Wu Junyong, Hao Xinyan, Qi Lin, Xu Wenjie, Yin Chi, Tang Yucheng, Sun Pengcheng, Liao Dehua, Hu Xiongbin, Tang Tiantian, Tu Chao, Xiang Daxiong, Li Zhihong
Department of Pharmacy, The Second Xiangya Hospital Central South University Changsha 410011, China; Institute of Clinical Pharmacy, Central South University Changsha 410011, China; Department of Orthopedics, The Second Xiangya Hospital, Central South University, Changsha, China; Hunan Key Laboratory of Tumor Models and Individualized Medicine, The Second Xiangya Hospital, Changsha, China.
Department of Pharmacy, The Second Xiangya Hospital Central South University Changsha 410011, China; Institute of Clinical Pharmacy, Central South University Changsha 410011, China.
Acta Biomater. 2025 Jan 24;193:348-361. doi: 10.1016/j.actbio.2024.12.049. Epub 2024 Dec 20.
Osteosarcoma tissues demonstrated elevated expression of proteins (FDX1 and DLAT) integral to cuproptosis in our preliminary study, indicating the potential effectiveness of anti-tumor strategies predicated on this process. Nevertheless, the overexpression of copper export proteins and the challenge of copper ion penetration may contribute to insufficient local copper ion concentration for inducing cuproptosis. Herein, we engineered a biomimetic copper-elesclomol-polyphenol network for the efficient delivery of copper ions and the copper ionophore elesclomol. Simultaneously, we integrated catalase (CAT) to alleviate tumor hypoxia, thereby inducing a greater reliance of tumor cells on aerobic respiration and enhancing cuproptosis sensitivity. In vitro analyses revealed that the nanocomplex exhibited potent cytotoxicity and displayed hallmark characteristics of cuproptosis. In vivo trials further validated targeted tumor accumulation, resulting in the suppression of tumor growth and lung metastasis. An augmentation in the proportion of activated immune cells in both tumor and draining lymph nodes was observed. The improvement of immunosuppressive microenvironment facilitated a synergistic antitumor effect with cuproptosis. The therapeutic efficacy was further evidenced in two osteosarcoma models, highlighting the potential as a safe and effective strategy against osteosarcoma and lung metastasis. STATEMENT OF SIGNIFICANCE: Osteosarcoma tissues exhibit a marked increase in the expression of proteins FDX1 and DLAT, which are crucial for cuproptosis. Moreover, cells that depend on mitochondrial respiration are more susceptible to cuproptosis. Here we developed a biomimetic copper-based nanocomplex to trigger cuproptosis against osteosarcoma and lung metastases. The nanocomplex demonstrated excellent biocompatibility and tumor targeting. Catalase incorporating facilitated oxygen generation within tumor microenvironment and alleviated hypoxia, thereby inducing a greater reliance of tumor cells on aerobic respiration and enhancing cuproptosis sensitivity. Simultaneously, the released Cu-elesclomol complexes induced proteotoxic stress responses and efficiently elicited cuproptosis, leading to increased release of proinflammatory factors and triggering anti-tumor immune activation. Our strategy holds promise for osteosarcoma treatment by inducing cuproptosis and achieving potent tumor suppression.
在我们的初步研究中,骨肉瘤组织显示出与铜死亡相关的蛋白质(FDX1和DLAT)表达升高,这表明基于该过程的抗肿瘤策略具有潜在有效性。然而,铜输出蛋白的过表达以及铜离子渗透的挑战可能导致局部铜离子浓度不足以诱导铜死亡。在此,我们构建了一种仿生铜-依斯氯胺酮-多酚网络,用于高效递送铜离子和铜离子载体依斯氯胺酮。同时,我们整合了过氧化氢酶(CAT)以缓解肿瘤缺氧,从而使肿瘤细胞对有氧呼吸产生更大的依赖性并增强铜死亡敏感性。体外分析表明,该纳米复合物表现出强大的细胞毒性,并呈现出铜死亡的标志性特征。体内试验进一步验证了其对肿瘤的靶向积累,从而抑制肿瘤生长和肺转移。在肿瘤和引流淋巴结中均观察到活化免疫细胞比例的增加。免疫抑制微环境的改善促进了与铜死亡的协同抗肿瘤作用。在两种骨肉瘤模型中进一步证明了治疗效果,突出了其作为一种安全有效的抗骨肉瘤和肺转移策略的潜力。
骨肉瘤组织中对铜死亡至关重要的蛋白质FDX1和DLAT的表达显著增加。此外,依赖线粒体呼吸的细胞对铜死亡更敏感。在此,我们开发了一种仿生铜基纳米复合物来触发针对骨肉瘤和肺转移的铜死亡。该纳米复合物表现出优异的生物相容性和肿瘤靶向性。掺入过氧化氢酶促进了肿瘤微环境中的氧气生成并缓解了缺氧,从而使肿瘤细胞对有氧呼吸产生更大的依赖性并增强铜死亡敏感性。同时,释放的铜-依斯氯胺酮复合物诱导蛋白质毒性应激反应并有效引发铜死亡,导致促炎因子释放增加并触发抗肿瘤免疫激活。我们的策略通过诱导铜死亡和实现有效的肿瘤抑制,有望用于骨肉瘤治疗。
