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层次化的微-介-宏观多孔 MOF 纳米系统用于局域跨尺度双生物分子加载和客体载体协同抗癌治疗。

Hierarchically Micro-, Meso-, and Macro-Porous MOF Nanosystems for Localized Cross-Scale Dual-Biomolecule Loading and Guest-Carrier Cooperative Anticancer Therapy.

机构信息

Key Laboratory of Food Nutrition and Functional Food of Hainan Province, School of Food Science and Engineering, Hainan University, Haikou 570228, PR China.

School of Materials Science and Engineering, Hainan University, Haikou 570228, PR China.

出版信息

ACS Nano. 2024 Aug 20;18(33):21911-21924. doi: 10.1021/acsnano.4c02288. Epub 2024 Aug 5.

DOI:10.1021/acsnano.4c02288
PMID:39102565
Abstract

Mass transfer of bulky molecules, ., bioenzymes, particularly for cross-scale multibiomolecules, imposes serious challenges for microporous metal-organic frameworks (MOFs). Here, we create a hierarchically porous MOF heterostructure featuring highly region-ordered micro-, meso-, and macro-pores by growing a microporous ZIF-8 shell onto a hollow Prussian blue core through an epitaxial growth strategy. This allows for localized loading of large bioenzyme glucose oxidase (GOx) and small drug 5-fluorouracil (5-FU) within specific pores simultaneously and triggers unique guest-carrier cooperative anticancer capabilities. The stable ZIF-8 outer layer effectively blocks the core pores, preventing the undesired leakage of GOx into normal tissues. The acidity-induced ZIF-8 degradation gradually releases Zn and loaded 5-FU for chemotherapy under acidic tumor microenvironments. With the loss of the shielding effect of the ZIF-8 coating, the released GOx depletes intratumoral glucose (Glu) for starvation therapy. Notably, an accelerated cascade reaction occurs between ZIF-8 decomposition and GOx release, facilitated by the modulator factor of Glu. This culminates in the realization of synergistic cancer therapy, as comprehensively demonstrated by and experiments, as well as transcriptome sequencing analyses. Our work not only introduces a hierarchically porous MOF heterostructure with highly region-ordered pores but also provides a perspective for guest-carrier cooperative anticancer therapy.

摘要

大体积分子的传质,......生物酶,特别是对于跨尺度多生物分子,对微孔金属有机骨架(MOF)提出了严峻的挑战。在这里,我们通过外延生长策略在中空普鲁士蓝核上生长微孔 ZIF-8 壳,创造了具有高度区域有序的微孔、介孔和大孔的分级多孔 MOF 异质结构。这允许在特定孔内同时局部加载大生物酶葡萄糖氧化酶(GOx)和小分子药物 5-氟尿嘧啶(5-FU),并触发独特的客体-载体协同抗癌能力。稳定的 ZIF-8 外壳有效地阻挡了核心孔,防止 GOx 不受控制地泄漏到正常组织中。在酸性肿瘤微环境下,酸诱导的 ZIF-8 降解会逐渐释放 Zn 和负载的 5-FU 进行化学治疗。随着 ZIF-8 涂层屏蔽作用的丧失,释放的 GOx 会耗尽肿瘤内的葡萄糖(Glu)进行饥饿治疗。值得注意的是,ZIF-8 分解和 GOx 释放之间的级联反应会受到 Glu 的调节剂因子的促进。这最终实现了协同癌症治疗,这一点通过 和 实验以及转录组测序分析得到了全面证明。我们的工作不仅引入了具有高度区域有序孔的分级多孔 MOF 异质结构,还为客体-载体协同抗癌治疗提供了新的视角。

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