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Tumor-Activated Photosensitization and Size Transformation of Nanodrugs

机译:纳米肿瘤激活的肿瘤活性光敏和尺寸变换

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摘要

Effective intratumoral distribution of anticancer agents with good tumor penetration is of practical importance for photo-chemotherapy. Herein, a metal-organic framework (MOF) assisted strategy is reported for smart delivery of aggregation-induced emission photosensitizer (AIE PS) and chemodrug for deep tumor penetration to realize effective image-guided photo-chemotherapy. A newly designed AIE PS is loaded inside an iron(III) carboxylate-based MOF, MIL-100, to produce PS@MIL-100, which is encapsulated by doxorubicin (Dox) conjugated poly(ethylene glycol) methyl ether (PEG) to yield Dox-PEG-PS@MIL nanoparticles (NPs) with a diameter of 120 nm. After Dox-PEG-PS@MIL NPs reached the tumor site, intratumoral H2O2 can cause the release of the loaded PS at the tumor surface for activatable photodynamic therapy (PDT). The Dox-PEG segment is simultaneously triggered to self-assemble into ultrasmall Dox NPs. Under light irradiation, PDT is activated at the tumor surface, synergistically enhancing the tumor penetration of Dox NPs along with their ultrasmall size. After endocytosis of Dox NPs, free Dox is released from Dox NPs under low pH to enter cell nuclei for effective chemotherapy. Accompanied by bright far-red/near-infrared emission from the PS, image-guided photo-chemotherapy with enhanced efficacy is achieved.
机译:具有良好肿瘤渗透性的抗癌剂的有效腹腔内分布对于光学疗法具有实际重要性。在此,据报道了金属 - 有机框架(MOF)辅助策略用于综合诱导的发射光敏剂(AIE PS)和Chemodrug进行深层肿瘤渗透以实现有效的图像引导光学疗法。将新设计的AIE PS加载到铁(III)基于羧酸盐的MOF,MIL-100内部,以产生PS @ MIL-100,其被多柔比星(DOX)共轭聚(乙二醇)甲基醚(PEG)包封产生直径为120nm的DOX-PEG-PS @ MIL纳米颗粒(NPS)。在Dox-PEG-PS @ MIL NPS达到肿瘤部位后,肠瘤H2O2可以在肿瘤表面释放加载的PS,用于可激活的光动力疗法(PDT)。 DOX-PEG段同时触发到自动组装成超时的DOX NPS。在光照射下,PDT在肿瘤表面激活,协同增强DOX NP的肿瘤渗透,以及其超大尺寸。在DOX NPS的内吞作用后,在低pH下从DOX NPS释放免费DOX以进入细胞核以进行有效化疗。伴随着PS的明亮远红/近红外发射,实现了具有增强功效的图像引导式光疗。

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