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联合使用血红蛋白和葡萄糖氧化酶的芬顿和饥饿疗法。

Combined Fenton and starvation therapies using hemoglobin and glucose oxidase.

机构信息

Polymer Science Group, Department of Chemical Engineering, The University of Melbourne, Parkville, VIC 3010, Australia.

出版信息

Nanoscale. 2019 Mar 21;11(12):5705-5716. doi: 10.1039/c8nr09107b.

DOI:10.1039/c8nr09107b
PMID:30865742
Abstract

Separately, Fenton and starvation cancer therapies have been recently reported as impressive methods for tumor destruction. Here, we introduce natural hemoglobin and glucose oxidase (GOx) for efficient cancer treatment following combined Fenton and starvation therapies. GOx and hemoglobin were encapsulated in zeolitic imidazolate frameworks 8 (ZIF-8) to fabricate a pH-sensitive MOF activated by tumor acidity. In the slightly acidic environment of cancer cells, GOx is released and it consumes d-glucose and molecular oxygen, nutrients essential for the survival of cancer cells, and produces gluconic acid and hydrogen peroxide, respectively. The produced gluconic acid increases the acidity of the tumor microenvironment leading to complete MOF destruction and enhances hemoglobin and GOx release. The Fe ions from the heme groups of hemoglobin also release in the presence of both endogenous and produced H2O2 and generate hydroxyl radicals. The produced OH˙ radical can rapidly oxidize the surrounding biomacromolecules in the biological system and treat the cancer cells. In vitro experiments demonstrate that this novel nanoparticle is cytotoxic to cancer cells HeLa and MCF-7, at very low concentrations (<2 μg mL-1). In addition, the selectivity index values are 5.52 and 11.04 for HeLa and MCF-7 cells, respectively, which are much higher than those of commercial drugs and those of similar studies reported by other research groups. This work thus demonstrates a novel pH-sensitive system containing hemoglobin and GOx for effective and selective cancer treatment using both radical generation and nutrient starvation.

摘要

芬顿疗法和饥饿疗法最近被报道为肿瘤破坏的有效方法。在这里,我们介绍了天然血红蛋白和葡萄糖氧化酶(GOx),用于联合芬顿和饥饿疗法进行有效的癌症治疗。GOx 和血红蛋白被包裹在沸石咪唑酯骨架 8(ZIF-8)中,以制造一种可被肿瘤酸度激活的 pH 敏感的 MOF。在癌细胞的微酸性环境中,GOx 被释放出来,它消耗 d-葡萄糖和分子氧,这是癌细胞生存所必需的营养物质,并分别产生葡萄糖酸和过氧化氢。产生的葡萄糖酸增加了肿瘤微环境的酸度,导致完全的 MOF 破坏,并增强了血红蛋白和 GOx 的释放。血红蛋白的血红素基团中的 Fe 离子也在内外源产生的 H2O2 的存在下释放,并产生羟基自由基。产生的 OH˙自由基可以在生物系统中迅速氧化周围的生物大分子,并治疗癌细胞。体外实验表明,这种新型纳米颗粒对癌细胞 HeLa 和 MCF-7 具有细胞毒性,浓度非常低(<2 μg mL-1)。此外,HeLa 和 MCF-7 细胞的选择性指数值分别为 5.52 和 11.04,远高于商业药物和其他研究小组报道的类似研究的选择性指数值。因此,这项工作展示了一种新型的 pH 敏感系统,该系统包含血红蛋白和 GOx,用于通过自由基生成和营养饥饿进行有效和选择性的癌症治疗。

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