中均过表达。
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