Department of Biomaterials, College of Materials, Research Center of Biomedical Engineering of Xiamen & Key Laboratory of Biomedical Engineering of Fujian Province & Fujian Provincial Key Laboratory for Soft Functional Materials Research, Xiamen University, Xiamen 361005, China.
School of Pharmaceutical Science, Fujian Provincial Key Laboratory of Innovative Drug Target Research, Xiamen University, Xiamen 361005, China.
ACS Appl Mater Interfaces. 2020 Apr 1;12(13):14884-14904. doi: 10.1021/acsami.0c00970. Epub 2020 Mar 18.
Low drug payload and lack of tumor-targeting for chemodynamic therapy (CDT) result in an insufficient reactive oxygen species (ROS) generation, which seriously hinders its further clinical application. Therefore, how to improve the drug payload and tumor targeting for amplification of ROS and combine it with chemotherapy has been a huge challenge in CDT. Herein, methotrexate (MTX), gadolinium (Gd), and artesunate (ASA) were used as theranostic building blocks to be coordinately assembled into tumor-specific endogenous Fe-activated and magnetic resonance imaging (MRI)-guided self-targeting carrier-free nanoplatforms (NPs) for amplification of ROS and enhanced chemodynamic chemotherapy. The obtained ASA-MTX-Gd NPs exhibited extremely high drug payload (∼96 wt %), excellent physiological stability, long circulating ability (half-time: ∼12 h), and outstanding tumor accumulation. Moreover, ASA-MTX-Gd NPs could be specifically uptaken by tumor cells via folate (FA) receptors and subsequently be disassembled via lysosomal acidity-induced coordination breakage, resulting in drug burst release. Most strikingly, the produced ASA could be catalyzed by tumor-specific overexpressed endogenous Fe ions to generate sufficient ROS for enhancing the main chemodynamic efficacy, which could exert a synergistic effect with the assistant chemotherapy of MTX. Interestingly, ASA-MTX-Gd NPs caused a lower ROS generation and toxicity on normal cell lines that seldom expressed endogenous Fe ions. Under MRI guidance with assistance of self-targeting, significantly superior synergistic tumor therapy was performed on FA receptor-overexpressed tumor-bearing mice with a higher ROS generation and an almost complete elimination of tumor. This work highlights ASA-MTX-Gd NPs as an efficient chemodynamic-chemotherapeutic agent for MRI imaging and tumor theranostics.
低药物载量和缺乏肿瘤靶向性是化学动力学治疗(CDT)产生的活性氧(ROS)不足的主要原因,严重阻碍了其进一步的临床应用。因此,如何提高药物载量和肿瘤靶向性以放大 ROS,并将其与化疗相结合,一直是 CDT 面临的巨大挑战。在此,甲氨蝶呤(MTX)、钆(Gd)和青蒿琥酯(ASA)被用作治疗学构建模块,共同组装成肿瘤特异性内源性 Fe 激活和磁共振成像(MRI)引导的自靶向无载体纳米平台(NPs),以放大 ROS 并增强化学动力学化疗。所得的 ASA-MTX-Gd NPs 表现出极高的药物载量(约 96wt%)、优异的生理稳定性、长循环能力(半衰期:约 12 h)和出色的肿瘤积累。此外,ASA-MTX-Gd NPs 可以通过叶酸(FA)受体被肿瘤细胞特异性摄取,随后通过溶酶体酸性诱导的配位断裂被分解,导致药物爆发释放。最引人注目的是,产生的 ASA 可以被肿瘤特异性过表达的内源性 Fe 离子催化生成足够的 ROS 以增强主要化学动力学疗效,这可以与 MTX 的辅助化疗发挥协同作用。有趣的是,ASA-MTX-Gd NPs 在很少表达内源性 Fe 离子的正常细胞系中产生较低的 ROS 生成和毒性。在 MRI 引导下,通过自靶向辅助,对过表达 FA 受体的荷瘤小鼠进行了协同肿瘤治疗,ROS 生成更高,肿瘤几乎完全消除。这项工作突出了 ASA-MTX-Gd NPs 作为一种高效的化学动力学-化学治疗剂,可用于 MRI 成像和肿瘤治疗。
